A short course in mRNA genetic therapy
The thinking of Robert Malone informs and educates; excepts from his talk
This is not easy reading; but you may learn some important information that reinforces negative views about mRNA COVID “vaccines.”
“the starting point is you have to understand that DNA makes RNA, and RNA makes protein. Not everybody has been through modern biology and understands the central dogma, but that's where this is going. mRNA is one of many different types of RNA. It's an acronym. It sounds scary to some people. It means messenger RNA. There's other kinds of RNA. Ribosomal RNA, transfer RNA. They do different things. RNA is just a molecule, a polymer that your body uses for many different things.
And one of them is to transfer information from DNA to the protein manufacturing machinery. And so, the idea of using mRNA as a drug is basically like hijacking the normal apparatus. If you think of RNA like a ticker tape to tell the little machine that makes protein what to make, you're taking and sticking in a foreign molecule, a foreign RNA that's not made from a copy of your DNA, and that's going to make the protein manufacturing machinery make a different protein, protein from a virus. I just wanted you to understand that. And this is just a diagram of those different types of RNAs and the machinery. We don't need to go into the molecular biology of it.
And we all know this virus now. Everybody's become a virologist and an epidemiologist over the last three years. And the spike protein on the right, as you can see, has kind of two parts. One is a part that sticks into the cell. And by the way, it exists as a trimer. I like to think of it as a treble hook, anybody go fishing. It's a trimer. And the little hook's on the end, so the barbs or the receptor binding domain, and the part that you tie the string to is the S1 subunit that sticks itself into the cell when it's being manufactured. That's the basic structure of the virus and the protein. Now, these are images, and they're hard to see from where you are. I'm going to talk to you about the tech, the formulation platform.
These are not liposomes. These are positively-charged fats, and RNA is negative. And you take these fats and you mix them with the RNA, and it all collapses into a glob. The problem with that is that when it collapses into a glob like this, it can stick to other globs. It produces very large aggregates. That's why the people that are administering these vaccines have very strict guidelines. Once they open the bottle and they hydrate it, they need to use it within a short period of time because otherwise, it forms big aggregates. And those big aggregates can be toxic to people. And there is a technology used to keep this aggregation from happening. And it's one of those different little parts that are in that upper panel that shows examples schematically of the chemicals that are used, these positively charged fats, and some of the other things that are added into the formulation, which includes cholesterol, among other things.
And one of those is polyethylene glycol. And polyethylene glycol is probably responsible for a lot of the short-term anaphylaxis. These are people that die within an hour or two after administration. Some people have hypersensitivity to polyethylene glycol. Polyethylene glycol is in there to keep these things from aggregating, and it's specifically engineered in this case so that it falls off of the particle soon afterwards because otherwise, it would keep the particle from binding to cells and delivering the RNA. That's kind of all I want to talk about, about the core idea. And as you can see from that little spiral, all of this aggregates and forms around a synthetic RNA that's made in the test tube. It's not really RNA. The stuff that's being administered is not natural RNA.
Another one of the lies is that the stuff that's being injected with these vaccines is not truly RNA. It's modified. One of the four parts, AUGC, that forms the bead, the string of pearls. Think of string of pearls with four different colors. That's RNA. But one of those colors, the U, is actually a modified U. It's pseudouridine. And it's put in there because the RNA has two problems as a mechanism for vaccination, as a delivery mechanism.
One is that these formulations are incredibly inflammatory. They provoke... If you want to generate pus, take these formulations without all the bells and whistles they've had to put on them, and inject them into an animal. They are highly inflammatory, and they're still inflammatory now. We know that now. We've experienced over the last three years. That's always been the problem with the tech. And they tried to solve it by incorporating this modified U called pseudouridine, which depresses the immune response to the RNA and a lot of other things. And it makes the RNA last a much longer time so it can keep making protein.
Pseudouridine is what's put all the way through this RNA rather than regular uridine. And because it has, it confers these activities, but it is not a natural RNA. It's not what the ideas that I originally came up with. The stuff would only stick around for a few hours. Now, this is too small for me to read and probably is too small for you to read, but the bottom line, as I said, is that pseudouridine greatly modifies this whole equation in so many different ways. And when it was developed and patented at UPenn as a modification to the core patents and technology, it wasn't really understood what it does.
