WEBVTT 01:00.000 --> 01:29.840 I don't have the sound alerts. 01:29.840 --> 01:33.120 It's on the blank scene here. 01:33.120 --> 01:37.760 I apologize for that for playing that biology chant. 01:37.760 --> 01:41.640 If you play it when I'm on screen or when there are any graphics on, then we'll hear 01:41.640 --> 01:42.640 it. 02:29.840 --> 02:37.320 I think truth is good for kids. 02:37.320 --> 02:41.960 We're so busy lying, we don't even recognize the truth no more in this society. 02:41.960 --> 02:44.160 We want everybody to feel good. 02:44.160 --> 02:49.520 That's not the way life is. 02:49.520 --> 03:13.200 The world's protected stuff at all times, follow my instructions, keep it clean, touch 03:13.200 --> 03:16.000 gloves if you wish, let's do it. 03:16.000 --> 03:23.000 This is so crazy, like these bumps, this is so crazy, I feel so nervous, like what 03:23.000 --> 03:44.000 in the world, man? 03:44.000 --> 03:49.520 Good evening, ladies and gentlemen, good evening, welcome to the show, this is GIGO and biological. 03:49.520 --> 03:55.120 We're a little late tonight at 20 in the hour, but that's the way it works. 03:55.120 --> 04:00.200 Sometimes you can get on during the day like I plan to, sometimes I can't. 04:00.200 --> 04:01.800 Welcome very much to the stream. 04:01.800 --> 04:06.120 If you've been here for a while, you're here at the top of the wave, we are staying focused 04:06.120 --> 04:10.720 on the biology here, we don't take the bait on television, we love our neighbor. 04:10.720 --> 04:14.000 We're trying to rescue these skilled TV watchers down here at the bottom, the way 04:14.000 --> 04:19.600 this works is that people are donating, subscribing to the stream, and it's really, there is 04:19.600 --> 04:25.720 a small degree of momentum that's happening, you go to GIGO and biological.com, you can 04:25.720 --> 04:30.440 support the stream there with a one time little thing, you can communicate with us at GIGO 04:30.440 --> 04:41.560 and my confession is there, you can donate there, and then, whoa, hang on, you can see 04:41.560 --> 04:45.880 the schedule, and then down here at the bottom you can subscribe, and we're actually at 04:45.880 --> 04:55.720 about a 132 subscribers right now, and ideally I think if this was going to go on forever, 04:56.200 --> 05:02.600 if we were going to be here forever, we would need between 900 and 1,000 subscribers and 05:02.600 --> 05:07.560 we would be able to do this forever, and that's what we're really shooting for, I know that's 05:07.560 --> 05:15.320 a big goal, but we need to work as hard as we can to share the stream, if you can please support it, 05:16.520 --> 05:21.160 because I do want to keep it going, I do think we're making a difference, I do think that the 05:21.240 --> 05:26.920 message is getting out there, and so if you can share the work, get it out there, 05:27.960 --> 05:34.040 the independent bright web is growing very slowly, and I'm really, really excited how much progress 05:34.040 --> 05:46.920 we've made. So let's see here, I do believe I am prepared to shift over 05:46.920 --> 05:51.480 to the desktop. 05:54.040 --> 05:58.120 Good evening ladies and gentlemen, this is Giga Ohm Biological, a high resistance low noise 05:58.120 --> 06:04.840 information brief brought to you by a biologist, it is the 14th of February, that's right 2024, 06:05.800 --> 06:12.440 and we are still trying to continuously push back against that big hand in the picture there, 06:13.400 --> 06:19.640 that is consciously manipulating the organized habits and opinions of the masses, 06:20.600 --> 06:26.360 and we really need to start to understand this. More importantly, we need to help our children 06:26.360 --> 06:32.280 understand how vulnerable they are to this and how easily we were misled with just a few TV 06:32.280 --> 06:40.680 channels and a few newspapers, and now it is ever ever ever easier for these kinds of ruling powers 06:40.760 --> 06:46.920 to control everything that matters, and these weaponized piles of money are what we're really 06:46.920 --> 06:56.040 up against. So I've got my empire jacket on today, I used to be a cat and magician, I used to work 06:56.040 --> 07:01.720 at the University of Pittsburgh School of Medicine, so I was knee deep in this, I was neck deep into 07:01.720 --> 07:09.080 this, I fully believed that the vast majority of science being funded in America was a great idea, 07:09.160 --> 07:14.040 I was pretty skeptical of the just sheer amount of money they were throwing at cancer, 07:14.040 --> 07:19.800 but it never really dawned on me that the fundamental idea of how they were trying to cure it was wrong. 07:20.840 --> 07:25.960 Anyway, here we are, the principle of informed consent has been ignored for the duration of the 07:25.960 --> 07:34.440 pandemic, and it's not a lot we can seem to do about it, that's not what I want and I want this one, 07:35.320 --> 07:43.880 and so we're trying to push against this, and I went past that a little fast, because actually 07:43.880 --> 07:52.120 this hidden ruling power in our country, one proxy for it, one way to kind of understand it is how 07:52.120 --> 08:00.760 these intellectual dark web people were put in place between 2017, 18 and 19 and slowly used 08:00.840 --> 08:08.040 the algorithm and artificial means and you know, bros with shows having each other on their shows 08:08.040 --> 08:15.400 and collectively promoting each other through social media, we have an invisible sort of governance 08:15.400 --> 08:21.480 structure that influences us through social media and it shouldn't be underestimated how much of those 08:22.440 --> 08:26.680 avenues and opportunities have been harvested by the people who would like to control us. 08:27.320 --> 08:33.880 I really think we're very close to people starting to really catch on to the big picture that people 08:33.880 --> 08:40.680 like Mark and I have been able to see for quite some time. I think it's really starting to come 08:40.680 --> 08:47.800 into focus for us and we're starting to get better handles on how to share it with you and with others 08:47.800 --> 08:52.600 and so I'm very excited about it. I do think one of the bigger insights that we've had in the last 08:52.680 --> 08:58.280 six or eight months is really honing in on the idea that there was likely a coordinated worst 08:58.280 --> 09:06.440 case scenario team of medlers. People in behind the scenes funded by various sources of money, 09:06.440 --> 09:14.520 including you know, just weaponized piles of money and the idea was to fuel this worst case 09:14.520 --> 09:18.760 scenario so that the fear and uncertainty and doubt that would be necessary for people to go 09:18.760 --> 09:23.560 along with the lockdowns, to go along with the school closures and to go along with the 09:23.560 --> 09:28.040 testing and all this other yada yada that they rolled out in order to make sure that that was 09:28.040 --> 09:34.440 taken very seriously. They needed this to be taken as real and the worst case scenario is being 09:34.440 --> 09:41.480 plausible and in fact we know that this was not only drilled into number one, the publication 09:41.480 --> 09:47.800 record and number two, the upper level bureaucracy with tabletop drills. We also know that it was 09:47.800 --> 09:54.920 most likely done in a way in terms of the preparation for this or any other of such crisis, 09:54.920 --> 09:59.720 it was already drilled into those crisis preparations that when this happens, 10:00.840 --> 10:07.880 before we know how bad it is, we need the citizens of every nation in the world to take it seriously 10:07.880 --> 10:13.400 as though it is the worst case scenario in order to achieve the level of compliance that we're 10:13.480 --> 10:19.400 going to require if any of these non-pharmaceutical interventions are going to have any effect. 10:19.400 --> 10:23.800 In other words, if you don't take everybody doesn't take the masking seriously, the effect 10:23.800 --> 10:29.800 won't be significant. That's exactly what Brett Weinstein argues even now as he pseudo-apologizes 10:29.800 --> 10:33.480 for having allowed our children to be forced masks for a year and a half. 10:35.400 --> 10:41.000 Well, the effect wasn't significant. Was I dumb for advocating for masks? No, because we didn't 10:41.000 --> 10:47.080 know if they wouldn't work. That was his argument. And again, that's about teamwork case scenario. 10:47.080 --> 10:53.560 You don't have to be necessarily on board with the worst case scenario. You have to be on board 10:53.560 --> 11:00.360 with the possibility. And that's what would make the idea of wearing masks. If this was really 11:00.360 --> 11:08.120 a 50% kill rate virus, wearing masks to increase your chances of not getting it from 50% to 55%, 11:08.760 --> 11:15.800 according to Brett Weinstein might be a different difficult thing to measure, but it's definitely 11:15.800 --> 11:21.640 a significant. That's the kind of thinking that's going on in his head. As long as the numbers 11:21.640 --> 11:28.120 are small enough, they're not zero. And so since they're not zero, I wasn't wrong for advocating 11:28.120 --> 11:33.960 for this stuff. But what he doesn't see is that masking children for a year and a half and confusing 11:33.960 --> 11:39.480 adults for a year and a half with the use of lockdowns and the use of masks and goggles, 11:39.480 --> 11:46.840 which he also advocated for, created the illusion of worst case scenario as a legitimate possibility 11:46.840 --> 11:52.360 of a billion people dead, like Kevin McCarran said, a legitimate possibility. 11:55.880 --> 12:01.800 And so as we focus on the team worst case scenario, the other half of this idea of driving you into 12:01.880 --> 12:07.800 this fear, uncertainty and doubt was to get you motivated to solve the mystery of where did this 12:07.800 --> 12:13.480 thing come from? Because once you're considering that maybe I'm going to lose half of my family 12:13.480 --> 12:18.120 to this in a year and a half, you start to become very curious about where this actually came from 12:18.120 --> 12:26.040 and who's telling the truth. And that cleverly enough was also part of the orchestrated plan 12:26.040 --> 12:33.880 to make sure that they got maximum compliance. Because if they convinced the left and the right, 12:34.760 --> 12:42.200 when the mystery was solved, the conclusion is the preponderance of evidence points to a lab leak, 12:43.000 --> 12:49.640 then the worst case scenario has just been accepted. And you've just gone as far away from the truth 12:49.720 --> 12:55.880 as you possibly can if you accept that, wow, we just experienced a lab leak. It might have even been a 12:55.880 --> 13:02.600 lab release. And now you're as far away from understanding that intramuscular injection of 13:02.600 --> 13:07.640 any combination of substances with the intent of augmenting the immune system is dumb. Here is far 13:07.640 --> 13:13.560 away from understanding that is possible. And maybe you've even bought into the idea that 13:13.560 --> 13:18.520 transfection and healthy humans saved millions of lives rather than being criminally negligent. 13:19.800 --> 13:23.560 Again, as far away from the truth as you possibly could be. 13:26.760 --> 13:31.560 And if you believe that viruses are capable of circulating the globe for five years with high 13:31.560 --> 13:38.040 fidelity, and we have recorded millions of sequences as a result of this, this high fidelity, 13:38.760 --> 13:43.240 then you are as far away from the truth as you possibly can be because viruses are not pattern 13:43.240 --> 13:50.360 integrity. Holy cow, look at this. Whatever these signals are, these viruses, they're not 13:50.360 --> 13:57.960 pattern integrity. So, so we have this all cracked now, we have the broad, broad strokes of biology 13:57.960 --> 14:03.160 here. And if we can bring people to want to understand this, we have answers for this stuff. 14:03.160 --> 14:07.400 We can go as deep as they want to. And this, I think, is the way we're going to fight the spread 14:07.480 --> 14:10.680 of these bad ideas is we're going to spread good ideas. 14:12.440 --> 14:16.680 We don't have to worry about the spread of any RNA molecule right now. I assure you of that. 14:16.680 --> 14:23.320 But the illusion of consensus is still spreading. Brett Weinstein is on the Tucker Carlson show, 14:23.320 --> 14:28.200 and and Alex Jones spreading the illusion of consensus everywhere he goes. 14:28.200 --> 14:36.920 And Joe Rogan, quite around of of of PR for a guy who whose boat is sinking rapidly 14:38.280 --> 14:46.040 as the vast majority of the people on the internet realize that this guy is not the sort of thought 14:46.040 --> 14:53.080 leader that that we want him that he wants us to believe he is, and that his fans want to believe he 14:53.080 --> 15:01.160 was. But unfortunately, the real unfortunate thing is, is that a lot of the people on this 15:01.160 --> 15:06.200 screen back here were not the thought leaders that we they should have been. I was not the 15:06.200 --> 15:14.600 thought leader I should have been in 2020. And at at at some moment, I could have come to the truth 15:14.600 --> 15:21.880 had it not been for so many of these medlers. And yes, I'm very willing to blame it on other 15:21.960 --> 15:30.440 people in this scenario, because I tried my best to bounce the ideas that I'm now feeling are the 15:31.080 --> 15:37.320 closest to the target. I have been bouncing those ideas off of other people for quite some time and 15:37.320 --> 15:44.360 running into quite a lot of resistance to them. And it is with that resistance that creates the 15:44.360 --> 15:49.080 confusion and the doubt, you know, I didn't start out a virologist at the beginning of the pandemic, 15:49.080 --> 15:54.200 believe it or not. In fact, I didn't start out as an immunologist before the pandemic either. 15:55.000 --> 16:01.080 I started out as a broadly trained biologist, and a specifically trained neurobiologist. 16:02.600 --> 16:07.400 But I started with the requisite skills, which are, you know, reading and critical thinking. 16:11.640 --> 16:15.720 And so we have to push back. We're trying to organize a a sort of, 16:16.600 --> 16:20.840 uh, not we're trying to organize, we are noticing the organization 16:22.040 --> 16:25.320 of a group of people that seems to all have the same argument. 16:26.360 --> 16:32.120 And there's not a lot of coordination involved in in getting this group to finally coalesce. 16:34.440 --> 16:38.920 And so the question really is how long and how long is it going to take us to push back on this 16:38.920 --> 16:46.600 before the, the idea starts to become to penetrate just our side of the discussion where 16:46.600 --> 16:51.000 ladies and gentlemen, we need to consider the possibility there there was no significant spread 16:51.000 --> 16:57.240 of a risk pathogen. It's just not there. And that we might not understand the molecular biology 16:57.240 --> 17:01.560 as well as they think we should or they want us to believe we do. 17:01.960 --> 17:10.440 And so I've, I've been very, well, this is why that repeating. Am I pushing the wrong 17:10.440 --> 17:19.480 universal? There we go. So I wanted to do three videos of Ralph Barrick right at the beginning 17:19.480 --> 17:27.240 of the pandemic or right around the start or an hour in, an hour in a year in, because 17:27.560 --> 17:38.040 in a way, the naive betrayal of Ralph Barrick as being just this guy who's just trying to do his best 17:38.040 --> 17:46.760 to do good in the world is part of the Scooby-Doo. It's supposed to be so over the top that you think, 17:46.760 --> 17:51.960 wow, isn't it obvious that he's a bad guy? He's obviously responsible for this. 17:52.760 --> 18:00.760 Or the people who took his recipes are, maybe Alison Totura brought the recipe of this to 18:01.320 --> 18:07.560 US Amered. And that's the reason why, I don't know, in 2019, she wrote a paper with Cina Bavari 18:07.560 --> 18:12.600 about a coronavirus pandemic from China from a bat cave that needed Remdesivir. 18:15.400 --> 18:20.200 So let's watch a couple of these videos and see if we notice any patterns with the story that they 18:20.280 --> 18:27.560 tell about Ralph Barrick. And then after that, what I want to watch is a video from 2020 18:29.960 --> 18:36.600 where members of the US Department of Defense and US military are explaining how they plan to 18:36.600 --> 18:43.000 contribute to the look, the search for effective countermeasures. And this is at the beginning 18:43.000 --> 18:48.200 of March 2020. I think you're going to find this video very, very interesting. And I think I will, 18:49.160 --> 18:53.960 so we'll watch them all together. And these, I actually have only scanned one of them. The 18:53.960 --> 18:59.800 other two I didn't have before. These are both from PBS North Carolina. At least two of the three 18:59.800 --> 19:03.720 of them are from PBS North Carolina. I put them on Twitter before I even watched them. 19:03.720 --> 19:08.760 Universal specialists. That's a strange word. Universal specialists. 19:10.200 --> 19:16.200 People who have a creative toolbox that can rapidly employ that toolbox to whatever happens 19:16.200 --> 19:24.280 to come down the pipe in the future. You could say Ralph Barrick has an infectious passion for 19:24.280 --> 19:32.120 science, discovery, and coronaviruses. It's why he's known as the coronavirus hunter. I've studied 19:32.120 --> 19:41.560 coronaviruses since about 1984. I guess that's... It's hard to do the math. 36, 37 years. 19:41.560 --> 19:50.840 The coronavirus that causes COVID-19 took most of the world by surprise, but not Ralph Barrick. 19:50.840 --> 19:56.040 He's been on the front lines investigating coronavirus outbreaks throughout his career. 