COVID Vaccines May Bring Avalanche of Neurological Disease
In this interview, return guest Stephanie Seneff, Ph.D., a senior research scientist at MIT for over five decades, discusses the COVID-19 vaccines. Since 2008, her primary focus has been glyphosate and sulfur, but in the last year, she took a deep-dive into the science of these novel injections and recently published an excellent paper1 on this topic.
Significant Death Toll Will Rise in Months and Years to Come
Five months into the vaccination campaign, statistics tell a frightening story. Seneff cites research2 showing deaths are 14.6 times more frequent during the first 14 days after the first COVID injection among people over the age of 60, compared to those who aren’t vaccinated. That is extraordinary. You can read the full paper here.
Other data,3,4 reviewed in the video above, show that after COVID-19 vaccines were implemented, overall death rates have increased, with the exception of a few areas. Interestingly, Seneff believes she may have discovered why. It appears countries in which COVID-19 vaccines have not raised mortality rates are also not using glyphosate.
Ultimately, Seneff believes, as I do, that the COVID-19 “vaccines” will end up killing far more people than the disease itself, and will in fact make the disease worse. Seneff cites a disturbing case history of a cancer patient in the U.K. who was treated for severe COVID-19 for 101 days.
The antibody cocktails they gave him didn’t work, and after his death, they concluded that the predominant SARS-CoV-2 variant in his body had a dozen different mutations in the spike protein. Somehow, his body figured out how to evade the antibodies, which is a critical piece of the puzzle.
“I think the vaccines are doing the same thing,” Seneff says, adding that, among the immune compromised, only 17% of vaccinated individuals actually produce antibodies.5Surprisingly, these people may actually have drawn the short end of the stick. The antibodies may not work because their immune function is low, thereby allowing the virus to build resistance and mutate.
COVID-19 Vaccines Are a Public Health Disaster
The typical unprecedented vaccine takes 12 years to develop, and of all the unprecedented vaccines in development, only 2% are projected to ever make it through phases 2 and 3 of clinical testing.
The COVID-19 vaccine was developed with Operation Warp Speed in less than one year, which makes it virtually impossible for this vaccine to be adequately tested for safety and efficacy.
Hundreds of millions of people are now being vaccinated around the world, based on nothing more than preliminary efficacy data. Disturbingly, while sudden death is one apparent side effect, the vast majority of side effects won’t be known until a decade or more from now.
Seneff predicts that in the next 10 to 15 years, we’ll see a sudden spike in prion diseases, autoimmune diseases, neurodegenerative diseases at younger ages, and blood disorders such as blood clots, hemorrhaging, stroke and heart failure.
Understanding Your Immune System
As your cells start producing the viral spike proteins, your immune cells rally to mop up the proteins and dump them into your lymphatic system. This is why many report swollen lymph nodes under the arms. This is also a sign of breast cancer. The antibody response is part of your humoral immunity. You also have cellular immunity, which is part of your innate immune system.
Your innate immune system is very powerful. And, if you’re healthy, it can clear viruses without ever producing a single antibody. Antibodies are actually a second-tier effect when your innate immune system fails. The problem is your innate immune system is definitely going to fail if you get a COVID-19 shot, because it’s bypassing all of the areas where your innate immune system would be brought to bear.
Your body will essentially believe that the innate immune system has failed, which means it must bring in the backup cavalry. In essence, your body is now over-reacting to something that isn’t true. You’re not actually infected with a virus and your innate immune system has not failed, but your body is forced to respond as if both are true.
How COVID-19 Vaccine Circumvents Healthy Immune Responses
But there’s more. As explained by Seneff, the synthetic RNA in the mRNA vaccines contains a nucleotide called methyl-pseudouridine, which your body cannot break down, and the RNA is programmed to trigger maximum protein production. So, we’re looking at completely untested manipulation of RNA.
It is very important to recognize that this is a genetically engineered mRNA for the spike protein. It is in no way shape or form the same that SARS-CoV-2 produces. It’s been significantly altered to avoid being metabolized by your body. Additionally, the spike protein your body produces in response to the COVID-19 vaccine mRNA locks into your ACE2 receptor.
This is because the genetically engineered NEW spike protein has additional prolines inserted that prevent the receptors from properly closing, which then cause you to downregulate ACE2. That’s partially how you end up with problems such as pulmonary hypertension, ventricular heart failure and stroke.6,7
As noted in a 2020 paper,8 there’s a “pivotal link” between ACE2 deficiency and SARS-CoV-2 infection. People with ACE2 deficiency tend to be more prone to severe COVID-19. The spike protein suppresses ACE2,9 making the deficiency even worse. As it turns out, the vaccines essentially do the same thing.
How Long Might Effects Last?
As mentioned, RNA is highly perishable, so to get it past the enzymes that would normally break down free mRNA, it’s encased in a lipid nanoparticle combined with polyethylene glycol or PEG. The PEG helps protect the RNA from breaking down. The RNA can easily enter the cell via natural endocytosis pathways, taking advantage of the nanoparticle design made to look like an LDL particle.