The biology of pseudouridine is still not understood. And that's part of the story of all of this is that folks have kind of gotten ahead of their skis all the way through. They've pushed the technology because they want it so badly because the unmet medical need is so profound. They're so afraid of the risk, in part because we're creating that risk. But that's another story. And they wanted to have something that would be universal, that they could apply for any new pathogen and that could go straight from gene to vaccine. That's the idea.
And what they did is they kind of rushed things without understanding it. Now, you'll recall that we're administering, we're all receiving... Those that have received the vaccine, receive it in their deltoid. And what the FDA has told all the docs and Pfizer has told all the docs, is that that RNA, those complexes go to draining lymph nodes, and they do. The axillary lymph nodes that drain from that deltoid take that complex, it's piped into there through the lymphatics, and a lot of it does go there. Unfortunately, the data show that it also goes all over the body. But back in the day when this was just getting started, three years ago, well, we could argue about that, but as these particular products were being developed, they were being sold, the technology was being sold that the formulations used would only go to those lymph nodes. Now, we know that that's not true, but that's how it was pitched.
Now, what happens when that's done? The big story here underlying all this fraud … is the FDA did not do its job. FDA did not do its job, I think, because it was being pushed into a position of having to go along with what the intelligence community wanted and all of the push from the White House and everywhere else that we needed to have this technology, we needed to have this technology deployed globally. And so, we're going to just allow a lot of corners to be cut.
Finally, at the beginning of this year, with this paper published in January, a group from Stanford University asked the questions. How long is the RNA there? How long is the protein, spike protein being made? How much spike protein is being made? Fundamental questions that should have been known at the very beginning. But the FDA did not force the pharmaceutical companies to do those tests because they justified it. They did a little hand waving.
... because they justified it, they did a little hand waving. They said, "These are not gene therapy products. These are vaccine products." Now that's a lie, a convenient lie, but that's what they did and that allowed them to justify only applying the vaccine safety checklist at the FDA rather than also applying the gene therapy checklist. This is why when I first started talking about this and I said, "This is gene therapy." I got so much blow back from all the fact checkers in the press, et cetera, is because they could not allow the narrative to come out that this is actually a gene therapy product applied for vaccine purposes. But we know that the manufacturers knew that to be the case because they had said so in their SEC filings before all this happened years ago, okay? So this is another one of the little slights of hand that was used.
But this group at Stanford went and finally did the work that should have been done before this was administered to all of us, and what did they find? Well, among other things they documented, this is one of the first key papers that immune imprinting is happening, which is why when you get multiply jabbed, and I think these boosters are going to make it even worse, you actually become more susceptible to the viral infection because your immune system is tuned to only responding to the historic strain, not the current strain.
But they found some other things in here, and I'm sorry this is too much text, so I'll just tell you. What they found was that the levels of protein, these are actual patients, this isn't animal models or anything else, this is patients that have received vaccine, the levels of spike protein in the blood of these patients were much higher than the levels of spike protein found after infection. With infection, the virus is slowly starting to replicate in your nose and your oral pharynx and your mouth and your upper respiratory tract and your immune system is kicking in and starting to neutralize that, and they're having a fight as a gradual balance and it results in a slow growth in the amount of antigen.
With the RNA, when that young gentleman there that's going to sleep gets his vaccine, which hopefully he didn't take, what happens is his body gets a truckload of spike antigen that's basically dumped into his bloodstream on a very short time course, very different from natural infection. And so when people say, "Well, why would you see toxicity with the spike protein from the vaccines and not see the same... Why would it be worse with the vaccines than with the infection?" Well, because of dosing, there's so much more protein being produced, and by the way, it's being produced for a long time, about 60 days or longer. They didn't test beyond 60 days. Furthermore, the RNA doesn't just go away after a few hours like real RNA, this RNA that has pseudouridine in it lasts for up to 60 days as long as they test it. Again, this is not theoretical, this is putting needles into patients axillary lymph nodes, taking a sample and asking is the RNA there and taking blood samples and asking how much protein is in those blood samples. So that explains a lot of what we've experienced.