19:56.040 --> 19:59.880 I was attracted to coronaviruses for a couple of reasons. The first reason is we knew nothing 19:59.880 --> 20:04.760 about this family of viruses. The second thing is that what little we did know suggested that 20:04.760 --> 20:09.480 they had a very unique way to replicate in the cell that had never been described for any other 20:09.560 --> 20:15.960 RNA virus. I was interested in how viruses replicate, how their genomes are organized, 20:15.960 --> 20:22.360 and how they regulate gene expression. So coronavirus, a virus that has dominated our lives, 20:22.360 --> 20:27.640 what's it look like? How does it work? I'm going to do my best here at drawing this. I'm going to 20:27.640 --> 20:36.120 draw it from the inside out. The payload of the virus is called a nucleic acid. It's an RNA 20:36.120 --> 20:41.800 molecule that sort of is wrapped around here in the middle of the virus particle. And that RNA 20:41.800 --> 20:47.880 is coated in a protein that I'm going to call the nucleic acid protein. Now surrounding that 20:47.880 --> 20:54.520 is a little bubble of fat. Projecting out from this particle are these large petalimer spikes, 20:55.160 --> 21:00.120 and it gives the virus its unique appearance in the electron microscope, and it looks like a 21:00.200 --> 21:06.760 corona, or a halo around the sun. Hence the name coronavirus. Have you ever seen the 21:06.760 --> 21:12.200 movie Alien? There's these little plant-shaped things that sort of open up those flaps opening 21:12.200 --> 21:18.600 up right on the top is what happens on the coronavirus spike, and three of them anywhere from one to 21:18.600 --> 21:24.600 three of these can open up. Here's your host cell, and there's a protein here called ACE2. It has 21:25.160 --> 21:31.240 spaces in it that this can stick into that, and once that happens, boom. That was a bad 21:33.000 --> 21:38.120 that was whoops that was oh gosh I forgot that this was this was in PowerPoint. My bad 21:38.120 --> 21:43.480 strength in my mouth. It looks like they showed a picture they weren't supposed to show there. 21:43.480 --> 21:50.440 Those little details, but scenes and antibody, they show up, and it looks like they're showing 21:50.440 --> 21:57.640 antibody picture antibodies neutralizing the virus. Have you ever seen the movie Alien? There's 21:57.640 --> 22:03.880 these little plant-shaped things that sort of open up those flaps opening up. So think of this 22:03.880 --> 22:11.160 as a little bit of worst-case scenario as well, right? You don't need to provoke the alien, 22:11.160 --> 22:16.280 you know, you don't need to provoke alien as a way of explaining this. You could also explain 22:16.360 --> 22:25.560 it like a flower or something beautiful, but they always choose war or disease, right? 22:25.560 --> 22:32.120 And combating or it's always a negative and scary thing. Now they're actually showing a picture of 22:32.120 --> 22:38.520 the alien movie. Right on the top is what happens on the coronavirus spike, and three of them 22:38.520 --> 22:43.640 anywhere from one to three of these can open up. Here's your host cell, and there's a protein here 22:43.640 --> 22:50.680 called ACE2. It has spaces in it that this... Oops, that's not the right picture, right? That's 22:50.680 --> 22:55.800 not the right picture at all. This picture is, looks like antibodies that are neutralizing the 22:55.800 --> 23:01.720 spike and preventing them from binding, which is a bad cut on the part of PBS, but maybe not, 23:01.720 --> 23:07.800 if they're trying to throw this image into your head. Stick into that, and once that happens, boom, 23:08.520 --> 23:13.960 virus goes inside the cell and affects it. Look at his face, he's so excited. Look at that. 23:21.960 --> 23:31.480 Emerge, adapt, and revert with like a virus with like jaws in the middle, looks like. 23:32.280 --> 23:43.000 I mean, I don't know, you know, it's really a little bit like, is this a Scooby-Doo villain here? 23:43.000 --> 23:50.840 Is that what a Scooby-Doo villain would put on his door? Or is it like he is definitely a 23:50.840 --> 23:55.480 bio-weapon scientist, and so they put this there to make sure that nobody actually believes he is, 23:55.480 --> 24:00.920 because nobody who is really a bio-weapon scientist would put a bio-weapons jaws picture on their door, 24:01.720 --> 24:09.960 that says Emerge, adapt, and revert? It's just so comical to me, who are supposed to take this 24:09.960 --> 24:17.000 guy seriously. He's definitely a puppet or a pawn, even if he belongs in jail, because he figured 24:17.000 --> 24:23.080 some of this stuff out. He's not the guy who masterminded any of this. Like, he researchers 24:23.080 --> 24:29.560 worked 15 hour days in secure labs under strict protocols. Everyone united in the 24:29.560 --> 24:36.120 tedious process of analyzing the virus, and then testing drugs to create a vaccine to stop it. 24:37.880 --> 24:42.040 It's been a whirlwind of, you know, just absolute pressure, 24:43.000 --> 24:47.960 enjoyed to at the same time when we figured out that a lot of these projects that we were involved 24:47.960 --> 24:53.080 with was some of the major vaccine players. In fact, two out of the five Operation Warp Speed 24:53.800 --> 24:58.840 vaccines, both Johnson and Johnson and Moderna, so it was really a good day whenever we heard that 24:58.840 --> 25:03.560 the vaccines were incredibly effective in humans and face-free clinical trials. 25:05.480 --> 25:09.000 So there he's talking about the vaccines being very effective and them being very 25:09.000 --> 25:13.320 proud of it, because they were involved in both of them. That's pretty cool. I mean, I'd be pretty 25:13.320 --> 25:20.440 proud too, right? Not only have we been involved in developing vaccines and antibody therapeutics 25:20.440 --> 25:25.560 against the COVID-19 virus, but we're also preparing for treatments and therapeutics for 25:25.560 --> 25:30.760 other cousins of the COVID-19 virus that could potentially emerge into humans later on. 25:35.320 --> 25:40.840 Gentle ability to have a very large and experienced lab, so a lot of people are working pretty 25:40.840 --> 25:45.320 independently, heading up their own projects, forming working groups of like, okay, these people 25:45.320 --> 25:49.800 are really great cloner, so they're going to work on making a molecular clone of the virus. 25:49.800 --> 25:53.960 These people are really good with primary cells, so we're going to start collaborations with the 25:53.960 --> 25:58.600 Mercico Lung Institute and really try and understand what cell types are being infected 25:58.600 --> 26:03.320 and what's happening with them. These are our core mouse users, and so these people are going 26:03.320 --> 26:10.360 to work on developing mouse models of disease. Successful vaccines create a protective immune 26:10.360 --> 26:15.240 response in the body. Let's go back to the book. So all they really need is the sequence off the 26:15.240 --> 26:19.160 internet, and then they've got the cloners over there that can make the virus, and then they got 26:19.160 --> 26:23.400 these people with the cell cultures, and they got people with the animal models, 26:24.120 --> 26:28.600 you know, the humanized mice. I mean, it's all right there for you. It's really easy to see 26:28.600 --> 26:35.560 how easy this arrogant laboratory can go from virus to gain a function disaster in a matter 26:35.560 --> 26:45.160 of weeks. It's just brilliant. I mean, I don't know what questions are left to be answered other 26:45.160 --> 26:49.240 than which one of these people is responsible for. To see just how that happens. 26:50.760 --> 26:57.400 When the virus infects you, you make a protein called an antibody, and the goal of that antibody 26:57.400 --> 27:05.800 is to bind to the virus particle and prevent it from binding into that receptor, and prevent it 27:05.800 --> 27:13.800 from infecting that cell. The Beric Labs research was also central to the creation and clinical trials 27:13.800 --> 27:20.120 of the antiviral drug Remdesivir. Antiviral medicines prevent the development of severe 27:20.120 --> 27:27.960 disease. Similar drugs are in the pipeline. We're scientists, but what drives us really in people 27:27.960 --> 27:33.880 in this field is really public health, right? Yes, we're interested in the minutiae of how does 27:33.880 --> 27:38.280 the virus get in, how does it replicate? We're interested in all those little details, but the 27:38.280 --> 27:44.360 reason we're interested in them is because it translates to public health, to what's happening 27:44.360 --> 27:51.320 in people, and what can we do to help mitigate the disease burden, the suffering among people. 27:52.680 --> 27:58.840 It was an all-hands-on-deck approach, and it turned Chapel Hill into a lab bench to bedside 27:58.840 --> 28:06.600 place of research. Lots of interaction, especially as people moved in from other research areas where 28:07.240 --> 28:12.920 they maybe didn't understand quite how coronaviruses were, but they had some ideas about lung biology, 28:12.920 --> 28:18.040 or clotting, or other aspects of disease processes, and they needed to talk to people like Ralph, 28:18.040 --> 28:24.840 so that they could really make sure that they're thinking about the nature of the disease process 28:24.840 --> 28:30.440 correctly. Is the virus in the brain? Would you expect that to happen? Is the virus targeting 28:30.440 --> 28:34.680 different tissues? A lot of these things were still trying to get the answers to. 28:34.680 --> 28:42.760 And so, really, what he's describing is that a few people are the central hubs for any answers, 28:42.760 --> 28:50.120 in this case. And so, you can basically consider the entire NIH hierarchy to be more or less 28:50.120 --> 28:57.160 briefed based on what Ralph Barrack and Mark Denison and a couple other people say is 28:57.960 --> 29:04.920 the gold standard or the running truth right now. If Ralph Barrack says coronaviruses do this, 29:04.920 --> 29:10.840 and Mark Denison says, yes, Ralph's right, then that's what they're going to tell the bureaucracy. 29:10.840 --> 29:17.800 That's what's going to go all through this machine. And you're hearing that even the pharmaceutical 29:17.800 --> 29:23.240 companies and even these developers are calling Ralph for advice and consulting him. 29:24.120 --> 29:30.360 I doubt that he's taking all those calls for free, but there's where we are. 29:31.480 --> 29:35.960 If he is, he's taking those calls for free because they give him the prestige and the 29:35.960 --> 29:41.560 centrality and the control over the narrative that he's supposed to have. And it also puts him 29:41.560 --> 29:44.600 right at the focus of the Scooby-Doo, which is right where they want him to be. 29:44.600 --> 29:50.600 It's pretty fun stuff. 29:53.000 --> 29:59.480 Barrack's work saved countless lives and gave the world hope at a time it was desperately needed. 30:00.120 --> 30:05.480 Because of that, Barrack was given the OMAX Gardener Award, the highest honor for a faculty 30:05.480 --> 30:12.680 member in the UNC system. And when the pandemic happened, he and his team were able to move into 30:12.680 --> 30:20.440 action right away because they had this knowledge of these viruses. So not only could he understand 30:20.440 --> 30:27.320 the virus and work at the basic science level, but what Ralph does, it's really amazing, 30:27.880 --> 30:34.200 is that he also cares about applying that knowledge to developing vaccines, 30:34.200 --> 30:41.880 developing treatments, helping people avoid these diseases. He cares about individuals 30:41.880 --> 30:48.920 and populations, and that's what's really public health. And what he has done, he and his colleagues 30:48.920 --> 30:57.240 have done, will change the course of human history. Yeah, COVID-19, but that's funny. 30:57.240 --> 31:02.120 Infectious disease. Definitely gonna change the course of his actual questions here. 31:02.120 --> 31:07.800 Boy PBS works well with North Carolina, with the University of North Carolina, don't they, 31:07.800 --> 31:13.640 they work well from now. But we will be better prepared because of Dr. Barrack's work. You don't 31:14.360 --> 31:20.680 achieve these awards on your own, right? It's unfortunate enough to work with 31:21.480 --> 31:28.920 a large number of extraordinarily competent and proficient professionals who care deeply 31:28.920 --> 31:35.880 about human health and have dedicated a tremendous amount of their time and energy 31:38.200 --> 31:41.880 to not only build their credentials, but to make me look smarter than I really am. 31:42.280 --> 31:45.000 Quite frankly. 31:47.560 --> 31:50.760 Thanks y'all for watching this video, and if you want more where that came from. 31:50.760 --> 31:54.440 All right, let's keep going. This is awesome. I didn't realize they were going to be this good. 31:55.000 --> 31:59.800 Well, the last couple of years have been just incredibly intense. You have to understand, though, 31:59.800 --> 32:06.280 that this is what the Human Vaccine Institute is for. Our niche is to respond to the needs of 32:06.280 --> 32:11.240 society on problems that are not immediately attractive to the pharmaceutical industry, 32:11.240 --> 32:12.360 because they're so difficult. 32:14.920 --> 32:20.600 To really understand what researchers at the Duke Human Vaccine Institute are searching for, 32:22.360 --> 32:32.280 you have to go back to a 13th century legend. To this guy, King Arthur, who sent his 32:32.280 --> 32:38.760 nights of the roundtable on a quest for the Holy Grail. That term is now a metaphor for 32:38.760 --> 32:45.160 anything eagerly sought after. Uh oh. And after the COVID-19 pandemic 32:45.160 --> 32:50.520 had killed more than six million people in disrupted life across the entire planet, 32:51.080 --> 32:57.320 the Holy Grail for these scientists is creating a vaccine that protects against all kinds of 32:57.320 --> 33:03.720 coronaviruses. You know, we've had three epidemics now of coronaviruses. We had SARS, 33:04.360 --> 33:10.520 severe acute respiratory syndrome that occurred in 2003. We had Middle Eastern 33:10.520 --> 33:15.640 respiratory syndrome, MERS, that occurred in the Middle East, and then we have SARS-CoV-2 that 33:15.640 --> 33:21.560 arose from a bat virus in China. There's reason to expect there'll be another, and that candidate 33:21.560 --> 33:29.800 will be somewhere on the universe of coronaviruses. A vaccine that addresses a broad array of coronaviruses 33:29.800 --> 33:36.680 could stop a future pandemic. That type of vaccine is called a pan vaccine. I have a picture 33:36.680 --> 33:45.880 here of SARS-CoV-2. The receptors on those spikes are how the virus infects us. So the virus uses 33:45.880 --> 33:53.080 these red spikes on its surface to physically attach to cells of the respiratory system, 33:53.080 --> 34:00.600 either the upper respiratory system in our nose or down in our lungs and uses this molecule 34:00.600 --> 34:06.600 to infect our cells. But those receptors can also be targeted by antibodies and prevented from 34:06.600 --> 34:15.480 binding to human cells. So this is a model of an antibody. Vaccines teach our bodies to make 34:15.480 --> 34:21.800 antibodies, and those antibodies block viruses from attaching to the cells in our bodies 34:21.880 --> 34:28.680 and creating infections. Then I have here a model of this red molecule, the spike protein. So this 34:28.680 --> 34:37.560 is the spike protein that is present on all over a SARS-CoV-2 virus. Within the spike protein, 34:37.560 --> 34:43.880 there are pieces of it that bind to that host protein that it uses to infect ourselves. And 34:43.880 --> 34:52.440 that is called the receptor binding domain or RBD. This is the piece of the spike protein to which 34:52.440 --> 34:58.840 this antibody binds to prevent it from infecting. So by physically binding here, it blocks the 34:58.840 --> 35:09.160 infection of the SARS-CoV-2 virus. The key to creating a pan vaccine is finding a common receptor 35:09.160 --> 35:18.120 between many types of coronaviruses that an antibody can bind onto. That's easy. We have a pathway 35:18.120 --> 35:22.840 forward for how we expect to make the universe of coronavirus vaccine. And so that's what the team 35:22.840 --> 35:28.040 here is working on. We have a path forward. So we're going to go forward. The two vaccine developed 35:28.040 --> 35:35.000 at Duke and now in clinical trials may point the way to creating a pan vaccine. Oh come on. This 35:35.000 --> 35:39.560 vaccine is constructed. So if you've ever looked at a soccer ball, you'll know that it has tiny hexagons 35:39.560 --> 35:43.720 that come together to make the larger sphere. So that's what's shown here. And to the sphere, 35:43.720 --> 35:49.480 we basically use it as a scaffold where we can take a small piece of a virus. There you go. This looks 35:49.480 --> 35:53.640 a lot like what they did in Seattle, except Seattle, I think was a little bit more of this 35:53.640 --> 35:59.720 spherical soccer ball. And that allows us a really potent way of being able to target that specific 35:59.800 --> 36:05.880 piece of the virus. Early studies show the vaccine generates a strong immune response to the virus 36:05.880 --> 36:10.760 that causes some kind of particle. So that's how the vaccine has been designed is to really 36:10.760 --> 36:16.840 activate the immune system to see a specific site. And in this animation, it shows a blue 36:16.840 --> 36:23.320 molecule that's the receptor Biden domain from SARS-CoV-2. And so that blue molecule gets a 36:23.320 --> 36:29.080 rate around the surface of the molecule, the scaffold, and it makes the overall nanoparticle. 36:30.680 --> 36:35.720 But what if you place pieces of other types of coronaviruses on that scaffold? 