They strategically chose a cationic lipid, meaning it’s positively charged. “Usually you have phospholipids in your membranes that are negatively charged,” Seneff explains. The problem with cationic lipids is they disturb the plasma membrane and cause an immune response.
However, that may also be a key reason for why they were used. Typically, conventional vaccines contain an aluminum adjuvant to initiate an immune response. Aluminum was not appropriate for the COVID-19 vaccines, but the cationic lipids serve a similar function spectacularly well.
Being extremely toxic to the cell membranes, the positively charged lipids trigger immune cells to rush in to aid the cells and mop up the spike protein now being produced, while also being the vehicle that allows the RNA to slip into the cells. Once inside the cell, the mRNA delivers the instructions to produce enormous amounts of spike proteins.The really worrisome thing is there’s potential for it to become part of the DNA and then it will last forever. Stephanie Seneff, Ph.D.
Importantly, there’s no telling how long these instructions will persist. Manufacturers are guessing the synthetic RNA may survive in the human body for about six months, but we really don’t know if that’s true or not.
Again, the alterations they’ve done to the synthetic RNA are meant to prevent it from breaking down. It could be years or even decades that these spike proteins are being produced, and you will find out shortly why this is a really bad scenario.
Tracing Spike Protein From Cells to Lymph to Spleen
As explained by Seneff, your immune cells mop up mRNA and spike protein and dump them into your lymphatic system. From there, they make their way into your spleen, where they can remain for quite a long time.
Potential Vaccine Shedding Mechanism Revealed
Seneff also sheds light on the mysterious reports of unvaccinated individuals experiencing unusual bleeding symptoms after spending time in proximity to a newly vaccinated person. She believes this may be due to exosomes being released from the lungs.
So, to be clear, what’s being “shed” or spread by vaccinated individuals is the spike protein — which is itself toxic — not the SARS-CoV-2. So, it’s not an infection but rather the shedding of a toxic protein.
Can mRNA Vaccines Change Your DNA? That Is the Question
Getting back to the potential issue of gene editing, I’ve been accused of being scientifically ignorant for stating that COVID-19 vaccines are not vaccines but rather a form of gene therapy. But when you delve into the genetics and molecular biology of this vaccine you discover that they are in fact a form of a stealth gene editing tool that can change your DNA and integrate instructions to make even more spike proteins.
It’s counterintuitive because, typically, mRNA cannot be integrated directly into your genes because you need reverse transcriptase. Reverse transcriptase converts RNA back into DNA (reverse transcription). Seneff, however, discovered there’s a wide variety of reverse transcriptase systems already embedded in our DNA, which makes this possible. She explains:
LINEs and SINEs are sequences of nucleotides, pieces of DNA, and they make up a huge percentage of the genome. For example, LINE1 is 10% of your genome. Most of the time they’re inactive and scientists were puzzled about what they actually do. They’re rather strange, as they fold DNA backward and stick it back in different areas. For example, in people with Alzheimer’s, the amyloid beta protein gets duplicated all over the place in their genome.
In a nutshell, LINEs and SINEs appear to be activated when an alternative solution for a problem is needed. One such problem could be glyphosate exposure. When the body is too sick to function normally, it finds a way around the problem by mutating proteins. “It’s a process that we use to deal with environmental toxic chemicals that we’re confronted with generally,” Seneff says.
So, in summary, mRNA can be reverse transcribed and converted back to DNA by LINEs and SINEs in your body. This cloned DNA can then be integrated into your genome. In this way, it truly is genetic editing.
Are We Creating a Generation of Super-Spreaders?
What comes next is truly chilling. Seneff cites research10 showing that sperm has this ability to take exogenous mRNA, either from a virus or an mRNA vaccine, and reverse transcribe it into DNA and then produce plasmids that contain this cloned DNA. The sperm then releases these plasmids around the egg, which takes them up.
The egg hangs on to those plasmids and puts the new code into the cells of the growing fetus. Hypothetically, a man having been vaccinated with a COVID-19 vaccine could produce a child born with the genetic code to make the SARS-CoV-2 spike protein.
This is not a good thing, because this means the child will not have antibodies against the spike protein. Since it’s part of their genetic code, it registers as one of their own proteins and their body won’t produce antibodies against it. If that child is exposed to SARS-CoV-2, their immune system won’t react at all. What happens next is anyone’s guess, but it’s bound to be severely problematic in one way or another.
Even if such a child were to be unaffected by the virus, we could be looking at a serious problem, as they could turn into lifelong super-spreaders and a chronic hazard to everyone around them. At least that’s what happened in cows.
Seneff recounts a story of herds plagued by a viral diarrhea. They finally realized that “killer calves” were the problem. Calves were being born that had viral protein integrated into their genome. When exposed to the virus, these calves, unable to clear the virus naturally, then spread it to the adult cows, which got sick.