Then there's this issue, and this is part of the lies that Paul was talking about that we've all experienced, that natural immunity is not as good as vaccine-induced immunity. There are many, many papers out now that show that that's not true. And from first principles it's easy to understand why it's not true. When they built these vaccines they chose to basically start with what had been done before and failed with MERS and SARS 1 vaccine development and only use a single protein, only used the spike protein and used the whole spike protein because they were in denial that the whole spike protein was a toxin and they still are, but they're kind of starting to have to concede that point.
But they only used one antigen. When you get infected by the virus, you mount a antibody and a cellular immune response against a whole bunch of antigens, and so if the virus starts to evolve to evade immune surveillance on the spike protein, which is what's happened in the face of all these jabs that everybody's got all over the world, if it starts with a natural immunity, if it starts to evolve to escape that immune suppression, immune pressure on the spike, it can't do that at the same time that it's evolving to escape all the other forms of immune pressure that are there because of all the other proteins that it makes. This is fundamental. Everybody knows this in my field, but they've been in denial about this and this is this insistence that their approach is the best and is accurate and it won't drive the immune escape, et cetera, et cetera. But the data are in now, natural immunity is more robust, longer lasting, more protective, and likely, results in much less [inaudible 00:33:50] development.
What are the risks? Let's see if I can read them here. This is actually the Cumulative Analysis of Post-Authorization Adverse Event Report from Pfizer, this is from the data that was forced to be released by Pfizer by court order instead of being delayed for 7 years, like Paul was talking about. Central general disorders, nervous system disorders, musculoskeletal disorders, gastrointestinal disorders, respiratory disorders, skin disorders, infections, cardiac, vascular, psychiatric, blood and lymphatic, eye, immune, it goes on and on. In the Pfizer disclosure, it's 11 pages, okay? They've known all this stuff. This isn't what they thought might happen, this is coming from pharmaco vigilance at Pfizer with their licensed vaccines, because the stuff that's here in the United States is not the licensed product, by the way. This is data coming from all over the world accumulated by Pfizer by the pharmaco vigilance team, and this is what they're reporting to the FDA, which the FDA of course then denied was actually happening.
The list of adverse events is huge, it's like nothing any of us have ever really seen with a product like this. I've certainly never seen anything like with this vaccine, let alone the mortality. And why our government and our regulatory agencies, both in the US and globally, aren't willing to address that is another whole discussion about the politics and the corruption that's gone on….
Now, the last key thing I kind of want you to understand as we talk about this, we talk about these genetic vaccine technologies, and I guarantee they're going to be deployed on you for years now, but you need to understand some of these fundamentals, platform versus payload, and everybody gets mixed up in this. There's the platform technology, which has the potential to enable a whole new class of pharmaceuticals, therapeutics, customized treatments for individuals for their cancer, all kinds of good stuff, this is why these companies have their market cap, potentially to enable a new class of pharmaceuticals based on delivery of genetic information.
The idea, as I mentioned with the platform, is that you can go direct from genetic sequence to product and shorten the development time because the manufacturing is the same no matter what the sequence is. You just key it into the computer. That's why they love it. They think that once they get one standard manufacturing process with all the characterization associated with it, they don't have to do it again. They can just go to the computer, key it in, sequence whatever the thing is, make customized medicines for your wife because she's got cancer or any new pathogen that's come out of Central Africa or whatever the thing is. That's their belief system.
The mRNA platform includes all of the things that are required to manufacture and deliver the RNA, that's separate from the thing that's made, the protein that's made, that's called the payload. It's kind of important for you to understand going forward to make sense out of all this stuff. Okay, so you understand platform versus payload, the spike protein and the RNA coating the spike protein is the payload. The way that it's packaged, assembled, manufactured, tested, et cetera, is the platform. The platform consists of these fats, the polyethylene glycol, other RNAs, the synthetic mRNA, other components.
Is there graphene oxide? The problem I have with that question, which has been coming at me for almost two years now, is there's no way for me to know whether there's graphene oxide or not. There's a lot of graphene oxide in the general environment, and the only way that this can ever be demonstrated to either true or false is either if, number one, the pharmaceutical companies come clean with the components that are in these products, and they will not release that, okay? They will not release a full component list. Or, a regulatory agency or someone else empowered will test the lots coming off of the line rigorously in a controlled way with a clear chain of custody as they have always done in the past, and which they are forbidden from doing by contract from these manufacturers.