36:36.440 --> 36:41.400 So what we know right now is that with one receptor Biden domain, you can induce a broad 36:41.400 --> 36:45.560 neutralizing antibody response. So these are the antibodies that block infection. 36:45.560 --> 36:50.280 But that can only get you so far. So that covers a certain number of viruses. 36:50.280 --> 36:54.840 But to really go towards a universal coronavirus vaccine where you really are covering the majority 36:54.840 --> 36:59.640 of coronaviruses, we know that we're going to need more than just one. And so this technology 36:59.640 --> 37:04.760 is amenable to that, meaning that you can then take multiple pieces of viruses from multiple 37:04.760 --> 37:07.960 different coronaviruses and array it and show it to the immune system. 37:10.920 --> 37:14.600 That's totally one of the things that yours are scrambling to find. 37:15.480 --> 37:20.360 Which parts of those of the spike protein are similar among all these viruses? 37:21.480 --> 37:26.360 So I think with the- And so the important thing to understand here is that if you talk about 37:26.920 --> 37:33.000 there being potentially a universal epitope or epitopes that are common across coronaviruses 37:33.000 --> 37:38.760 and you talk about targeting those with an antibody, it doesn't mean either of those things 37:38.760 --> 37:45.000 are possible that you can target an epitope with an antibody reliably and then produce it and get 37:45.000 --> 37:53.880 it to work. And number two, it doesn't mean that you're going to be able to create the immunity to 37:53.880 --> 38:02.120 that target and have it be meaningful. This is a- This is something that again, it kind of frames 38:02.120 --> 38:07.320 the- I almost lost my train of thought there. It frames the spectrum of debate with certain 38:07.320 --> 38:13.000 assumptions that if you're not sophisticated enough to realize that these assumptions aren't 38:13.000 --> 38:17.800 good assumptions, then you go along with their little charade here about what's possible. 38:18.600 --> 38:26.600 And so they- they repeat the- the assumptions that if we make this particle with more things on it- 38:26.600 --> 38:28.360 But to really go towards a universal- 38:28.360 --> 38:30.200 That we'll just create a universal- 38:30.200 --> 38:37.160 We'll cover the majority of coronaviruses by adding other spike proteins or other 38:37.160 --> 38:41.560 proteins to the outside of it and this technology is a minimal to that. 38:41.560 --> 38:46.520 What you need to understand what he's saying is that he can fit grant applications. 38:47.800 --> 38:55.160 He knows that there are upcoming grant calls that are going to ask for vaccine candidates 38:55.160 --> 39:01.560 that can generate immunity to specific targets and show demonstrate correlates of immunity that 39:01.560 --> 39:08.440 are antibodies. Hello. They all know how to play the game of getting money from the- 39:08.440 --> 39:15.080 from the NIH for vaccines. It's about generating an antibody response in a robust one at that. 39:16.520 --> 39:23.240 And that's why they're all telling the same story. We were just here a minute ago. The first video was 39:23.240 --> 39:29.480 Robert- was Ralph Barrack singing at a passion coronavirus for coronaviruses since 1984. That's a 39:29.640 --> 39:35.240 little weird. Why? Because we knew nothing about them and because they had a unique way of replicating. 39:37.000 --> 39:39.960 Is that really why he started to work on them? Because they had a unique 39:40.680 --> 39:49.560 way of replicating, isn't that weirdly on theme for the the exo gene exon gene and the proof 39:49.560 --> 39:52.680 reading of coronaviruses debate that we're in right now. 39:52.680 --> 39:57.480 And he said on what in that video as well that he just told the story of antibodies as being 39:57.480 --> 40:03.560 the primary immunity to coronaviruses. Then we moved on to the Duke Vaccine Institute that 40:04.120 --> 40:08.840 clarified that the pandemic disrupted life across the planet. We've had three pandemics, 40:08.840 --> 40:13.560 therefore another pandemic is coming and they want to make a pan coronavirus vaccine. 40:13.560 --> 40:18.360 They then emphasized that antibodies are primary immunity just like Ralph Barrack's video did. 40:18.360 --> 40:23.480 And then they said they have a nano particle carrier candidate that can augment the immune 40:23.480 --> 40:30.360 system usefully to several different targets. Well, holy crap, that's pretty impressive. 40:34.120 --> 40:41.000 Holy grail researchers are scrambling to find which parts of those of the spike protein 40:41.000 --> 40:47.000 are similar among all these viruses. So I think with the upfront work that we're doing now to 40:47.000 --> 40:51.640 really put in place the technology for manufacturing, we'll be able to move this really quickly once 40:51.720 --> 40:55.240 we decide on what's the right mix of coronaviruses for us to target. 40:59.560 --> 41:03.160 Thanks y'all for watching this video. And if you want more where that came from, 41:03.160 --> 41:08.200 check out our channel, Cy and C. So I had to. I had to. 41:14.200 --> 41:20.520 The opportunity to take fundamental scientific advances. And so I had to stop that one there 41:20.520 --> 41:27.160 because I couldn't believe what I was hearing, but so which parts which parts of the spike 41:27.160 --> 41:31.400 are shared across coronaviruses is what that guy asked at the end of that video. 41:33.400 --> 41:42.520 So there are approximately 29 to 31 proteins encoded in the coronavirus genome. And then you 41:42.520 --> 41:53.160 can also argue because virology talks often about alternative reading frames in a viral genome that 41:53.160 --> 41:58.680 can encode for more variants of proteins. And so you could have even more proteins than 30 or so 41:59.480 --> 42:04.360 in a in a virus genome, depending on how those alternate reading frames are used. 42:05.080 --> 42:11.800 Now secondly, the spike protein is one of the more variable proteins in the coronavirus genome. 42:11.800 --> 42:18.360 And there are lots of other more highly conserved proteins in the genome. The E protein tends to be 42:18.360 --> 42:25.080 more conserved. The N protein tends to be more conserved in the and many of the small proteins 42:25.080 --> 42:33.880 in poly protein one A and one AB are also conserved. I'm not sure if it's one A and one B or if it's 42:33.880 --> 42:40.920 one A and one AB. I think it's one A and one B, but it doesn't matter. There's a large open reading 42:40.920 --> 42:45.240 frame that encodes for a poly protein that needs to be cut into several proteins, then reassemble 42:45.880 --> 42:51.480 into the replication transcription complex or one of them. And those are also very conserved 42:51.480 --> 42:57.800 proteins. So it's very interesting already in that that video from Duke, where they have already honed 42:57.800 --> 43:06.200 in on and decided that all the relevant epitopes are in the spike because primary immunity is 43:06.280 --> 43:12.040 antibodies to the spike. And so what we were talking about last night is actually really 43:12.040 --> 43:19.960 important because that's the bad model, right? Anybody's in your blood for a apparently respiratory 43:19.960 --> 43:29.480 and interior virus is just ridiculous. And all of these people should know this. And if they don't, 43:29.480 --> 43:36.040 it's just shows how incompetent this this Academy edition factory has become. 43:37.000 --> 43:42.920 So this is another Ralph Barrick video, but I think it's a little later or it's by it's not 43:42.920 --> 43:49.320 by PBS. Let's put it that way. The clinic and see it undergo a trial and then see that the data 43:49.320 --> 43:54.920 is spectacular. That's incredibly rewarding. And in 2020, it happened twice. 43:55.080 --> 44:02.680 Our group has participated in the testing and development of the Moderna vaccine. 44:03.400 --> 44:09.240 The other time was remdesivir. Nice. Which we had worked on since about 2014. Twice. 44:11.080 --> 44:17.400 About two to three years before the SARS-2 pandemic, we started testing mRNA-based vaccines 44:18.120 --> 44:24.120 against other coronaviruses about the time that date. I mean, I would go so far as to say that 44:24.200 --> 44:31.880 Ralph Barrick's work and contribution to the use of remdesivir during the coronavirus pandemic 44:31.880 --> 44:39.720 is something that he should he should answer for because he should have come out and so 44:39.720 --> 44:44.200 should have marked Dennis and should have come out and said there's no way that this drug is 44:44.200 --> 44:49.640 appropriate for humans. And it's certainly not appropriate for humans that are already in the 44:49.720 --> 44:54.200 hospital because we already showed that. And both of those guys should have said something about 44:54.200 --> 44:58.760 it. And the fact that they didn't say anything about it means either they are on the take or 44:58.760 --> 45:04.840 they're on the the don't talk list like what I've listed back here behind the movie 45:06.200 --> 45:11.560 or they're they're actively participating in the worst case scenario because they they realize 45:11.560 --> 45:16.760 that it's a national security operation that whose goal is total compliance. 45:19.640 --> 45:23.960 I mean, mentioning remdesivir in multiple promotion videos and taking credit for it. 45:23.960 --> 45:30.520 I mean, that's that's that's as nasty as it gets because remdesivir is one of the things 45:30.520 --> 45:35.240 that's really helped to exacerbate the fear, uncertainty and doubt about what's going on in 45:35.240 --> 45:41.640 our hospitals and what's happening in our health care system. So you want to you want to call 45:41.640 --> 45:47.800 Barrick out for that? That's fine. But don't don't give me this he invented the no-seum technique. 45:47.880 --> 45:50.520 And that's the reason why we're here because that's ridiculous. 45:51.400 --> 45:57.160 Once the no-seum technique was published, once that somebody in virology said, hey, by the way, 45:57.160 --> 46:03.480 these these enzymes that recognize a sequence but cut somewhere else, these are really handy for 46:03.480 --> 46:10.200 making sticky ends and and litigating large pieces of DNA together and doing it usefully and making 46:10.200 --> 46:15.480 very big constructs. Oh, wow, cool. We wanted to do that in coronaviruses. We wanted to do that in 46:15.480 --> 46:18.760 all RNA viruses. We'll start using those enzymes. That's great. Thanks. 46:20.520 --> 46:25.880 And just like that, a technique becomes universal just like when somebody says, hey, you know, 46:25.880 --> 46:30.040 if you use powdered sugar in your angel food cake, you get a better result. Oh, wow, great. Cool. Thanks. 46:31.800 --> 46:35.480 You don't have to give credit to the French chef that came up with that idea. 46:35.480 --> 46:38.760 Oh, I learned that from the guy who learned that from the guy who learned that from the guy 46:38.760 --> 46:42.760 who learned that from that guy. And so it's his fault that we all make our cakes like this. 46:42.760 --> 46:50.200 That's ridiculous. This is a very simple insight into assembly of DNA. And it is the 46:50.200 --> 46:55.320 application of already long standing molecular biological techniques to make large quantities 46:55.320 --> 47:00.840 of it. And then it's already the application of large long standing techniques of converting 47:00.840 --> 47:08.760 that DNA to RNA. Just happens to be that this RNA is viral. And so apparently it does stuff. 47:08.840 --> 47:12.040 And it makes any codes for proteins that make stuff. 47:13.640 --> 47:19.160 And that's what RNA virology is all about. It's what that's what Ralph Berwick is covering up. 47:19.960 --> 47:28.200 And pretending is some kind of special magic potion book or or secret grimoire of recipes that only 47:28.200 --> 47:35.400 he has. But I guarantee you that Alison Totura took all those ideas and all those that knowledge 47:35.400 --> 47:43.800 with her to us amored when she went. And I guarantee you that when they wrote that paper in 2019 47:43.800 --> 47:50.520 Alison Totura and Cina Bavari when they wrote that paper, they were talking about the very 47:50.520 --> 47:56.760 techniques that Alison learned in Ralph Berwick's lab for reverse genetics that were first pioneered 47:56.760 --> 48:06.280 by people like David Baltimore. I was about to call him James Baltimore, David Baltimore. 48:09.720 --> 48:15.960 And so David Baltimore is the first guy who made a clone of RNA virus in DNA and then translated it 48:15.960 --> 48:20.920 RNA and it found out that it worked or did what they wanted it to do and made particles. 48:21.880 --> 48:28.200 Now you want to look at that in those experiments and decide if that's really what happened, 48:28.200 --> 48:35.880 go ahead and shoot and knock yourself out. But the point is is that Ralph Berwick didn't invent it. 48:37.160 --> 48:42.520 He's just one guy in a long list of dudes who's you know clever with molecular biology, 48:42.520 --> 48:48.120 but once it's out there, it's like bacon cakes. Once he figured out how to do it, 48:48.120 --> 48:53.160 yes, the DoD knew how to do it. And there were lots of other scientists in the DoD who are 48:53.160 --> 49:01.880 just as capable at the bench at mini-preps and and maxi-preps as as Ralph Berwick's grad students. 49:01.880 --> 49:02.600 I assure you. 49:02.600 --> 49:10.120 It was rolling out SARS-Coronavirus 2 emerge. 49:16.600 --> 49:22.760 We were charged very early on to develop animal models of human disease so that we could immediately 49:22.760 --> 49:29.960 test these vaccine candidates by April of 2020. We had to have all the data completed by the end 49:29.960 --> 49:34.920 of June of 2020 so it could be included in the FDA packets that went forward for approval, 49:34.920 --> 49:38.840 for phase three testing. So a lot of stress on people in the lab. 49:41.240 --> 49:47.080 We're going from a new virus that we received in late February to having all of that done 49:47.080 --> 49:51.720 by the end of June so that we could begin phase three testing with the Moderna. 49:51.720 --> 49:57.880 Late February, he says, they received the virus in late February as if he needed the virus to, 49:57.880 --> 50:00.600 you know, to make the synthetic clone. 50:04.920 --> 50:08.920 When was this the Hohomish County man? Was that February? Was he February? 50:08.920 --> 50:15.000 Is anybody out there? Talk to me, Goose. Was it February that that's the Hohomish County man? 50:15.000 --> 50:23.320 Was he January? Talk to me, Goose. Vaccine by August. It was non-stop here for for some of 50:23.320 --> 50:29.800 the coronavirus. I volunteered to be part of the trial. I figured if I was involved in the 50:29.800 --> 50:34.600 preclinical development, I should be one of the first ones to see how well it worked in humans 50:34.600 --> 50:39.000 and so I volunteered for the phase three trial and when they jabby in the arm with the vaccine, 50:39.000 --> 50:44.920 it was very real. I could assure you it was very real. There's a protein here called ACE2. 50:44.920 --> 50:51.240 It has spaces in it that this can stick into that and once that happens, boom. 50:52.200 --> 50:54.680 Virus goes inside the cell infection. That's the infection. 50:56.760 --> 51:01.800 This was a collaborative effort. There it is again. Other key players certainly were Moderna 51:01.800 --> 51:08.120 and researchers at the National Institute of Health. The unsung heroes are 15 people in my lab 51:08.120 --> 51:14.760 that work non-stop from February through December. So is this already a hint that they're going to 51:14.760 --> 51:19.320 throw Pfizer under the bus for process two but they're going to say that Moderna didn't cut that 51:19.400 --> 51:25.320 corner or what? I don't understand how that works. Did Moderna cut that corner or not? I don't 51:26.360 --> 51:36.520 understand. I don't remember what was the what Kevin McCurnan's data shows if there's DNA in both 51:36.520 --> 51:43.560 or not. The rapid response in terms of therapeutic antibodies, vaccines and drugs against COVID-19 51:43.560 --> 51:49.000 is sort of an unparalleled scientific achievement in biology and microbiology and medicine. 51:54.520 --> 51:59.080 That entire infrastructure of collaboration and interaction. I think he could have taken it 51:59.080 --> 52:06.520 interface paid off. It paid off for the American people. Having said that, we can do better. 52:06.520 --> 52:12.200 We learned that we need to reinvest in public health. We need to speak with a single voice 52:12.200 --> 52:19.720 in a pandemic. And we need to figure out how to deal with misinformation on social media, 52:19.720 --> 52:25.160 which we have not been able to deal with effectively. It's tough. We're strong. We have a new variant 52:26.120 --> 52:32.760 and the lab is gearing up to respond to that variant to understand its biology, its impact on 52:32.760 --> 52:39.480 therapeutics and vaccines and drugs, how best to counter it if some of the products that are on 52:39.560 --> 52:50.040 a shelf lose their potency. There's no time to celebrate. I mean, there's always another variant 52:50.040 --> 52:56.840 emerging. There's other other products that need to be tested. We just keep grinding on and on and 52:56.840 --> 53:02.520 on. Hey, you got to get up and make the donuts every day, baby. Investing into looking and studying 53:02.520 --> 53:08.920 that basic biology of life will result in modern miracles of medicine. Oh, here we go. 53:10.200 --> 53:15.800 The basic biology of life and the modern miracles of medicine. Okay, check this out. Check this out. 53:15.800 --> 53:24.520 This is the website that I'm on. It is a defense website. I'm going to put the linky link in the 53:24.520 --> 53:31.960 chatty chat because I want you to be able to download this. It's actually downloadable. 