Such children would be true super-spreaders, and the indoctrination we’re currently seeing, where children are told their mere presence could pose a mortal risk to the people they love, would then turn into grim reality. The calves in question were euthanized to safeguard the rest of the herds. How would we address human equivalents?
Hopefully, this nightmare scenario will not occur, but it appears biologically possible, and that is the problem. The fact that the available science allows for this kind of speculation is reason enough to put the brakes on this vaccination campaign. We have no clue what the long-term consequences are. We don’t even know what the short-term consequences are, other than more vaccinated people are dying, collectively, compared to unvaccinated ones.
Spike Protein Appears Highly Problematic
A particularly fascinating part of Seneff’s paper addresses the toxicity of the spike protein. A key problem with all of these gene-based COVID-19 vaccines is that the spike protein itself appears toxic, and your body is now a spike protein-producing factory.
Why Spike Protein May Cause Serious Neurodegenerative Disease
Creutzfeldt-Jakob disease (CKD), the human version of mad cow disease, is a prion disease. Other human forms of prion disease include Alzheimer’s, Parkinson’s and Lou Gehrig’s disease (ALS). “You have all these horrible neurodegenerative diseases and each one is tied to specific prion proteins,” Seneff says. The SARS-CoV-2 spike protein also appears to be a prion protein, although this has yet to be thoroughly verified.
Disturbingly, the spike protein produced by COVID-19 vaccines, due to the modifications made, may make it more of a prion than the spike protein in the actual virus, and a more effective one.
Why Long-Term Neurological Damage Is To Be Expected
In her paper, Seneff describes key characteristics of the SARS-CoV-2 spike protein that suggests it’s a prion:11
So, in summary, the take-home here is that COVID-19 vaccines, offered to hundreds of millions of people, are instruction sets for your body to make a toxic protein that will eventually wind up concentrated in your spleen, from where prion-like protein instructions will be sent out, leading to neurodegenerative diseases.
Vaccine Remedy May Be Worse Than the Disease
In her paper, Seneff goes into far more detail in her description of the spike protein as a metabolic poison. While I recommend reading Seneff’s paper in its entirety, I’ve extracted key sections below, starting with how the spike protein can trigger pathological damage leading to lung damage and heart and brain diseases:13
Commercial Vaccines Are Not as ‘Clean’ as Trial Vaccines
Seneff’s paper also highlights the unknown hazard of injecting fragmented RNA, found in greater quantity in the commercially manufactured Pfizer vaccine compared to the vaccine used in the initial trials:14
Seneff and I cover a great deal more than I’ve covered in this article, including how the vaccines may trigger autoimmune problems by way of molecular mimicry. This includes things like celiac disease, Hashimoto’s thyroiditis and lupus. So, if you have ANY interest in learning more about this vaccine I strongly suggest you watch the entire video.
We also discuss how the shots are causing idiopathic thrombocytopenic purpura (ITP), a rare blood disorder in which you end up with blood clots, a drop in platelet count and hemorrhages, all at the same time.
Also, be sure to read through Seneff’s paper, “Worse Than The Disease: Reviewing Some Possible Unintended Consequences of mRNA Vaccines Against COVID-19,” published in the International Journal of Vaccine Theory, Practice and Research.15
How Can You Protect Yourself From the Vaccine or Exposure to Those That Were Vaccinated?
Indeed, that is the question of the day. We talked about shedding from the vaccine. Obviously, the vaccine does not classically shed virus particles but it can easily cause people to shed spike proteins, and it is these spike proteins that may cause just as much damage as the virus.
While Seneff’s paper didn’t delve deeply into solutions, it provides a major clue, which is that your body has the capacity to address many of these problems through a process called autophagy. This is the process of removal of damaged proteins in your body.
One effective strategy that will upregulate autophagy is periodic fasting or time-restricted eating. Most people eat more than 12 hours a day. Gradually lowering that to a six- to eight-hour window will radically improve your metabolic flexibility and decrease insulin resistance.
Another beneficial practice is sauna therapy, which upregulates heat shock proteins. I have discussed this extensively in previous articles. Heat shock proteins work by refolding proteins that are misfolded. They also tag damaged proteins and target them for removal.
Another vital strategy is to eliminate all processed vegetable oils (seed oils), which means eliminating virtually all processed foods as they are loaded with them. Seed oils will radically impair mitochondrial energy production, increase oxidative stress and damage your immune system.
Seed oils also are likely to contain glyphosate, as it is heavily used on the crops that produce them. Obviously, it is important to avoid glyphosate contamination in all your food, which you can minimize by buying only certified organic foods.
Finally, you want to optimize your innate immune system and one of the best ways to do that is to get enough sun exposure, wearing in your bathing suit, to have your vitamin level reach 60 to 80 ng/ml (100 to 150 nmol/l).
– Sources and References
1, 11, 13, 14, 15 International Journal of Vaccine Theory, Practice and Research May 10, 2021; 2(1): 402-444
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