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If a genetic sequence is injected that causes the body to manufacture a foreign protein, the body recognizes it as an invasion and launches an attack on cells. This autoimmune reaction can occur anywhere the injection lands, potentially causing myocarditis or a heart attack if it lands in the heart, stroke or neurological conditions if in the brain, blindness if in the eyes, or sterilization if in the ovaries. The body is being made to manufacture something that does not belong in it. The speaker believes the so-called vaccines encode spike proteins, which are acutely toxic to blood cells, prompting blood clots, and to nerve cells, causing them to malfunction. The body is forced to make something directly toxic, intentionally. The injectables are wrapped in lipid nanoparticles.

The discussion centers on evidence linking myocarditis and pericarditis to mRNA vaccination and the proposed mechanism behind it. It references a 2022 German study reporting that endomyocardial biopsy data from people with myocarditis showed cardiac detection of the spike protein and CD4+ T cell–dominated inflammation, suggesting a vaccine-triggered autoimmune reaction. The presenters note headlines at the time comparing myocarditis risk to infection, with claims that infection causes more myocarditis, and remind that vaccines were said not to stop transmission. They then cite a large Israeli population study from the same year involving subjects not vaccinated against SARS-CoV-2, which found no increase in the incidence of myocarditis or pericarditis, implying no observed vaccine-related signal in that cohort. Attention shifts to a more recent study published in Circulation by the American Heart Association, described as a high-impact, non-fringe journal, indicating a clearer mechanism has been demonstrated. The study described used an experimental mouse model to induce cardiac damage and then compared it to human cases with heart damage following vaccination. It states that T cells from patients with acute myocarditis or myopericarditis recognize vaccine-encoded spike epitopes that are homologous to cardiac self proteins, meaning the immune response to the spike protein can cross-react with heart tissues. The researchers further report that functional responses to potassium channels in patients with mild pericarditis after mRNA vaccination, but not in patients with COVID-19, showed an expanded pattern of cytokine production similar to that observed in myopericarditis mice and in autoimmune myocarditis. In plain terms, the summary of their takeaway is that post-mRNA vaccine myopericarditis is driven by molecular mimicry: the immune system cannot distinguish self from non-self, leading to an autoimmune attack on heart tissue in susceptible patients. The distribution of the vaccine (its widespread dissemination) is cited as a factor that makes patients susceptible by promoting heart-homing imprinting, effectively creating an anti-heart autoimmune response. The speakers emphasize that this Circulation article is a top-tier source, underscoring that the mechanism has been demonstrated with both animal models and human pathology, supporting the claim that the phenomenon has a defined immunological basis.

Studies show that more people who received the injections are ending up in the hospital and dying. Repeat injections can lead to tolerance issues by the immune system, preventing an effective immune response. The speaker is focused on the damages caused by these products and believes that the voices of the injured have been taken away. They hypothesize that the spike protein in the injections could cause hyper inflammation, especially in people with preexisting conditions. The speaker also mentions that the contents of the injection were supposed to remain at the injection site, but evidence suggests they can travel to the ovaries. They suspect that there is information being withheld from the public.

A study comparing gene profiles of 800 healthy individuals to mRNA-injured individuals found severe genetic dysregulation in the latter. Seven of the injured individuals developed new-onset cancers within a year of mRNA injection, while three experienced cardiovascular or long vaccine syndrome. Gene expression comparisons revealed thousands of dysregulated gene expressions in the mRNA-injured, linked to mitochondrial failure and oncogenic activations. Cancer suppression genes were not being suppressed, and immune dysregulation was observed. The study claims to be the first to show long-term genetic disruptions in the vaccinated, indicating molecular chaos within cells. This may be the biological mechanism behind cardiovascular and carcinogenic issues seen in the vaccinated, possibly due to genomic integration of DNA plasmids from the manufacturing process. The speaker states that this is a landmark report and calls for further investigation into the effects on the population, noting that a large percentage of the global population received COVID vaccines.

Speaker 0: The transcript cites multiple studies indicating severe behavioral changes in those who receive mRNA shots. A study by Oten colleagues found that the mRNA vaccine mRNA and spike protein were being produced in cerebral arteries of stroke patients. It is stated that the mRNA shot is based on the second largest COVID vaccine safety study ever conducted with eighty five million people in it, which purportedly found a two hundred percent increased risk of stroke after dose two of mRNA shots. The claim is that the vaccine goes to the brain, causes brain damage and neuronal destruction, and that this is reflected in neuropsychiatric conditions. This is linked to a study by Doctor James Thorpe and colleagues, which allegedly identified eighty-six neuropsychiatric safety signals for these COVID shots, including homicide, homicidal tendencies, psychosis, schizophrenia, Alzheimer's, cognitive impairment, and violent behavior, all claimed to be far in excess of what was reported with flu vaccinations, and described as corroborating multiple other studies. The transcript also references a study from Korea finding increased Alzheimer's risks and increased cognitive impairment risks, and another Korea study reporting a massive increased risk of depression, sleep disorders, and anxiety from these injections. The overall assertion is that, based on peer reviewed evidence, the injections damage the brain, cause brain damage resulting in neuropsychiatric conditions.