53:33.080 --> 53:38.760 So you can scroll down to the video here and you can actually just click download and download it. 53:38.760 --> 53:43.640 And so I already did that. And so I'm not going to use my bandwidth to show you the video. I'm 53:43.640 --> 53:48.920 just going to show it to you back here. Okay. And this is a video that took place on March 5th, 53:49.000 --> 53:58.200 2020. And I can't stress enough. The people are like these guys are like James Giordano. They're 53:58.200 --> 54:03.400 going to throw a lot of lingo at us, but I'm going to I'm going to I'm going to try and 54:03.960 --> 54:09.240 keep up with my notes. And I think you're going to find it quite shocking. I want to give 54:09.240 --> 54:18.040 Sorry, I want to give a shout out to 54:27.080 --> 54:29.480 I want to give a shout out to 54:29.480 --> 54:37.640 where is this sub stack democracy manifest sub stack. 54:39.960 --> 54:45.320 The writer or one of the writers of that sub stack gave me a heads up on this video and I 54:45.320 --> 54:49.160 thought it was just so cool. The first five minutes of it I wanted to watch with you tonight. So 54:49.160 --> 54:54.280 here we are. Hopefully this will go rather quickly and I won't have to interrupt too much, but it's 54:54.280 --> 55:02.120 pretty shocking. Remember, this is March 2nd or March 5th. It's March 5th and it's the Pentagon 55:02.120 --> 55:07.080 and it's a real DoD video. It's the first one on their little private site. 55:10.680 --> 55:19.240 No masks. March 5th. Warp speed and the development of vaccines. 55:19.240 --> 55:25.480 Okay. Good afternoon, everybody. Thanks for coming to our press briefing on the army support 55:25.480 --> 55:30.440 to vaccine development. My name is Colonel Kathy Turner. I'm the director of the Army 55:30.440 --> 55:35.720 Media Relations Division and I will moderate today's session. The following senior leaders 55:35.720 --> 55:41.000 will be on our on today's panel. We have Brigadier General Mike Talley, commanding general of 55:41.000 --> 55:46.600 U.S. Army Medical Research and Development Command and Fort Detrick. We have Colonel Wendy 55:46.600 --> 55:51.480 Sammons Jackson, director of military infectious disease research program, 55:51.480 --> 55:57.400 U.S. Army Medical Research and Development Command. We have Dr. Nelson Michael, director of the 55:57.400 --> 56:03.320 Center for Infectious Disease Research, Walter Reed Army Institute of Research, and we have Dr. 56:03.320 --> 56:10.440 Kavan Majerad, director of emerging infectious diseases, Walter Reed Army Institute of Research. 56:10.440 --> 56:15.320 Today's discussion is on the record. After Brigadier General Talley's opening remarks, 56:15.400 --> 56:20.680 I ask that you limit yourselves to one question and one follow-up until we have gotten around 56:20.680 --> 56:25.800 the room and then we'll continue to field questions until we're at a time. We have about 30 minutes 56:25.800 --> 56:32.200 today and with that I'll turn it over to you, sir. Okay. Hey, good afternoon and thank you for 56:32.200 --> 56:38.360 participating in today's briefing. Our hearts go out to those that are affected or know someone 56:38.360 --> 56:45.080 who's affected by this disease. You know, emerging to infectious diseases like this coronavirus 56:45.080 --> 56:51.080 that we're facing now are COVID-19 or why a global network of military infectious disease 56:51.080 --> 56:57.640 surveillance laboratories exist around the world. Military medical research is a force multiplier 56:57.640 --> 57:02.760 designed to support the service member and the public in every conceivable circumstance. 57:03.480 --> 57:09.000 Through both emerging science and technological advances, the United States Army Medical Research 57:09.000 --> 57:13.240 and Development Command is on the forefront of delivering medical capabilities faster 57:13.720 --> 57:19.320 and more efficiently than ever before. We are supporting a whole-of-government approach 57:19.320 --> 57:25.480 to detect, prevent, and treat COVID-19 and when it comes to infectious disease threats, 57:25.480 --> 57:29.560 we have extensive capabilities and an international research infrastructure 57:30.200 --> 57:34.760 already in place that allows our scientists to anticipate and develop countermeasures 57:34.760 --> 57:40.920 against emerging infectious diseases. COVID-19 infrastructure development command is on the 57:40.920 --> 57:45.960 forefront of delivering medical capabilities faster and more efficiently than ever before. 57:46.920 --> 57:52.760 We are supporting a whole-of-government approach to detect, prevent, and treat COVID-19 57:53.480 --> 57:58.920 and when it comes to infectious disease threats, we have extensive capabilities and an international 57:58.920 --> 58:04.040 research infrastructure already in place that allows our scientists to anticipate 58:04.040 --> 58:09.400 and develop countermeasures against emerging infectious diseases. Okay, so I hear a global 58:09.400 --> 58:16.040 network of surveillance laboratories already in place. I hear global extensive capability of 58:16.040 --> 58:23.880 existing research infrastructure and I hear him advocating for a whole government approach to 58:23.880 --> 58:29.560 responding to the coronavirus. Let's make sure I got that about right. Wow. The United States Army 58:29.560 --> 58:34.200 Medical Research and Development Command is on the forefront of delivering medical capabilities 58:34.200 --> 58:40.840 faster and more efficiently than ever before. We are supporting a whole-of-government approach 58:40.840 --> 58:47.000 to detect, prevent, and treat COVID-19 and when it comes to infectious disease threats, 58:47.000 --> 58:51.080 we have extensive capabilities and an international research infrastructure 58:51.720 --> 58:56.280 already in place that allows our scientists to anticipate and develop countermeasures 58:56.280 --> 59:04.040 against emerging infectious diseases. COVID-19 is the infection caused by the SARS-CoV-2 virus 59:04.520 --> 59:10.280 and this is familiar territory for our team. Our labs have previously studied SARS and MERS, 59:11.080 --> 59:16.600 both of which are coronaviruses. They're in that same family. Our researchers and scientists at 59:16.600 --> 59:23.000 the Walter Reed Army Institute of Research conducted the first in-human phase one trials of the MERS 59:23.000 --> 59:30.440 vaccine and that's the only MERS countermeasure and the only and only the third coronavirus vaccine 59:30.440 --> 59:37.320 ever tested in humans. We're building upon the science for COVID-19 solutions as we speak right 59:37.320 --> 59:45.160 now. Just this week we were able to develop new versions of COVID-19 candidate, one of the first 59:45.160 --> 59:50.520 candidates that we've tried, and we initiated research to determine if there is a response to 59:50.520 --> 59:56.520 the vaccine. Again, this is just one piece of the solution. There's other vaccine candidates 59:56.520 --> 01:00:02.120 being developed by other organizations, but we're all working toward a solution and we want to 01:00:02.120 --> 01:00:06.520 get it done as quickly as possible and we're doing this in a whole of government fashion 01:00:06.520 --> 01:00:13.160 and certainly a whole of DOD fashion. In addition to vaccine prevention, we are also exploring 01:00:13.160 --> 01:00:18.920 treatments. Efforts are ongoing right now to identify new drug candidates to respond to the 01:00:18.920 --> 01:00:25.320 COVID-19 infection. A cooperative research and development agreement with an industry partner 01:00:25.320 --> 01:00:30.520 is under review for the DOD to gain access to an antiviral drug for treatment use 01:00:30.520 --> 01:00:36.120 in our medical centers, our military treatment facilities. So together with our United States 01:00:36.120 --> 01:00:42.840 government partners, we are progressing at very fast rates, revolutionary rates almost, 01:00:43.720 --> 01:00:49.320 constant effort, and this is in order to deliver effective treatment and prevention products. 01:00:49.320 --> 01:00:53.240 Products that will protect the citizens of the world and preserve the readiness 01:00:53.320 --> 01:01:00.600 and lethality of our DOD's service members. I want to thank you in advance, but I'd also like to 01:01:01.720 --> 01:01:09.800 tell you a little bit about my teammates here. So Colonel Dr. Wendy Sammons-Jackson is the director 01:01:09.800 --> 01:01:16.040 for our military infectious disease portfolio. She dual hats as the joint program committee 01:01:16.840 --> 01:01:23.080 director for the entire DOD. So when you're looking at the capabilities and capacity within 01:01:23.400 --> 01:01:28.920 the medical research and development command, the demand signal is coming from all over the 01:01:28.920 --> 01:01:35.960 joint forces. She's managed that portfolio for the last two years, and when you talk about some 01:01:35.960 --> 01:01:44.520 of the most recent accomplishments with MERS, with Zika, she has been involved in all those things. 01:01:45.320 --> 01:01:54.680 Dr. Nelson-Michael, about 37 years of experience. Same thing. We talk about some of our latest 01:01:54.680 --> 01:02:01.320 successes with MERS. Both he and Dr. Kavan Mujarit have been right at the forefront, 01:02:01.320 --> 01:02:08.920 and even with Zika, I'm very proud to say that within nine months, this is the team that was able 01:02:08.920 --> 01:02:20.360 to start the first inhuman clinical trials. And just last December of 19, the MERS CO-V 01:02:20.920 --> 01:02:28.840 correction, the Ebola-Zaire version vaccine was given full FDA approval. These two gentlemen were 01:02:29.880 --> 01:02:38.600 played a big part of that. Dr. Kavan Martin, again, having been the scientist behind a patented 01:02:38.600 --> 01:02:46.520 adjuvant that's designed for this same family of diseases, it's an adjuvant that's being used 01:02:46.520 --> 01:02:52.920 right now, being shared with our whole of government partners. He just recently returned from 01:02:52.920 --> 01:02:58.520 Switzerland. We were lucky enough to be able to recruit him from the World Health Organization, 01:02:59.560 --> 01:03:05.560 he's been back for about a week from Switzerland. So when you look at certainly the scientists that 01:03:05.560 --> 01:03:12.520 that we recruit and train within the DOD, they are well integrated with some of the top scientists 01:03:12.520 --> 01:03:17.080 in the country. And so we're very proud to take part in this effort, and we look forward to your 01:03:17.080 --> 01:03:25.400 questions. That is hysterical. I love the help of the Associated Press. They got somebody to come 01:03:25.960 --> 01:03:34.760 from the World Health Organization. So they had their own candidate of vaccine. Is that what 01:03:34.760 --> 01:03:40.760 you understood too? Because I couldn't tell whether he was hinting that the DOD was working with NIH, 01:03:40.760 --> 01:03:45.880 or whether the DOD had their own vaccine that was in competition with the NIH vaccine versions. 01:03:48.360 --> 01:03:55.240 He established that SARS-CoV-2 causes the disease COVID, and he started this by apologizing and 01:03:55.240 --> 01:04:02.280 expressing condolences for anybody that suffered from this disease. They were supporting a new drug 01:04:02.280 --> 01:04:10.520 search. And the team that ran the Zika trials is this same team. And these guys were also involved 01:04:10.520 --> 01:04:16.120 in the Ebola vaccine. And then the last person is somebody that they got from the who. Wow, this is 01:04:16.120 --> 01:04:22.840 just, this is just, this is just, I mean, wow, a proprietary adjuvant also. So handy. What a great, 01:04:22.840 --> 01:04:29.880 what a great team. However, this most applies. Just on the vaccine. Can you talk a little bit, 01:04:29.880 --> 01:04:35.560 just more detail about the vaccine, your work that's being worked on. Is it different than 01:04:36.520 --> 01:04:43.240 NIH's approach and how soon are you to for like a phase one trial? And then I'll just 01:04:43.240 --> 01:04:51.160 throw the follow up out just in case that's easier. The rapid diagnostic that is being worked on, 01:04:51.720 --> 01:04:56.040 can you talk a little bit about that and how sort of where you are in the rapid diagnostic 01:04:56.120 --> 01:05:02.280 tool and how soon that might also be available for testing? 01:05:03.080 --> 01:05:09.080 Yes, ma'am. Let me just take the first two questions quickly and give you over to Dr. 01:05:09.080 --> 01:05:14.600 Majard who can talk about some more granular aspects of this vaccine. First thing, 01:05:14.600 --> 01:05:20.200 it's one I want you all to know is that we have been around the Walter Reed Armada Institute of 01:05:20.200 --> 01:05:25.800 Research for 127 years. I mean, we are, a lot of people like to ask, well, why is the army 01:05:25.800 --> 01:05:29.800 involved in vaccine development? We've been doing this for an extremely long period of time. Walter 01:05:29.800 --> 01:05:34.600 Reed, I've obviously made his notoriety on figuring out countermeasures to yellow fever. So we've 01:05:34.600 --> 01:05:39.240 been doing this for an extremely long time. It's one, two is that we work very closely in the 01:05:39.240 --> 01:05:45.080 interagency space. The, my first raider in the army, I recently retired as Bob Redfield as a 01:05:45.160 --> 01:05:49.640 CDC director. My second raider is Debbie Burks. Now, obviously, the global AIDS coordinator and 01:05:49.640 --> 01:05:55.320 running the COVID response under the vice president and Dr. Fauci is close enough to him that he 01:05:55.320 --> 01:06:01.080 retired me about 18 months ago. So we work very, very closely in the interagency space in the 01:06:01.080 --> 01:06:07.560 vaccine that I'll let Dr. Majard talk about. We worked with Dr. Fauci's team to find a space 01:06:08.200 --> 01:06:13.800 where we could find a vaccine candidate that was scientifically not duplicative but mutually 01:06:13.800 --> 01:06:19.640 supportive of what others were doing, but also made sense. And so we ended up moving on two 01:06:19.640 --> 01:06:26.600 different vaccine platforms in coordination with Dr. Fauci and his team. Let me let Dr. Majard 01:06:26.600 --> 01:06:32.200 tell you a little bit more about that and what our rough timelines could be. Thanks for your 01:06:32.200 --> 01:06:38.600 question, Dr. Fauci and his team. His name is Dr. Nelson Michael and he's the director of the 01:06:38.600 --> 01:06:45.720 Center of Infectious Disease Research at Walter Reed Army Institute of Research. Dr. Nelson Michael. 01:06:46.920 --> 01:06:52.680 Let me let Dr. Majard tell you a little bit more about that and what our rough timelines 01:06:52.680 --> 01:06:59.800 could be. Thanks for your question. So from the first day that the sequences of the new virus 01:06:59.800 --> 01:07:12.680 were published, this guy is Dr. Kavran, Kavan, Maad Majarad, M-O-D-J-A-R-R-A-D. 01:07:13.400 --> 01:07:19.240 And I think this is the dude that they got from the World Health Organization. He looks like a 01:07:19.240 --> 01:07:25.720 very dark version of beaker from the Muppets. We were working on this vaccine and we were doing 01:07:25.720 --> 01:07:32.600 so in coordination with our interagency partners at the NIH, specifically the vaccine research 01:07:32.600 --> 01:07:38.360 center where the president was visiting just a couple of days ago and which is the place that I 01:07:38.360 --> 01:07:44.280 came from where I trained under Dr. John Mascol and Dr. Barney Graham there and have been in constant 01:07:44.280 --> 01:07:50.200 communication very much like we did for the Zika vaccine where the NIH and Walter Reed Army Institute 01:07:50.200 --> 01:07:58.280 of Research had two complementary approaches towards a vaccine candidate for Zika. Here again, 01:07:58.280 --> 01:08:05.480 we're taking a platform that actually has been used in clinical trials so far for influenza or 01:08:05.480 --> 01:08:14.840 different respiratory virus and focusing on a component of the virus that a lot of groups are 01:08:14.920 --> 01:08:21.160 working on but with a unique platform and a unique what's called adjuvant which is a 01:08:23.320 --> 01:08:29.800 chemical that is used in combination with vaccines all the time to enhance their immune response 01:08:30.440 --> 01:08:38.360 and that adjuvant is actually patented by the Army. So we see this as a unique and complementary 01:08:38.360 --> 01:08:44.840 approach that is non duplicative that is being coordinated as part of the whole of government 01:08:44.840 --> 01:08:50.040 response. It's such a weird it's such a weird thing to say it's non duplicative when he started 01:08:50.040 --> 01:08:55.480 four or five sentences earlier saying that we're going to make a vaccine using basically the same 01:08:55.480 --> 01:09:01.080 viral component that everybody else is focusing on listen carefully. So it's totally duplicative 01:09:02.040 --> 01:09:08.280 especially when you realize there are 30 proteins in the or 31 or 45 depending on what reading 01:09:08.280 --> 01:09:14.600 frames are read with a unique platform and a unique what's called adjuvant which is a 01:09:16.600 --> 01:09:22.600 a chemical that is used in combination with vaccines all the time to enhance their immune 01:09:22.600 --> 01:09:29.480 response and that's not right it's not used in combinations in combination with a vaccine 01:09:29.560 --> 01:09:36.600 it is a component of almost every vaccine the adjuvant is the chemical that irritates the 01:09:36.600 --> 01:09:45.720 immune system and gets it activated to do something and the big joke among amongst adjuvant chemists 01:09:45.720 --> 01:09:51.880 is the toxicity and that more toxic it is the more adjuvant it is the better adjuvant it is 01:09:51.880 --> 01:09:58.040 it's a joke amongst them. Ladies and gentlemen this is already in fifth of December somebody 01:09:58.040 --> 01:10:05.880 misleading very important people or misrepresenting the immune system because they don't understand 01:10:05.880 --> 01:10:12.600 it in either way screwing a lot of people over starting on March 5th 2020 by emphasizing antibodies 01:10:14.360 --> 01:10:19.800 and saying that adjuvants are something other than separate from a vaccine are you kidding me 01:10:20.760 --> 01:10:21.800 are you kidding me? 01:10:27.160 --> 01:10:33.160 Under Dr. John Mascol and Dr. Barney Graham there and have been in constant communication 01:10:33.160 --> 01:10:38.440 very much like we did for the Zika vaccine where the NIH and Walter Reed Army Institute of Research 01:10:38.440 --> 01:10:46.760 had two complementary approaches towards a vaccine candidate for Zika. Here again we're taking a 01:10:46.760 --> 01:10:54.280 platform that actually has been used in clinical trials so far for influenza a different respiratory 01:10:54.280 --> 01:11:03.640 virus and focusing on a component of the virus that a lot of groups are working on but with a 01:11:03.640 --> 01:11:13.000 unique platform and a unique what's called adjuvant which is a chemical that is used in 01:11:13.000 --> 01:11:19.240 combination with vaccine. So the army had their own thing and the army was going to do an adjuvanted 01:11:19.240 --> 01:11:23.720 vaccine that's what you're hearing right here. It means all the time to enhance their immune 01:11:23.720 --> 01:11:31.960 response and that adjuvant is actually patented by the army so we see this as a unique and 01:11:31.960 --> 01:11:38.840 complementary approach that is non-duplicative that is being coordinated as part of the whole 01:11:38.840 --> 01:11:44.120 of government response. I know you asked a question about the point of care testing. 