So the problem I have with the graphene oxide and the other contaminants is that in most cases there is no good way to answer that question because we are forbidden from answering that question because, through contract, the regulatory agencies aren't able to do their job all over the world and assess what's actually in those vials. Are they truly pure? Is the identity what's defined? Is the potency what's defined? The pharmaceutical companies have executed contracts that prevents that from being known.
There's no question that we have contaminants of small glass fragments and small metal fragments in many lots, not necessarily all lots, and those are known types of contaminants that come from existing pharmaceutical manufacturing processes like fill/finish, and they're absolutely toxic. And again, that's evidence that the regulatory agencies have not been doing their job. That's their job is to ensure purity, potency, and identity.
The payload also includes the manufacturing, purification and testing processes, which I've just talked about, have been co-opted. It includes the regulatory package, including the nonclinical testing. So this is the notorious animal testing that was done not with the spike encoding RNA, but with the firefly protein called luciferase, using the least sensitive method for detecting where the product goes, which is whole body imaging as opposed to dissecting the tissues and analyzing them. Somehow the FDA allowed the wool to be pulled over their eyes by the pharmaceutical companies and they allowed them to use the least sensitive method for determining where this stuff goes and where it's making protein. That's another huge failure.
But the platform includes all of that data, fill, finish, distribution and storage, all of that goes into the platform tech. And the payload is, as I mentioned, the RNA, which causes your cells to become the manufacturing facilities. And that RNA itself can have biologic activity, so I've talked about the pseudouridine immunosuppression, increased half life. Another major problem with these products is that during the manufacturer of the RNA itself or the pseudouridine RNA, what happens is that the polymerase, the thing that's making it in this biologic reaction stops periodically and when it does that it releases a fragment of RNA that's incomplete. Those RNA fragments...
RNA that's incomplete. Those RNA fragments are biologically active. They can interfere, they can elicit immune responses, all kinds of things. And they don't have a good way to purify those. So the material that's being injected, it's not just a false RNA, a pseudo uridine, including RNA, but it's a whole mixture of stuff of which they hope the majority is the thing they want. But they haven't created any purification guidelines for all these other contaminants. If it was a normal drug or a normal biologic, the FDA would be rigorously scrutinizing and ensuring that it is only the biologic that it's claimed to be and doesn't have any other contaminants or so, if they're contaminants there's strict guidelines about how much. That doesn't exist here.
The payload also includes the protein. And the primary protein in this case is spike. In other cases is the influenza hemagglutinin for the new flu vaccines. But that protein we now know can have other things embedded in it. And I mentioned the snake venom story. I don't think that the sequence analysis supports that thesis of Dr. Artis. I'm absolutely not convinced. But the possibility that these proteins can be engineered to include other antigens, or do include other antigens is absolutely feasible, is absolutely viable. So the payload and the sequence of the payload and what it causes your cells to manufacture are crucial.
Now, how and why is this being pushed? Obviously, we've all experienced the propaganda and censorship, and Paul's talked about that. I've experienced it personally. This is uncontrolled information warfare, unrestricted information warfare at a level the world has never seen before. We have a situation in which all of the major media is controlled by large financial entities that happen to be the same ones that control the pharmaceutical industry. And functionally, control our government. What we've seen is that the propaganda information warfare blocking of anybody disclosing adverse events, like all of you that got up and said you've known of people directly that have either died or been damaged. I've been vaccine damaged. That's not allowed to be discussed.
It's not allowed to be discussed because of the potential impact on the deployment of this product, which they believe that the ends justify the means. That it is absolutely essential that they get the world to be able to accept this new technology because if they don't... And there's all the other agendas about the vaccine card, and the personal ID and central bank digital currency, et cetera. But, at the fundamental level, there's a belief that this technology is so important that we have to push it through the entire population. And we have to get people to accept it. And so, that's so important that they believe that they were justified in deploying the largest propaganda effort the world has ever seen.
It was over a billion dollars spent by the CDC, okay? And it's still ongoing. What that results in is that people cannot have informed consent. So I have a colleague who blames me, says that because I talk about mass formation psychosis, I'm saying that everybody is responsible and the global predators are not responsible. In no way is that true. That's a false narrative. And I'm in no way saying that individuals are responsible if they, like I, took the vaccine. We were not able to obtain informed consent.