01:11:45.960 --> 01:11:50.600 Unfortunately I think we have the world's leading expert in infectious disease diagnostics. This 01:11:50.600 --> 01:11:56.600 happens to be in the army at the Walter Reed Army Institute of Research Dr. Sheila Peel. Sheila 01:11:56.600 --> 01:12:02.840 like me really isn't has been working on HIV almost her whole professional career and there isn't a 01:12:02.920 --> 01:12:09.880 what did I say yesterday every one of these people cut their teeth in the HIV industry in the HIV 01:12:10.520 --> 01:12:21.480 space every one of them. It is absolutely extraordinary. It's just absolutely extraordinary. Single HIV 01:12:21.480 --> 01:12:25.800 rapid test that's out in the market that hasn't at some level passed through her hands so 01:12:26.360 --> 01:12:31.960 she's really our lead for looking at the diagnostics that are currently being used a test that would 01:12:31.960 --> 01:12:36.760 allow us to understand whether someone's infected or has been exposed and I can tell you that for 01:12:36.760 --> 01:12:42.840 now most of those tests are based on detecting the virus itself so developing the kind of test 01:12:42.840 --> 01:12:48.520 like a pregnancy test that you might be familiar with is requiring a different kind of technology. 01:12:48.520 --> 01:12:54.360 Sheila's is already having those kinds of discussions. I think what you're going to probably see is 01:12:54.360 --> 01:12:58.440 much more sophisticated and higher throughput tests that initially would be done in more 01:12:58.440 --> 01:13:03.560 sophisticated laboratories and then as time goes on that technology will then roll out 01:13:03.560 --> 01:13:07.560 to establish platforms to allow these tests to be moved more at the point of care. 01:13:08.760 --> 01:13:16.120 And so what he's describing there are the dissemination of EUA approved testing platforms, 01:13:16.120 --> 01:13:21.480 testing supply companies all this stuff needed to happen behind the scenes. 01:13:22.120 --> 01:13:26.760 It's not just like you know my wife and I if we would have gotten it in our heads we could have 01:13:26.760 --> 01:13:31.080 started doing a PCR testing company in 2020 and be millionaires now. 01:13:32.360 --> 01:13:35.400 Would you have thought to do that? How many of your friends thought to do that? 01:13:37.000 --> 01:13:42.280 And yet somehow or another all around the United States there were these private companies that 01:13:42.280 --> 01:13:49.080 sprung up out of nowhere and had had the wherewithal to set up a pretty complex molecular biological 01:13:49.080 --> 01:13:54.760 testing laboratory without any know-how about how to do it. And they were able to source all their 01:13:54.840 --> 01:14:00.760 materials and all the necessary supplies that they needed to do it and then they got contracts 01:14:00.760 --> 01:14:05.880 from state and local governments to do it. It's really extraordinary when you think about how 01:14:06.520 --> 01:14:11.240 quickly it all came out even if they pretended like it wasn't very good and we were really behind 01:14:11.240 --> 01:14:13.560 and we should have had testing in February and we didn't. 01:14:17.240 --> 01:14:21.800 We had testing in February we'd have been testing with the the PCR test that had the 01:14:21.880 --> 01:14:25.960 primers that curled up on themselves like Kevin McCurnan was fighting against. 01:14:28.040 --> 01:14:33.240 Not that we shouldn't test with a PCR test he wouldn't fight against that because Kevin McCurnan 01:14:33.240 --> 01:14:37.400 after working on the Human Genome Project started a company called Agencourt 01:14:37.400 --> 01:14:41.240 who's one of its primary things was was HIV testing. 01:14:45.240 --> 01:14:50.680 So he definitely wouldn't say you can't use PCR to test for a virus. He's he's been using PCR 01:14:50.680 --> 01:14:56.680 to test for viruses since he was like 30 years old and he started a company with his dad and his brothers. 01:15:02.280 --> 01:15:07.400 And so here we are talking about the diagnostic tests coming out and the how long is it going to 01:15:07.400 --> 01:15:12.200 take for the development of the diagnostics and on the 5th of March they already know that they 01:15:12.200 --> 01:15:17.160 need a vaccine. They already know they need a vaccine for the world they're already bragging 01:15:17.160 --> 01:15:23.240 about the global research and surveillance infrastructure that was already in place. 01:15:25.720 --> 01:15:28.760 Some pretty bold claims already in this first 20 minutes. 01:15:29.960 --> 01:15:37.000 I mean do you have a sense on when when you'll have it just ready to roll out do you have a sense of 01:15:37.000 --> 01:15:42.040 any timing on that and you have a sense on whether the vaccine when that would be have you 01:15:42.040 --> 01:15:46.600 started testing in animals or have you the phase one time trial. Dibs timing. 01:15:46.600 --> 01:15:52.440 So so as far as the diagnostics are concerned there are large and very competent commercial 01:15:52.440 --> 01:15:58.200 concerns that are looking literally in the next month or two to be able to take to convert the 01:15:58.200 --> 01:16:04.520 current assays that are really relatively slow to execute and can you only do a small number of 01:16:04.520 --> 01:16:09.880 samples at a time to being able to do these on very robust machines that could execute up to 01:16:09.960 --> 01:16:15.640 800 tests for eight hours which is a standard work shift. So those are the kinds of approaches 01:16:15.640 --> 01:16:21.480 that the the industry has already done. I mean I mean we do HIV testing we do almost a million 01:16:21.480 --> 01:16:27.320 HIV tests a year at our laboratory up in Silver Spring and we use those kinds of instruments so 01:16:27.320 --> 01:16:33.400 they can be adapted for those kinds of other technologies. Let me let Dr. Majora talk about 01:16:33.400 --> 01:16:40.040 the point is though is if you're going to adapt a high throughput sequencing or PCR 01:16:40.840 --> 01:16:47.720 machine to doing high throughput PCR testing for sea for coronavirus with only one or two 01:16:47.720 --> 01:16:56.200 amplicons it's a very different setup in a 384 well plate than it is if that 384 well plate is 01:16:56.200 --> 01:17:03.880 supposed to take all the same DNA and all 3348 wells versus it's supposed to have different DNA 01:17:03.880 --> 01:17:11.000 and each one of those wells are every two wells and so converting these commercial platforms to 01:17:11.000 --> 01:17:17.000 being able to use to go from essentially those commercial platforms existed before the pandemic 01:17:17.000 --> 01:17:23.240 specifically to do genome screens for like you know a bunch of genetic markers that we're going 01:17:23.320 --> 01:17:27.400 to talk about tomorrow when we watch an Eric Lander video that was inspired by 01:17:28.040 --> 01:17:35.640 Mark Coolack's work today what a great show he did and it I was like 30 seconds away from watching 01:17:35.640 --> 01:17:41.400 an Eric Lander video from 2019 when I decided at the last minute to switch to this because I'm 01:17:41.400 --> 01:17:46.840 trying to keep all the people that are monitoring my my text messages and emails on their toes 01:17:47.560 --> 01:17:51.720 but tomorrow we're going to do the Eric Lander video and it's going to be just spectacular it's 01:17:51.800 --> 01:17:59.720 just great what he he continues to be so honest it's just really cool so let's keep this going 01:17:59.720 --> 01:18:04.360 sorry about that the where we are in terms of stages of development pre-clinically then into 01:18:04.360 --> 01:18:10.600 the clinic for a vaccine so if we think about vaccine development at different stages the first 01:18:10.600 --> 01:18:16.280 stage is the design and the discovery to decide what is going to be your candidate we've completed 01:18:16.360 --> 01:18:22.840 that and we have gone into small animals mice so we're looking at what the 01:18:23.560 --> 01:18:30.280 response is to that vaccine in mice and then as far as a timeline to getting into humans I 01:18:30.280 --> 01:18:35.800 wouldn't want to speculate too much on that I think the important thing to consider also is that 01:18:36.760 --> 01:18:44.440 going beyond a phase one study there's the second phase which is oftentimes looking at a larger 01:18:44.440 --> 01:18:49.880 population at the safety and the immune response but also then transitioning to see if it's 01:18:50.440 --> 01:18:57.400 effective in populations what I think the field is trying to do is position itself as a whole 01:18:57.400 --> 01:19:04.360 so that if there's a second wave during the next season in the winter that those candidates have 01:19:04.360 --> 01:19:12.440 made it through phase one studies to be ready to look at the effectiveness during the next now 01:19:12.440 --> 01:19:17.880 that's pretty curious because I know that my friend Mark Koolack has often suggested that 01:19:17.880 --> 01:19:25.400 the original plan for covid was two years before the vaccine rollout not one and that for some 01:19:25.400 --> 01:19:31.880 reason or another it was accelerated a bit and here he's he seems to be even downplaying the 01:19:31.880 --> 01:19:36.680 possibility of a second wave is even maybe not going to happen which is very different than 01:19:37.240 --> 01:19:41.880 than what a lot of other worst-case scenario people at the time were saying so that's cool season 01:19:42.600 --> 01:19:47.720 okay so let's go to Caitlin and we'll come over to Tara Caitlin it's a question slash request 01:19:48.760 --> 01:19:56.040 with describing like the vaccine can you be a little bit more broken down in terms of language 01:19:56.040 --> 01:19:59.560 about what you're talking about because you're talking about candidates which what does that mean 01:19:59.560 --> 01:20:05.400 what does it mean for a vaccine it's March 5th March 5th 2020 so that we can communicate best 01:20:05.400 --> 01:20:11.080 about what you're kind of really talking about yeah thank you so think of this as the virus my 01:20:11.160 --> 01:20:17.320 fist you know it's a sphere right and it's got little spokes coming off of it that makes it 01:20:18.040 --> 01:20:22.280 the corona when you look at it on cross-section it's got that crown look to it 01:20:23.160 --> 01:20:28.840 so almost all the vaccine candidates out there are focused on that little spoke what we call the 01:20:28.840 --> 01:20:37.000 spike the spike protein and there are different parts of the spike that mediate the attachment 01:20:37.000 --> 01:20:43.240 of the virus and the entry of the virus into our cells in our lungs so if you block that 01:20:43.240 --> 01:20:48.360 attachment if you give a vaccine that trains and educates your immune response your immune 01:20:48.360 --> 01:20:54.920 system to recognize that part of the virus that attaches to your cells and blocks it 01:20:55.560 --> 01:21:00.840 that's going to be a good vaccine so that's why everybody's focused on that so we are looking 01:21:00.840 --> 01:21:05.640 and then so what's a candidate then candidate means that you're looking at options you got 01:21:05.640 --> 01:21:11.560 your different options that's your different candidates and you look in mice or other animals 01:21:11.560 --> 01:21:15.960 other people are looking at other animals as well as as our scientists are doing 01:21:16.600 --> 01:21:25.560 within our command to see which of those options looks best in small animals and then 01:21:25.560 --> 01:21:33.560 larger animals before you go into humans as far as a platform so you have that little piece of the 01:21:33.560 --> 01:21:39.720 virus that is going to be the part that educates your immune response but you need to deliver it 01:21:39.720 --> 01:21:44.760 in something to the body you need to get it expressed in your body and there are different ways 01:21:44.760 --> 01:21:52.520 to do that you can have it on a nanoparticle basically something another sphere that kind of 01:21:52.520 --> 01:21:59.560 looks like the virus you can have it in DNA which is part of you know the same kind of DNA but it 01:21:59.560 --> 01:22:05.480 goes into our body and our cells express that the Moderna vaccine that you've probably heard about 01:22:05.480 --> 01:22:12.440 in collaboration with the NIH it's mRNA it's a different kind of thing like DNA that's the platform 01:22:12.440 --> 01:22:19.640 parts the part that expresses that candidates that we're trying to find out how good it is in 01:22:19.640 --> 01:22:26.360 this so curiously he's already selling it as not a genetic therapy it's not transfection 01:22:27.240 --> 01:22:34.200 it's expressing a protein so we already have words for that if you use DNA it's called 01:22:34.200 --> 01:22:40.760 transformation if you use RNA it's called transfection we already have names for that 01:22:42.040 --> 01:22:47.640 and yet he says that a small piece of the virus needs delivering then he says it needs expressing 01:22:48.440 --> 01:22:53.240 but he doesn't specifically say what expressing is and that is really changing 01:22:54.200 --> 01:23:00.520 a genetic signal into a protein and the genetic signal if it's DNA that change is 01:23:00.520 --> 01:23:08.760 that that operation that methodology to use DNA to create expression of a protein that is called 01:23:08.760 --> 01:23:19.640 transformation and that's usually associated with viruses like AAB because AAB will often 01:23:19.640 --> 01:23:22.600 carry DNA and then transfection 01:23:26.760 --> 01:23:34.920 is with RNA and so that is less associated with with a virus particle and it's much much more 01:23:34.920 --> 01:23:48.520 associated with lipids or electricity and electroporation of course was the way that RNA and DNA was 01:23:48.520 --> 01:23:57.240 going to get inside a cell for a company called Inovial which was incorporated and took a lot of 01:23:57.240 --> 01:24:03.960 advice from or maybe even was was somehow owned by or whatever by Robert Malone Robert Malone 01:24:03.960 --> 01:24:09.880 participated in that that was his big thing was electroporation and the reason why he gave up on 01:24:09.960 --> 01:24:17.000 this RNA as a virus as a vaccine was because he knew that it couldn't be made safe 01:24:18.200 --> 01:24:23.320 and that's why he gave up on it and let it go and then years later he tells us that he assumed 01:24:23.320 --> 01:24:26.680 that they made it safe that's why he decided to take it it's a very strange 01:24:28.760 --> 01:24:34.840 set of almost contradicting ideas that he claims to hold in his head about RNA and its safety 01:24:35.320 --> 01:24:41.800 now versus when or his his own perception of its safety back then versus 01:24:41.800 --> 01:24:46.120 at the start of the pandemic when he claims to have taken it different animals 01:24:47.080 --> 01:24:51.880 hope that helps thank you for asking that question Kate we are going to go to Tara and then we'll 01:24:51.880 --> 01:24:56.040 head back over to Phil I'll say thank you too it's about to ask something kind of related but 01:24:58.120 --> 01:25:04.120 tied to that could you talk a little bit about what your scientists are actually doing in the labs 01:25:04.840 --> 01:25:10.440 are they working with test tubes are they did they actually get samples of coronavirus from 01:25:10.440 --> 01:25:19.160 someone who was infected how did they do this happy to so so our scientists are doing a number 01:25:19.160 --> 01:25:23.880 of things right now there comes there has been receipt of the virus in one of our 01:25:23.880 --> 01:25:30.360 laboratories and they're currently culturing growing that virus so that we can have stocks 01:25:30.360 --> 01:25:37.240 available for a number of things to test products with that's they're also doing characterization 01:25:37.240 --> 01:25:43.000 of the virus to try to understand learn more of what we know about the virus and how the virus 01:25:44.040 --> 01:25:50.120 impacts are the host and our immune response to that virus the scientists and our other 01:25:50.120 --> 01:25:56.600 subordinate laboratories are yes test tubes pipettes they're dealing with mice they're they're 01:25:56.600 --> 01:26:01.880 running cell cultures and and I can let the scientists here they're doing the hands-on work 01:26:01.880 --> 01:26:08.200 talk a little bit about that one description and the laboratory that received the samples 01:26:08.200 --> 01:26:13.560 that Colonel Sam and Jackson is talking about is the US Army Medical Research Institute of 01:26:13.560 --> 01:26:19.080 Infectious Diseases at Fort Detrick but if you think of the movie outbreak and the suits that 01:26:19.080 --> 01:26:24.520 they wore and a highly contagious environment without all of the drama of the movie certainly 01:26:25.000 --> 01:26:32.840 but that capability certainly exists within military medicine and that particular laboratory 01:26:32.840 --> 01:26:39.960 is the DOD's only biosafety level four laboratory so that type of work and we're not there yet with 01:26:39.960 --> 01:26:46.200 coronavirus where we would actually bring it into containment facilities or laboratory suites to 01:26:46.200 --> 01:26:52.360 test it at higher levels we mentioned small animals that would be an advancement to a larger 01:26:53.000 --> 01:26:59.240 specimen perhaps not there yet but that's what the laboratory work looks like and I think we're 01:26:59.240 --> 01:27:06.360 actually conducting that to some degree now in BSL three conditions biosafety level two conditions 01:27:06.360 --> 01:27:12.280 but that's to get a picture of what that looks like at low-scale levels in vitro under microscopes 01:27:12.920 --> 01:27:18.280 to all the way to where we would actually begin advanced types of testing there that's where 01:27:18.280 --> 01:27:23.960 that's where we're skating through if you will so MRDC is for medical research development 01:27:23.960 --> 01:27:29.400 command is really fortunate because we have a very unique national asset as the general mentioned 01:27:29.400 --> 01:27:37.880 in our institute for biosafety level three which is current virus is required to be handled within 01:27:37.880 --> 01:27:43.080 as well as biosafety level four and so those scientists the critical asset and those scientists 01:27:43.080 --> 01:27:50.200 are actively working we have biosafety level level crimson and we also actually have some 01:27:50.200 --> 01:27:57.240 facilities with biosafety level purple so you can rest assured that that whatever we do in this 01:27:57.240 --> 01:28:02.760 laboratory nothing could possibly go wrong it's almost comical how they talk about it when you look 01:28:02.760 --> 01:28:11.000 back on it you can't help but see it it almost like they have it's almost like they want you to think 01:28:11.000 --> 01:28:19.960 that to investigate the virus as well in addition we also have the Walter Reed Army Institute of 01:28:19.960 --> 01:28:24.840 Research with our two scientists here over here who are working in biosafety level two 01:28:25.880 --> 01:28:32.120 and doing the discovery the small animal work and have some of the most brilliant minds in the 01:28:32.120 --> 01:28:40.120 world working in infectious disease research and so within that we have a very robust science and 01:28:40.120 --> 01:28:49.000 technology platform in addition we also have the capabilities to take products from the science 01:28:49.000 --> 01:28:57.240 from from the prototype level and move them into advanced development which is required in order 01:28:57.240 --> 01:29:04.600 for us to move them into manufacturing and commercialization so within MRDC as a whole we have sort of 01:29:04.680 --> 01:29:10.200 entire pipeline for developing products and just super quick follow-up where did the sample come 01:29:10.200 --> 01:29:16.680 from uh the coronavirus sample you're working on the CDC okay but it's no that would be so 01:29:16.680 --> 01:29:22.360 very identified of where the infection was was it from China you know did it come from China or 01:29:24.120 --> 01:29:30.600 it came from a U.S. patient yeah but we yeah we yeah yeah it's a homeless county man baby so let's 01:29:30.600 --> 01:29:36.360 someone get some more questions so just to clarify really quick on the rapid diagnostic 01:29:36.360 --> 01:29:41.480 that Lita asked about what what first of all you said if I was clear you said it'd be about 01:29:41.480 --> 01:29:46.760 a month or two months before you think such a diagnostic would exist you know I was saying that 01:29:46.760 --> 01:29:52.840 that that industry right now is taking their very robust platforms they have been using for a 01:29:52.840 --> 01:29:56.680 long time to do high throughput screening for other infectious diseases and are adapting those 01:29:57.240 --> 01:30:05.080 for testing for the for the SARS coronavirus too the point of care tests if they're going to be 01:30:05.080 --> 01:30:10.840 actually detecting the virus itself that becomes I mean that's a lot trickier to actually take that 01:30:10.840 --> 01:30:15.880 that kind of technology and then make it really small so I will tell you that we ourselves 01:30:16.520 --> 01:30:22.680 are not involved directly in those efforts we're becoming aware of those that are because historically 01:30:22.680 --> 01:30:32.120 we've made so many kinds of research projects along with industry to advance point of care 01:30:32.120 --> 01:30:37.720 tests largely for infections like HIV because we're heavily involved in the presence of emergency 01:30:37.720 --> 01:30:43.160 plan for AIDS relief which obviously the you know the point of care there are places that are 01:30:43.160 --> 01:30:48.200 resource constrained in Africa largely and so you really need those kinds of robust tests that 01:30:48.200 --> 01:30:54.040 require very very little skill I could probably teach my cat to one to use one that's the sort 01:30:54.040 --> 01:30:58.440 of test you want to be able to use in the field and the same mindset we use is in the in the 01:30:58.440 --> 01:31:04.280 military to be able to have those in rucksacks right so those that technology I don't want to 01:31:04.280 --> 01:31:11.960 it really feels like the same kind of kind of bullshit pitch that David Hone gave in that talk 01:31:12.040 --> 01:31:19.640 that Mark Koolak has featured on his program a few times where he says that well what I wanted 01:31:19.640 --> 01:31:26.520 was the cart from Cuba Gooding Jr. in the movie and then his boss said no I want an arm band on 01:31:26.520 --> 01:31:31.560 one arm that detects the pathogen and an arm band on the other arm that makes the vaccine and so 01:31:31.560 --> 01:31:38.920 he's talking about carrying point of point of care tests in a backpack and all this other stuff so 01:31:38.920 --> 01:31:46.840 again just like the last discussion that we were talking about with Duke University and the person 01:31:47.400 --> 01:31:53.160 talking about how their their vaccine platform would be able to be universalized by adding more 01:31:55.560 --> 01:32:00.600 antibody targets to the outside of their platform and was talking hypothetically about how useful 01:32:00.600 --> 01:32:06.680 their platform could be what they're thinking is how they get grant money they're saying if their 01:32:06.680 --> 01:32:11.560 platform works like they imagine it will then you should give us money to develop it because the 01:32:11.560 --> 01:32:18.840 end when this perfect platform is developed it will be able to be a universal vaccine here he is 01:32:18.840 --> 01:32:24.280 again talking about you know little tiny tests that are really really accurate and when we get it 01:32:24.280 --> 01:32:30.600 right this is what they will be there are so many hypothetical you know if it works it would be great 01:32:30.600 --> 01:32:36.280 if we could have this if it works we greatly could have this and there they haven't managed 01:32:36.280 --> 01:32:43.000 to get any of these things to actually work they only work in the in the theoretical version on 01:32:43.000 --> 01:32:51.400 paper or in the future and what's crazy about Mark's video from today and the video that we will 01:32:51.400 --> 01:32:57.160 watch tomorrow what it will reveal is that when they told us that they had sequenced the human genome 01:32:57.160 --> 01:33:01.160 and that they spiked that football they hadn't come even anywhere near 01:33:03.240 --> 01:33:10.200 even close into the same stadium or even playing the same sport as sequencing the whole genome and 01:33:10.200 --> 01:33:18.520 funny thing is Eric Landers fine with admitting that and so they have so grossly overplayed their 01:33:18.520 --> 01:33:23.960 hand with regards to trying to convince us how much fidelity of understanding they have with 01:33:23.960 --> 01:33:30.040 so much of this complexity and they just don't have it and it's interesting because in the 01:33:30.040 --> 01:33:35.320 military space because they have these very specific applications that they're shooting for 01:33:36.200 --> 01:33:42.200 you know the superpower suits and the super soldiers and also their crap then the theoretical goal 01:33:44.600 --> 01:33:51.160 is revealed in the cartoon and it's it's almost easier in some ways in the military sense to 01:33:51.160 --> 01:33:59.320 understand if the if the DARPA grant says we want an armband on one side that detects RNA and the 01:33:59.320 --> 01:34:05.160 armband on the other side to make a vaccine for the RNA that's a grant proposal that lots of 01:34:06.280 --> 01:34:10.040 of spin-up technology companies could in theory write a grant to answer 01:34:11.960 --> 01:34:17.000 and not only that but you could imagine how one might write a grant to answer that call 01:34:17.000 --> 01:34:22.440 we have the you know the latest spandex and we're gonna we're gonna we're gonna cooperate with 01:34:22.440 --> 01:34:29.000 apple to get the sensory technology or whatever you can imagine that it's a little harder to imagine 01:34:29.800 --> 01:34:36.360 the grant applications that come in when a grant call for a particular gene in relation to a particular 01:34:36.360 --> 01:34:40.600 disease describes a animal model and they asks for a grant call 01:34:40.760 --> 01:34:48.680 DARPA asks for grant calls like we want to have a point-of-care test that can be carried in a 01:34:48.680 --> 01:34:53.720 backpack and used at all temperatures and doesn't require blood 01:34:57.800 --> 01:35:02.600 DARPA has grants that say that we want a cart that will make a vaccine DARPA has a grant that 01:35:02.600 --> 01:35:08.760 says this kind of stuff so when these guys are talking and when you hear academic scientists 01:35:08.760 --> 01:35:14.680 talking about especially infectious disease and responding to them you can hear the grant calls 01:35:14.680 --> 01:35:21.160 in their explanations because if it's explanations about about getting money for funding to respond 01:35:21.160 --> 01:35:26.840 to infectious diseases you're almost always going to hear about antibodies and you're almost always 01:35:26.840 --> 01:35:32.760 going to hear about vaccines it's extraordinary when you listen to them now a few years later 01:35:32.760 --> 01:35:37.400 leave you the impression that that's going to be available anytime soon clearly what we're 01:35:37.400 --> 01:35:43.960 focused on is the more complex laboratories so that we don't have state and local departments 01:35:43.960 --> 01:35:48.120 of public health that are simply overwhelmed with individuals that want to get tested so you had 01:35:48.120 --> 01:35:52.680 that so in those situations where the patients are coming to a central so they don't think it's 01:35:52.680 --> 01:35:59.000 going to blow over in march 5th they just think that this is just starting there is a whole 01:35:59.000 --> 01:36:05.560 industry of testing that is spinning up now that they expect to be relevant for the foreseeable 01:36:05.560 --> 01:36:14.360 future notice this this is not panic this is just state and facts we're about to 01:36:15.160 --> 01:36:20.840 you know roll out a new thing or two or a hundred well place they're having the high 01:36:20.840 --> 01:36:25.720 throughput test makes sense if now you're talking about distributing people that want to go detect 01:36:25.720 --> 01:36:30.200 in less dense populations that's where the rapid or point of care test will be important 01:36:31.160 --> 01:36:35.400 so you know you preparing yourselves for the possibility that the military is going to have 01:36:35.400 --> 01:36:39.880 to test military patients i mean it's large a very large community and when you think about 01:36:39.880 --> 01:36:43.400 all the people around the world you know it's unlikely that the civilian capacity would 01:36:43.400 --> 01:36:48.200 necessarily be there for one as fast as they need it absolutely what does that look like i mean 01:36:48.200 --> 01:36:52.120 like right now my understanding is there's only a small number of kits that have been distributed 01:36:52.120 --> 01:36:57.000 to a very specialized about a dozen or so labs so what does it what does that look like when you're 01:36:57.000 --> 01:37:01.320 talking about getting ready for testing over a million people maybe potentially 01:37:01.320 --> 01:37:06.920 in the u.s military so the goal and there's multiple approaches so the goal is just increased 01:37:06.920 --> 01:37:13.720 capacity and as dr michael mentioned um one way to do that is to develop these high throughput 01:37:13.720 --> 01:37:19.960 assays and place them in regional critically strategic regional areas so that we can so where 01:37:19.960 --> 01:37:25.080 did all these private testing companies come from if the whole thing was a military coordinated 01:37:25.160 --> 01:37:30.440 exercise or private testing companies all around the united states that we're up and operating 01:37:30.440 --> 01:37:37.800 by april this is now march what are we talking about here did they just put one ads out in major 01:37:37.800 --> 01:37:42.120 cities in the united states looking for managers for biotech labs 01:37:48.120 --> 01:37:54.600 this is extraordinary increase the throughput of the diagnosis another approach as was mentioned 01:37:54.600 --> 01:37:59.400 before with the point of care is actually reaching further out into the environment to 01:37:59.400 --> 01:38:06.440 be able to test and rapidly as an initial screen for folks to kind of help understand what the 01:38:06.440 --> 01:38:12.600 epidemiology is and so there's multiple approaches within the army across the dvd and in across the 01:38:12.600 --> 01:38:17.880 u.s government as well certainly critical and all each one of those approaches is our industry 01:38:17.880 --> 01:38:23.880 partners in this to be able to take a product and develop it and commercialize it so we are 01:38:23.880 --> 01:38:29.320 working with a number of partners and providing the support within the laboratories to help 01:38:29.320 --> 01:38:33.320 develop the escape okay so let's go to lucas and then we'll hit courtney and back and the 01:38:33.320 --> 01:38:38.120 lucas tolinson fox news in your modeling how many u.s military service members do you think 01:38:38.120 --> 01:38:47.240 are going to contract the quantifiers that that'd be speculative sir uh not uh i i don't think we 01:38:47.880 --> 01:38:52.600 have done any estimates on that uh it would depend on the spread certainly uh the way it's 01:38:52.600 --> 01:38:59.240 progressing now but uh right now unless uh well we uh we're i i think that's the general 100 01:38:59.240 --> 01:39:03.720 percent right we we don't have any data um right now i didn't but where we're beginning to work 01:39:03.720 --> 01:39:08.600 with partners that dr major can get a little bit more into that there are lots of people now that 01:39:08.600 --> 01:39:15.160 have gotten pretty sophisticated by trying to model infectious disease outbreaks um you know 01:39:15.160 --> 01:39:19.320 regrettably because one seems to come up you know every year or so we're getting very good at this 01:39:19.800 --> 01:39:24.680 um the problem with with the models it's as only as good as as the data that you have that would 01:39:24.680 --> 01:39:30.120 build into it right so i would just say that that that we're beginning so i would just say that if 01:39:30.120 --> 01:39:38.120 they created a mass casualty event if they created a mass casualty event in new york city and then 01:39:38.120 --> 01:39:44.040 extrapolated from that very bad model where the spread would be in a few months you could get a 01:39:44.120 --> 01:39:51.960 pretty worst case scenario going in fact if you look at the slope that you see in the first four 01:39:51.960 --> 01:39:58.120 weeks or three weeks of the major bomb-like event that jessica hockett has worked so hard at 01:39:58.120 --> 01:40:03.880 characterizing you're going to see a slope that if it's projected into the future at that angle 01:40:04.680 --> 01:40:11.320 we're talking about billions dead it's really extraordinary and of course that's exactly what 01:40:11.320 --> 01:40:18.600 was done in those weeks while we were all told to stay at home and just shelter in place and watch 01:40:18.600 --> 01:40:25.640 tv they showed us that curve they showed us that slope and they said holy crap i don't know what's 01:40:25.640 --> 01:40:36.120 going on but this looks pretty and serious to set ourselves up with really good modeling groups 01:40:36.120 --> 01:40:40.520 to be able to ask questions in areas of the world where it's the virus is already spreading 01:40:41.480 --> 01:40:46.200 and we have good epidemiology data that would allow us to inform those models that's going to 01:40:46.200 --> 01:40:51.720 give us some prediction but i can tell you during the Ebola outbreak i literally sat in a WHO meeting 01:40:51.720 --> 01:40:56.840 and had one modeler talk about when the epidemic in liberia was going to peak and 01:40:56.840 --> 01:41:01.320 essentially i looked at the