In my case, I had a teleconference because of who I am and my background. I had a teleconference specifically with Peter Marks at the FDA early on where I said, "Peter, I'm concerned about these things that are in this non-clinical package. You guys have been hoodwinked." And he told me, basically, "Robert, give me some time to get this out. I have the new data package from Pfizer. I have no concerns now. Please don't make a big issue out of this." And I stayed silent for a few months based on that, and I took the jab. And I got the toxicity. My point is I was fooled. We were all fooled. And we were all prevented from having informed consent. So forgive each other, please. Forgive me.
Now, this is new information that was just published. In April of 2021 there was a World Health Organization consultation. Now, that's fancy bureaucratic talk for we all get together and figure out what we're gonna do. It was chaired by Margaret Liu of Merck, who was the person that was at the forefront of the team trying to get DNA vaccines developed back in the '90s and failed. But she was the chairperson, very much an industrial scientist. In this meeting that brought together all the regulatory agencies from all over the world, it was decided to circumvent normal preclinical and clinical testing based on this shared core platform concept. That's why I wanted you to understand what the platform was as opposed to the payload.
So there was a conference at WHO in which all the Western regulatory agencies got together and China, and they all agreed that we're gonna treat this as a platform technology, and we're going to push it through with very limited testing. And then once we've done that, new products can be rapidly developed by grandfathering in that old inadequate data package. Now, I'm not saying this as a conspiracy theory. It's published. And we are now seeing that being deployed. The only new data that will be required for these new vaccine and mRNA based therapeutic products is going to be that associated with the payload. So they're gonna assume that the platform is safe now because it's been deployed in billions of people. That's another reason why they have to deny all the adverse events 'cause the whole logic collapses otherwise.
The FDA position, and we've now seen this deployed, thank you for five minutes... We've now seen this deployed with the new boosters. The FDA position is that changes in the mRNA sequence for similar payloads do not require substantial non-clinical or clinical data. What that means is what we've seen. They went to manufacturing, sales, and deployment of these new vaccines with virtually no real testing. To the extent that they did any testing in mice what they found was that it didn't in any way interfere with infection of those mice by the pathogen. It didn't work in the mice. It doesn't matter. They've all agreed that this is the new rules.
So now, we have over 100 clinical trials for mRNA vaccines, 51 of which are currently enrolling, the rest are about to start enrolling in the United States, and they're all grandfathered based on what they assert is the clear evidence that there is no safety risks associated with this technology because it's been deployed in billions of people in the United States and worldwide.
In addition, there's over 200 clinical trials for mRNA based drugs based on this same logic. This all grandfathers in a technology platform, ignores that what's being delivered is not natural RNA. And what it creates is a situation. This is how things work in regulatory space. There's only two companies right now that have those approved data packages. And what that means is that these two companies now have a monopoly on any new drugs, or vaccines developed and deployed with this technology. Because anybody else that's gonna try to come in with their own version of it is gonna have to go through all of that other testing and demonstrate that their stuff is at least as safe and effective as the stuff that's been deployed on all of us. So what the FDA has done is granted a monopoly in perpetuity to Pfizer, BioNTech and Moderna.
So I hope that instead of talking about this toxicity or that toxicity, the event rate for the cardio toxicity, or whether or not we're all going to die in five years that have taken the vaccines, what I've tried to do is to help you to comprehend what's really going on underneath all of this. And remember my statement at the start, that's not to say that this outbreak and the situation was not exploited for economic and power reasons by a bunch of other bad actors. It's not to say that there wasn't planning aforehand. It's not to say that Bill and Melinda Gates Foundation and Bill Gates has not made book on this. It's not to say that in any way I'm denying that the corruption in the FDA, and the CDC and academia, as Paul was talking about, is profound and deep and systemic. I'm only giving you this little lens of looking through the RNA technology environment so that you can comprehend at least that part as you try to make sense out of everything else.”
Special event going on NOW - livestream about the global dangers of WHO/WEF attempt to take control and what to do about it, the grave harms caused by the covid shots, & more. Now talking: Rabbi Jonathan Rietti. In 1 hour at 5:30 PM EDT - live with Dr. Pierre Kory MD in NY! Afterwards: Attorneys Thomas Renz and Bobbie Anne Cox. Please join! https://truth613.substack.com/p/critical-livestreamlive-event-this
Recording will G-d willing be posted on my substack afterwards.