numbers i said you're basically saying that it's only going to peak 01:41:01.320 --> 01:41:05.720 when every single human being in liberia is infected and he basically just shrugged so you 01:41:05.720 --> 01:41:09.640 just need to be careful that these models sometimes can really look bombastic 01:41:10.600 --> 01:41:12.760 and they're always good as the data that initially goes into them 01:41:13.320 --> 01:41:19.320 one thing i can say is that the current assay which is a test i think the throughput is 01:41:19.880 --> 01:41:25.960 around 60 patients every eight hours so when we're looking at volumes or what we are trying to 01:41:25.960 --> 01:41:33.400 develop in the area of detection our goal is anywhere from 275 to 500 every eight hours 01:41:33.480 --> 01:41:37.960 so if we can increase the throughput for this when you're talking about a large number 01:41:38.760 --> 01:41:44.280 that would be affected take the military for example we're certainly developing things 01:41:44.280 --> 01:41:48.280 in case that were to happen that goes for any any population okay so i want to go 01:41:52.840 --> 01:41:56.760 i i would just add so i think general tally is correct in that 01:41:57.160 --> 01:42:02.440 um any kind of numbers specific numbers you throw out there is speculative 01:42:02.440 --> 01:42:12.120 however we have epidemiologists at our institute working with others modelers who do this all the 01:42:12.120 --> 01:42:19.800 time in the defense threats reduction agency ditra who provide responses to the requests of all 01:42:19.800 --> 01:42:24.600 the different geographic combatant commands and we have been working with them for the past few 01:42:24.680 --> 01:42:30.040 weeks initially based on assumptions but now more importantly on real life data 01:42:30.760 --> 01:42:37.640 so we're trying to refine those models better based on the data that we feed into them so this 01:42:37.640 --> 01:42:42.760 is something that we're working on but i wouldn't speculate and give you a specific number 01:42:43.720 --> 01:42:48.280 what is the earliest that a vaccine would be ready for a u.s military service member go 01:42:49.080 --> 01:42:58.200 go go so again it depends on what you're talking about in terms of ready so as i said there's 01:42:59.800 --> 01:43:04.360 we when we go into phase one clinical trials when that we have done in the past 01:43:05.160 --> 01:43:10.920 we the volunteers who are involved in those trials are a mix of civilian and active duty 01:43:11.000 --> 01:43:19.880 populations and then as you go further on there is in discussions with our partners 01:43:19.880 --> 01:43:24.680 and our military treatment facilities the potential to have them involved in clinical trials 01:43:25.240 --> 01:43:30.840 as far as licensure whether you're talking about emergency use authorization or full licensure 01:43:32.440 --> 01:43:38.200 if you if you talk about vaccines in general i think dr fauci's remarks that he's 01:43:39.000 --> 01:43:44.680 stated over and over again are really the the benchmark that we should use as the most accurate 01:43:44.680 --> 01:43:50.760 as being the earliest earliest earliest probably 12 to 18 months to get something out to the 01:43:50.760 --> 01:43:55.720 populations and that would be whether it be civilian or military population and just recognize that 01:43:55.720 --> 01:44:01.480 part of that hesitation i mean the science can go very quickly but so that's closer to Mark's 01:44:01.480 --> 01:44:08.520 original estimate right 12 to 18 months 18 months would have put us in the middle of 2021 01:44:08.520 --> 01:44:17.320 or or late 2021 and that's so they got it out really fast you at first don't want to do harm 01:44:17.320 --> 01:44:22.520 right and you know there's obviously there are you know vaccines can cause harm and they provide 01:44:22.520 --> 01:44:28.680 benefit so that mixture is something you always have to look at and so so part of the hesitation 01:44:28.760 --> 01:44:33.160 to say all we can get a vaccine quickly is you need to make sure that it's really safe if you 01:44:33.160 --> 01:44:37.080 test the vaccine in a thousand people but one in ten thousand people is going to have something 01:44:37.080 --> 01:44:41.480 terrible that happens until you get to those numbers you may end up doing mass vaccination 01:44:41.480 --> 01:44:45.800 campaigns with a vaccine that could cause a significant amount of problems so you so that's 01:44:45.800 --> 01:44:52.680 pretty funny because also we have video of of tony fauci saying that 12 years ago about an HIV 01:44:52.680 --> 01:44:57.720 vaccine and and not rushing it out because you don't want to have it rushed out and then realize 01:44:57.800 --> 01:45:02.040 that thousands of people are going to get hurt by it that's what he's suggesting here too 01:45:02.040 --> 01:45:06.120 and i think most of the people who are watching this show for a while now are pretty much come 01:45:06.120 --> 01:45:11.560 to the conclusion that that's what's happened that everybody that we know that has taken a couple 01:45:11.560 --> 01:45:16.920 of these shots is damaged in some way even if they just get sick all the time or their kids have 01:45:16.920 --> 01:45:23.800 strep throat four or five times a school year or you're 22 and you have your third bout of of 01:45:24.680 --> 01:45:29.640 pneumonia in the last two years this needs to be a constant reassessment of the risk 01:45:30.120 --> 01:45:34.760 and the benefit um the other thing i would tell you and this is so a really good benchmark 01:45:34.760 --> 01:45:39.160 we were the first people that tested the vaccine that eventually got licensed by 01:45:39.160 --> 01:45:45.880 murk to to um for for Ebola okay that vaccine was first tested by the Walter Reed Army Institute 01:45:45.880 --> 01:45:52.040 of Research and so that's a that's a great thing i heard that was a pretty nasty vaccine wow 01:45:52.920 --> 01:45:58.440 five years later it was approved by they tested the vaccine on veterans then or they tested the 01:45:58.440 --> 01:46:05.560 vaccine on on soldiers what the hell the u.s. FDA in the meantime a half a million souls were 01:46:05.560 --> 01:46:10.440 vaccinated that largely in africa during especially during the outbreak in the democratic republic 01:46:10.440 --> 01:46:16.200 of Congo so wow you know again that was a risk benefit assessment the the leadership in the drc 01:46:16.200 --> 01:46:24.040 said okay we know it's not approved yet by european medicines or by the u.s. FDA but we have a 01:46:24.040 --> 01:46:28.840 terrible outbreak of Ebola which is highly fatal and so decisions were made to use that under 01:46:29.640 --> 01:46:34.840 emergency use authorizations and so you know there's always that kind of debate but just i think 01:46:34.840 --> 01:46:40.120 that's a good benchmark i didn't know they could give an EUA to a vaccine and then roll it out in 01:46:40.120 --> 01:46:51.160 another country that's wow he just said that they decided to roll it out with an EUA because you 01:46:51.160 --> 01:47:00.520 know i mean it was a real real emergency over there that's a pretty good way it's like i'm just 01:47:00.520 --> 01:47:06.680 trying to think of a better way to roll out a bio weapon attack than that so our CDC approved 01:47:06.680 --> 01:47:12.680 this vaccine for your country you better take it for vaccines let me also say that 01:47:13.400 --> 01:47:17.480 we haven't really talked much about this we are beginning to make other countermeasures 01:47:18.680 --> 01:47:23.160 one of those are monoclonal antibodies so antibodies are part of our immune response you 01:47:23.160 --> 01:47:28.920 you know it's part of the way the body tries to push infections back but we can actually make 01:47:28.920 --> 01:47:35.080 these in test tubes and these are becoming a much more common tool that are being used 01:47:35.160 --> 01:47:39.480 especially in the fields of oncology but increasingly in infectious disease so instead of actually 01:47:39.480 --> 01:47:45.080 waiting for a vaccine to be made giving you that vaccine and waiting the time it takes for it to 01:47:45.080 --> 01:47:49.640 develop the immune response you can give with these kinds of reagents you can give almost 01:47:49.640 --> 01:47:55.560 immediate protection so we're literally in the process now of beginning to take those he keeps 01:47:55.560 --> 01:48:01.560 saying literally when he doesn't need to say it and i want to smack him first baby steps as well as 01:48:01.640 --> 01:48:07.000 looking at at we talked about one drug the general talked about that one drug that's 01:48:07.000 --> 01:48:11.560 currently being repurposed and has been looked at for Ebola and now is being looked at for 01:48:11.560 --> 01:48:15.800 it's remdesivir baby there are other small molecules because remdesivir 01:48:15.800 --> 01:48:20.120 talked about that one drug that's currently being repurposed that one drug that's currently 01:48:20.120 --> 01:48:25.960 be repurposed that was used for Ebola is remdesivir so they're talking about remdesivir on March 5th 01:48:25.960 --> 01:48:31.560 they're talking about point of care testing on March 5th they're talking about PCR testing 01:48:31.560 --> 01:48:37.240 they're talking about lateral flow testing they're talking about seroprevalence testing and they're 01:48:37.240 --> 01:48:43.080 talking about vaccine candidates on March 5th 2020 they already know they're going to need all 01:48:43.080 --> 01:48:47.400 this stuff they're not sure there'll be a second wave next winter maybe and it's been looked at 01:48:47.400 --> 01:48:52.760 for Ebola and now it's been looked at for for CoV-2 but there are other small molecules that could 01:48:52.840 --> 01:48:59.720 be discovered and one capability that we have at our institute is every malaria drug that's 01:48:59.720 --> 01:49:03.400 ever been discovered it's at some level gone through the Walter Reed Army Institute of Research 01:49:03.400 --> 01:49:08.520 but we have a really good drug discovery program and so we're looking for other kinds of drugs 01:49:08.520 --> 01:49:14.360 that might be lead candidates in partnerships with the pharmaceutical industry that we could 01:49:14.360 --> 01:49:22.680 bring those to bear so vaccines monoclonal antibodies and small molecules drugs that could be brought 01:49:22.680 --> 01:49:31.080 to bear so we don't have one one theme in play I'm not I'm not so I'm noticing this that small 01:49:31.080 --> 01:49:37.960 molecules are somehow being considered different than drugs and I wonder how or why they did that 01:49:37.960 --> 01:49:44.120 I bet it has something to do with IP or it has something to do with regulatory structures and 01:49:44.120 --> 01:49:51.560 trying to avoid the regulations of biologics or trying to avoid the regulations of certain kinds 01:49:51.640 --> 01:49:56.760 of pharmaceuticals by calling them small molecules I'm I'm wondering 01:50:02.040 --> 01:50:06.600 Hey we have actually a number of things in play and all these are being coordinated very closely 01:50:06.600 --> 01:50:12.680 with our partners either in government or in academia or in industry so thank you sir I know 01:50:12.680 --> 01:50:16.040 I want to try to get a little bit more questions out there so Courtney will go to you 01:50:16.680 --> 01:50:22.280 I want to ask a couple of clarification so when you're saying that there's testing going on in 01:50:22.280 --> 01:50:26.840 my my Dr. Majard you mean you're not saying that they're being injected with the coronavirus and 01:50:26.840 --> 01:50:32.120 that right okay I just wanted to be sure of that just just injected with the vaccine candidates 01:50:32.120 --> 01:50:40.520 those options they have to see how the immune response yeah to see how antibody responses look 01:50:40.520 --> 01:50:44.920 they're not going to look at anything else they're looking for a robust antibody response that's it 01:50:44.920 --> 01:50:48.520 to see how it responds to the vaccine not the virus okay good I just wanted to be sure 01:50:48.520 --> 01:50:54.600 about that and then I was a little unclear Dr. Michael when you were talking about you were 01:50:54.600 --> 01:50:59.320 talking about potentially rolling something out the next time that the next season which I would 01:50:59.320 --> 01:51:03.240 assume would be fall winter or maybe it was you Dr. Majard forgive me yeah the next season but I 01:51:03.240 --> 01:51:07.720 don't quite understand what that was okay so you know that's a really important question too um 01:51:07.720 --> 01:51:12.680 was it was our third the third one was just about the production okay yeah I think you kind of answered 01:51:12.680 --> 01:51:17.400 the other one so 50 those that'd be great so so this is a respiratory virus and they're they 01:51:17.400 --> 01:51:22.280 always give us trouble you know during cold weather for obvious reasons we're all inside and you know 01:51:22.280 --> 01:51:29.000 windows are closed etc so so we typically call that the influenza or the flu season our expectations 01:51:29.000 --> 01:51:33.480 that this virus like every respiratory virus is going to be in less troublesome for us as the 01:51:33.480 --> 01:51:38.760 weather warms up and that's going to be true across the globe but our experience and most of our 01:51:38.760 --> 01:51:43.720 experience comes from influenza like which is sort of the you know the unfortunately the king of 01:51:43.720 --> 01:51:50.040 respiratory virus but we know a lot about that and our experience there is that every flu season 01:51:50.040 --> 01:51:55.000 equals you know when the weather gets cold again this is when these viruses tend to come back 01:51:55.000 --> 01:52:00.040 so this is why it's really important to understand that a lot of what we're doing now is really 01:52:00.040 --> 01:52:05.080 getting ourselves ready for what we're calling the second wave of this we hope that that doesn't 01:52:05.080 --> 01:52:13.160 happen if you remember SARS SARS came and went very quickly and you know I really hope that 01:52:13.160 --> 01:52:19.240 happens again but we we can't count on that we have to be ready is that that even if this 01:52:19.240 --> 01:52:24.760 epidemic begins to wane we have to be ready for the worst case scenario we have to be ready for 01:52:24.760 --> 01:52:29.720 next next winter when it may come back again I'm sorry I'm still don't understand what it was 01:52:29.720 --> 01:52:34.200 that you were hoping to roll out with the next wave so so we're saying that as we begin to develop 01:52:34.200 --> 01:52:41.480 any of these countermeasures we're talking about monoclonal antibodies drugs vaccines that even 01:52:41.480 --> 01:52:47.000 if this disease abates over the next few months we're pretty concerned that it will come back and 01:52:47.000 --> 01:52:53.240 it may come back you know again in the next flu season if that's the case then in the meantime 01:52:53.240 --> 01:52:57.960 we've been working steadily on these countermeasures so that they'll be ready if there's a next time 01:52:58.520 --> 01:53:04.280 thank you so let's see it current thank you I also just have a couple clarification so it's like 01:53:04.280 --> 01:53:10.120 this will go quick but following up with her just to reiterate so you're testing in small animals 01:53:10.120 --> 01:53:16.360 mice now you're testing the candidate and then you had said something about the second phase was 01:53:16.360 --> 01:53:21.720 looking at large populations of mice would that be with I mean large populations of mice or would 01:53:21.720 --> 01:53:27.400 that be of something else that you said that I'm thinking about this next phase in the winter 01:53:27.400 --> 01:53:33.080 I'm not quite sure what's going on so I'm just going to break it down again in terms of what are 01:53:33.080 --> 01:53:41.560 the general phases of vaccine development first you decide down at the end so they did a lot of 01:53:41.560 --> 01:53:47.880 messaging about this in March and April they used Fauci to do it and Berks to do it and Redfield to 01:53:47.880 --> 01:53:54.360 do it and Bill Gates to do it and they had lots of different little diagrams to show how you know 01:53:54.440 --> 01:54:00.040 phase 1 and phase 2 could overlap in time and then we would accelerate everything and this is what 01:54:00.040 --> 01:54:03.000 so he's already starting with that basic mythology right here. 01:54:03.000 --> 01:54:12.200 Tomic level what your vaccine is going to be and then you get have your best guess and you have 01:54:12.200 --> 01:54:17.560 a few different options as to what that will be then you test all those different options in mice 01:54:18.440 --> 01:54:25.880 meaning testing give them the vaccine and see what kind of immune response they have then typically 01:54:25.880 --> 01:54:35.080 you go into larger animals like monkeys right that's typically the case whether we this is a new 01:54:35.080 --> 01:54:43.480 virus we don't know which one of these animals is the most relevant one to humans you know mice 01:54:43.480 --> 01:54:51.560 or mice mice are not humans right monkeys may be closer to humans and then you go into humans 01:54:51.560 --> 01:54:58.120 and when you go into humans in that first phase you're just again looking at the safety of your 01:54:58.120 --> 01:55:05.640 vaccine and the immune response you're not looking at if it's effective again to protect you from 01:55:05.640 --> 01:55:16.920 the virus the next phase is where you look at larger numbers of people for safety and immune 01:55:16.920 --> 01:55:22.760 response again because the first phase in humans is just a few dozen people now we're talking hundreds 01:55:22.760 --> 01:55:32.600 to thousands and you start looking at is it protecting against infection and you need to have 01:55:33.160 --> 01:55:38.440 large numbers of infections going on to be able to know whether or not it's protecting 01:55:38.440 --> 01:55:46.520 against that so that's why we anticipate potentially if there's a second wave we got to be ready 01:55:47.080 --> 01:55:51.560 make it all the way through those first studies in the animals and the safety and the immune 01:55:51.560 --> 01:55:57.800 response so actually he reminds me of Raymond we're ready in position and ready to go if this 01:55:57.800 --> 01:56:01.640 comes back and there are a bunch of infections so we can know is it protecting 01:56:01.640 --> 01:56:06.600 okay so you're planning to be of that second phase of humans by next winter just that's where 01:56:06.600 --> 01:56:10.280 you are okay just wondering if there's anything I wanted to clarify as you said you've had a 01:56:10.280 --> 01:56:17.080 candidate that was complimentary but not duplicative what exactly is the candidate I know you talked 01:56:17.080 --> 01:56:23.720 about the spokes are you you two focusing on the spoke of the back of the virus yes but that's 01:56:23.800 --> 01:56:28.280 just what NIH is also working on so everybody's working on the spoke right now just different 01:56:28.280 --> 01:56:35.640 different ways different parts of the of the spoke or different versions of it and then different 01:56:35.640 --> 01:56:44.360 ways now that's and that is interesting because actually if the messaging had already been sharp 01:56:44.360 --> 01:56:52.040 enough he would have corrected her but it's actually not sharp enough yet in this in this video and he 01:56:52.840 --> 01:56:58.840 rather than correcting her goes along with it to get the message across which is actually what you 01:56:58.840 --> 01:57:03.560 would do if you were trying to communicate to a small group of people rather than the entire 01:57:03.560 --> 01:57:14.520 nation but that's fine it's very cool to see I I would bet dollars to donuts that there isn't a 01:57:14.520 --> 01:57:22.280 person in the world right now who isn't at least sufficiently brainwashed that if somebody 01:57:22.280 --> 01:57:26.760 made the mistake that that blonde lady made in talking about the coronavirus that they would correct 01:57:26.760 --> 01:57:32.520 them every teacher at my kid's school would correct me if I said yeah but the spokes of the 01:57:32.520 --> 01:57:39.400 coronavirus are what they made the vaccine from I think you mean spikes so this is pretty impressive 01:57:40.280 --> 01:57:49.560 to express it so different parts of the of the spoke or different versions of it and then 01:57:49.560 --> 01:57:54.840 different ways to express it see so he's already teaching everybody that who this isn't going to 01:57:54.840 --> 01:58:01.320 be a typical vaccine anymore but he's not actually saying that he's almost implying that other 01:58:01.320 --> 01:58:08.040 vaccines do the same thing they express it no no no no he's preparing everybody to understand 01:58:08.120 --> 01:58:12.840 that the methodology is wholly different and he's not calling it a transfection even though 01:58:12.840 --> 01:58:22.360 that's really what he means when he says express it's extraordinary so as I said there's different 01:58:22.360 --> 01:58:28.040 ways so there's a DNA platform where you can express it there's the mRNA that Moderna is doing 01:58:28.040 --> 01:58:35.000 with the NIH there are just using the protein itself there it's using it putting it on a nanoparticle 01:58:35.800 --> 01:58:40.760 protein the University of washing different versions of the vaccine and different ways 01:58:40.760 --> 01:58:44.680 to present it actually there was a guy at the University of Pittsburgh who was working on 01:58:44.680 --> 01:58:51.400 putting the spike protein on the outside of the measles virus I shit you not yes to the immune 01:58:51.400 --> 01:58:56.440 system okay so I know we're right 10 after right now so we'll hit Haley we're probably gonna wrap 01:58:56.440 --> 01:59:02.280 it up sir if you get so thank you and thank you all for doing this one question for you general 01:59:02.360 --> 01:59:08.600 tally last year in the fall for due trick the research institute had to pause testing for some 01:59:08.600 --> 01:59:14.200 safety concerns can you go into what has been done since then to sort of make that a non-issue 01:59:14.920 --> 01:59:20.040 and then it's also I know that rare has gone over you said different SARS and the different 01:59:20.040 --> 01:59:25.240 strains of this what makes this different from the previous strains that you've been looking at 01:59:25.240 --> 01:59:28.680 and how have you kind of noticed the differences and and how that will affect the vaccine that 01:59:28.680 --> 01:59:35.880 you're developing yeah absolutely I appreciate the question yes so United States Army Medical 01:59:35.880 --> 01:59:42.280 Research Institute of Infectious Diseases and that's the the BSL for biosafety level four lab 01:59:42.280 --> 01:59:51.240 that I that I mentioned but on the 18th of July of 2019 they were issued a cease and desist order 01:59:51.240 --> 02:00:01.480 by the CDC violations because of improper practices all resulting from a number of structural defects 02:00:01.480 --> 02:00:07.960 they develop workarounds that just just were not safe there was never any any danger of risk to 02:00:07.960 --> 02:00:16.360 the community or or breaking the containment which is what the labs are for since then proud to say 02:00:17.160 --> 02:00:24.120 worked very hard to come back and meet CDC regulatory standards the CDC came back for a 02:00:24.120 --> 02:00:32.040 reinspection after a about a 90 day plan of action in milestones very aggressively went after that 02:00:32.600 --> 02:00:41.400 and the CDC restored the laboratory to a limited operational capability limited in that the same 02:00:41.400 --> 02:00:49.880 volume that the laboratory had been become accustomed to through putting much much smaller levels 02:00:49.880 --> 02:00:56.840 and then certain types of testing as I mentioned BSL for being the highest type biosafety laboratory 02:00:56.840 --> 02:01:04.920 for being the highest level not to that level but probably a a smaller level or a level just shy 02:01:04.920 --> 02:01:10.520 of that where the the most dangerous procedures weren't being done this is what this was in it 02:01:10.520 --> 02:01:16.840 yeah I didn't see a Bavari after he left didn't he go like work for for the maker of Remdesivir 02:01:16.840 --> 02:01:21.880 like didn't he go alert for Gulad I don't know he will stand up of capabilities after being down 02:01:21.880 --> 02:01:33.000 for so long the CDC came back two weeks ago first two weeks actually three weeks ago now in February 02:01:33.000 --> 02:01:39.320 came back for a second inspection this inspection was to allow even more capabilities more capacity 02:01:39.320 --> 02:01:45.720 to be performed again proud to say night and day difference according to the CDC and we were 02:01:45.720 --> 02:01:53.160 issued a letter to restore even higher level capabilities that letter was issued to us just 02:01:53.160 --> 02:01:59.880 this past Friday and so with respect to coronavirus and coronavirus is not considered 02:02:00.440 --> 02:02:08.840 a a safety level type of type of virus that that that falls into the same category some of the 02:02:08.840 --> 02:02:15.880 other higher types so we have full authorization to perform at the highest levels of scientific 02:02:15.880 --> 02:02:24.120 capacity at the laboratory for coronavirus other types of diseases that might meet some 02:02:24.120 --> 02:02:31.800 of the CDC's criteria still having a gradual return to full operations but with coronavirus 02:02:32.520 --> 02:02:38.440 we're going to be able to conduct laboratory research at the highest levels at the laboratory 02:02:38.440 --> 02:02:44.760 and can perform so that's kind of where we are real proud it's been a work in progress 02:02:45.800 --> 02:02:49.640 we took the advantage of the operational pause if you will to to really 02:02:50.440 --> 02:02:56.200 refine our standard operating procedures and frankly the complete culture has changed at that 02:02:56.200 --> 02:03:04.840 institution and they're they're back and certainly with coronavirus it's amazing to watch the entire 02:03:04.920 --> 02:03:09.640 enterprise mobilize the way they have thank you 02:03:12.760 --> 02:03:18.920 regarding your second question about how this virus differs from others and what we've learned 02:03:20.200 --> 02:03:28.280 probably everybody's familiar now of some of the that there are seven human coronaviruses that we 02:03:28.280 --> 02:03:36.200 know of and that they highly pathogenic ones the ones that tend to kill are SARS-1 02:03:38.040 --> 02:03:44.760 Middle East respiratory syndrome coronavirus and then the current coronavirus and so we have been 02:03:44.760 --> 02:03:53.480 working on those other very more dangerous and deadly viruses like MERS and the first SARS 02:03:54.280 --> 02:04:03.640 what we've learned is really at the very basic atomic level when I mentioned that we first look 02:04:03.640 --> 02:04:10.680 at the atomic level of these spokes these spikes that's where we've been focusing on because that's 02:04:10.680 --> 02:04:19.400 the kind that's where the differences matter the most in terms of what kind of immune response you 02:04:19.480 --> 02:04:28.120 get to it how efficiently it attaches to the cells in your lung and one of our chief scientists 02:04:28.120 --> 02:04:34.840 Dr. Gordon Joyce has been doing a lot of the work on that in determining the structures in 02:04:34.840 --> 02:04:40.600 collaboration again with our partners at the NIH National Institutes of Health the Vaccine 02:04:40.600 --> 02:04:45.880 Research Center so Dr. Joyce myself we both came from the Vaccine Research Center working with 02:04:45.880 --> 02:04:51.080 Dr. Graham and Dr. Kismekia Corbett under Dr. John Mascola and then one of the other 02:04:51.080 --> 02:04:56.280 structures that came out is Dr. Jason McLennan at the University of Texas at Austin we've all 02:04:56.280 --> 02:05:01.000 this should give you an idea also how this is a very tight knit family we're kind of spread 02:05:01.000 --> 02:05:06.760 across different centers but we talk to each other all the time because we have that very close 02:05:06.760 --> 02:05:15.640 public health and scientific community so there are similarities between this virus and 02:05:15.640 --> 02:05:19.960 some of these other viruses but there are obviously very key differences between 02:05:20.600 --> 02:05:30.920 MERS and this SARS-CoV-2 there's about 50% difference in the sequence with SARS-1 there's 02:05:30.920 --> 02:05:37.880 about 20% difference but that that 20% matters obviously quite a bit and so that's the kind of 02:05:39.080 --> 02:05:43.960 studying that we've been doing when we first got those sequences and the world got those 02:05:43.960 --> 02:05:49.880 sequences back on January 10th we started looking down at the atomic level as to how they differ 02:05:50.760 --> 02:05:55.240 and so please in general I know we've been going for a little bit so I want to be able to wrap this 02:05:55.240 --> 02:05:59.000 up sir we're going to have folks standing by to do the follow-on questions but sir if you want 02:05:59.000 --> 02:06:07.400 to do closing remarks well since there will be a vaccine already in time for this cycle of 02:06:07.400 --> 02:06:12.600 coronavirus could you please give your best advice to the the force and the public in general 02:06:13.160 --> 02:06:15.240 about how to kind of ride this out for now 02:06:18.440 --> 02:06:24.600 well I you know it's really is I mean we are literally living in influenza season people are 02:06:24.600 --> 02:06:31.400 getting infected and dying of this disease I like to remind people that during the Ebola outbreak 02:06:31.400 --> 02:06:35.640 both the one that just happened in the democratic republic of Congo and in west Africa 02:06:36.200 --> 02:06:41.640 you know somewhere between 16 to 19 000 people were still dying every week of HIV infection so 02:06:42.360 --> 02:06:49.560 you know the the public the medical community's governments were really gotten very good at 02:06:49.560 --> 02:06:55.640 managing how we deal with the scourges of infectious disease so like any respiratory virus 02:06:55.640 --> 02:06:59.400 you know we're going to be getting ourselves into the habit of washing our hands much more 02:06:59.400 --> 02:07:04.200 frequently if you could if there's one thing that you can do it's wash your hands much more frequently 02:07:04.200 --> 02:07:08.280 height so I mean we're we're both clinicians as well we go into the hospital 02:07:08.280 --> 02:07:12.280 a nurse will wrap you on the on the knuckles if you don't wash your hands coming into the room 02:07:12.280 --> 02:07:17.320 or coming out even if you don't touch anything so that's critical the the things that we already 02:07:17.320 --> 02:07:22.840 know how to do we do social distancing you know we're not going to be doing a lot of hugging 02:07:22.840 --> 02:07:27.880 and kissing if people are sick they should stay home if they're you know if they really are 02:07:27.880 --> 02:07:33.080 are very very ill then they can go into the hospital so um but hospitals now are 02:07:33.080 --> 02:07:37.800 getting very good about about you know how they would approach making sure that they can 02:07:37.800 --> 02:07:42.200 protect their staff as well as protecting other patients from someone who might be a risk so 02:07:42.760 --> 02:07:46.920 you know I think people should should recognize at the end of the day this still remains on low risk 02:07:48.520 --> 02:07:55.080 infection to not just our service members but to the american public and that we are really good 02:07:55.080 --> 02:08:01.960 as a hospital system as a medical care system from both the EMT up to intensive care units that 02:08:01.960 --> 02:08:06.760 taking care of these I'm not minimizing I'm just saying that even the absence of a vaccine we still 02:08:06.760 --> 02:08:11.480 don't have a vaccine for HIV infection but we have very good drugs and we're beginning to develop 02:08:11.480 --> 02:08:18.440 monoclonal antibodies so you know we will continue to to campaign against these infectious disease 02:08:18.440 --> 02:08:23.800 threats as we would against enemies against the homeland and we're we're good at doing those 02:08:23.800 --> 02:08:28.760 sorts of things but the american public should be reassured that that this is a threat that we're 02:08:28.760 --> 02:08:33.960 used to from from the standpoint of influenza we are working on developing measures but 02:08:33.960 --> 02:08:41.080 everyone can assist just by washing their hands well I hope uh hopefully you've been able to hear 02:08:41.080 --> 02:08:45.720 that uh when you're talking to the different agencies that are out there and you're getting 02:08:45.720 --> 02:08:50.520 different responses for what they're doing individually this is truly a whole of government 02:08:50.520 --> 02:08:56.520 approach so certainly if if one uh one agency one organization if it's an industry partner if 02:08:56.520 --> 02:09:02.760 it's academia I think we're well nested and we're sharing information and collaborating so that 02:09:03.800 --> 02:09:10.920 we're able to leverage the right resources to bring a vaccination or vaccine candidate as we've 02:09:10.920 --> 02:09:16.680 learned about today across the finish line so we're going to continue to collaborate in the fashion 02:09:16.680 --> 02:09:23.560 that we that we have and we're going to work as hard as we can to find the right treatments 02:09:23.560 --> 02:09:28.280 the right preventative measures and um it's certainly the right detection capabilities that 02:09:28.280 --> 02:09:34.680 are out there those are our three focus areas within within the DoD um we really appreciate your time 02:09:34.680 --> 02:09:41.560 today and um uh again thank you very much it's been a it's been a pleasure so everybody thanks 02:09:41.560 --> 02:09:46.280 for coming today so we have some folks are going to stand by in this room to do follow up questions 02:09:46.280 --> 02:09:51.800 for you thank you very much for being here tonight um this has been giga ohm biological high 02:09:51.800 --> 02:09:55.640 resistance low noise information brief brought to you by a biologist you can support me at 02:09:55.640 --> 02:10:00.920 giga ohm biological.com and you can share this stream from twitch and elsewhere i'm going to be 02:10:00.920 --> 02:10:05.320 putting up a couple episodes on sub stack this week yet i apologize for not having up something 02:10:05.320 --> 02:10:10.440 already i've got the subtitles on a couple videos but i haven't actually done the transcript yet so 02:10:10.440 --> 02:10:18.040 i will very soon next couple days um tomorrow i'm going to be interviewed by uh the last american 02:10:18.120 --> 02:10:24.760 vagabond which i believe is the one of the the websites and news sources that has Whitney 02:10:24.760 --> 02:10:28.360 web on it i'm going to be interviewed by ryan christian tomorrow i'm not sure if i'm going to 02:10:28.360 --> 02:10:33.000 put that live or if i'm going to let him record it and then make it an episode we'll probably 02:10:33.000 --> 02:10:38.440 talk about that before i start so either it'll be right on there oh that's the old list sorry about 02:10:38.440 --> 02:10:46.360 that um it will either be uh live at around noon or it will i will be live sometime in the 02:10:46.840 --> 02:10:51.800 afternoon after that interview um but that's probably pretty fun um i'm excited about that 02:10:52.280 --> 02:10:58.520 uh so anyway um that's been a show sorry it was late i need to go get a midnight snack and then 02:10:58.520 --> 02:11:02.280 go to bed um and i will see you again tomorrow thank you very much for joining me 02:11:16.360 --> 02:11:31.240 so 02:11:46.360 --> 02:11:47.360 .