The speaker claims mRNA injections have caused a "catastrophic" level of damage, citing excess deaths, permanent disabilities, and injuries. Worldwide deaths are estimated at around 17 million as of September 2023. In America, estimations for the first year of mRNA injection deaths range between 480,000 and 600,000, based on extrapolations from a recent preprint and VAERS data. The speaker asserts the shots are cardiotoxic and neurotoxic, linking them to myocarditis, cardiac arrests, coronary artery disease, and 86 neuropsychiatric adverse events. Vaccine spike protein has allegedly been found in the brains of stroke patients 17 months post-vaccination. The speaker states the shots induce blood clotting and damage the kidneys and gastrointestinal system. Furthermore, the speaker believes the shots are carcinogenic, with over 100 studies indicating 17 distinct mechanisms by which they may cause cancer.

We compared gene expression profiles across several groups: a healthy control group pre COVID, individuals described as mRNA injured, a group with cancer, and a few individuals who had neurological and cardiovascular adverse events. The analysis showed that in the mRNA injured group, thousands of gene expressions become dysfunctional in several key cellular pathways. Specifically, dysfunction was noted in mitochondrial function, immune function, and protein production. The changes included the production of abnormal proteins as a result of these altered gene expressions. In addition, the analysis reported that cancer surveillance genes were literally turned off in the mRNA injured group. The genes mentioned as turned off include p53, KRAS, and BRCA. This observation is presented as part of the overall pattern of molecular disruption associated with the mRNA injury state. Overall, the findings are described as indicating that flooding the body with synthetic messenger RNA unleashes biochemical havoc. The speaker emphasizes that this biochemical havoc has severe consequences, as evidenced by the observed widespread gene expression dysfunction and the suppression of critical cancer surveillance genes, alongside the production of abnormal proteins and impairments in mitochondrial, immune, and protein production pathways.

A cardiologist provides an update on the Pfizer and Moderna vaccines. Studies have shown that the vaccines can cause direct harm to heart muscle cells, abnormal heart contractions, and abnormal electrical activity. Messenger RNA from the vaccines has been found in the human heart and circulating in the blood for up to 28 days. The spike protein produced by the messenger RNA has also been detected in the blood for up to 6 months. The spike protein is dangerous to cells, tissues, and organs in the body. The messenger RNA used in the vaccines has been modified and is synthetic. Autopsy studies have shown that the vaccine can cause myocarditis and cardiac damage. A basketball player who received the vaccine suffered a cardiac arrest and died two years later.

The speaker claims sequences found in vaccines are now also being found in people. According to the speaker, five peer-reviewed studies involving RNA sequencing of vaccinated and unvaccinated individuals show DNA from vaccine manufacturers in patients' blood. The speaker cites studies by Ryan et al., Chakrabarty, Rhine, and Odek as evidence of Moderna and Pfizer vaccine sequences in patients' blood, suggesting blood supplies are contaminated. The speaker mentions three additional papers (Lee, Navel, and Krauszik) that, while not explicitly looking for it, also confirm residual plasmid sequences in recipients. One study, which investigated a particular disease, revealed differential gene expression in the cGAS-STING and interferon pathways, indicating a potential DNA stimulatory response. The speaker suggests this RNA sequencing data reveals the nature of the contaminant, with gene expression changes indicating a cGAS-STING-like event potentially induced by the DNA.

Speaker 1 reports evidence from multiple sources, including InModia lab in Germany and John Cantazaro at NEO7 Bioscience, that Pfizer and Moderna code is reverse transcribed and inserted into human DNA. According to Speaker 1, this means individuals could carry a "stamp" of Pfizer or Moderna in their genome. The speaker suggests the body may not be editing out or repressing this code, as spike protein evidence persists for years. Transmission of spike protein producing genetic code is possible, along with fragments of code for the spike protein, SV40, and other DNA fragments. Speaker 1 raises concerns about potential health issues like blood clots, heart damage, autoimmunity, and unusual tumors. John Cantazaro's research indicates a dramatically altered genetic profile in vaccinated individuals, tilting towards neoplasm or cancer. Speaker 1 shares an anecdote about a patient who developed terminal cancer after vaccination, with Cantazaro confirming the presence of Pfizer code in the patient's genome.

A new study indicates mRNA injections induce severe, long-lasting genetic disruption linked to cancer and chronic disease. Comparing gene profiles of mRNA-injured individuals to pre-COVID samples revealed thousands of dysregulated gene expressions linked to mitochondrial failure, suppressed cancer suppression genes, and immune dysregulation. Molecular chaos may result in cardiovascular, neurological, and carcinogenic issues, possibly due to genomic integration of DNA plasmids. A separate study showed mRNA boosters trigger dangerous immune and blood abnormalities, including increased blood clotting and immune suppression, within 48 hours in healthy young adults. Additionally, pets are being used as self-amplifying mRNA vectors via Merck's Nobivac NXT, exposing pet owners to shedding of self-amplifying RNA and toxic antigens. This could potentially cause long-term genetic dysfunction in humans, with the possibility of the synthetic particle recombining with wild viruses. Individuals should ask vets about RNA or mRNA injections for pets and refuse mRNA injections for themselves.

Studies show that more people who received the injections are ending up in the hospital and dying. Repeat injections can lead to tolerance issues by the immune system, preventing an effective immune response. The speaker is concerned about the damages caused by these products and believes that the voices of the injured have been silenced. They suggest that the potential cytotoxicity of the spike protein should have been considered before proceeding. The exclusion criteria in the original trials excluded people with preexisting autoimmune conditions, which may be related to hyper inflammation. The speaker believes that the adverse events reported are a result of systemic damage caused by the spike protein. They also mention that the contents of the injection were expected to remain at the injection site, but evidence suggests that lipid nanoparticles can travel to the ovaries. The speaker suspects that there is information being withheld from the public.

The speaker clarifies they are injured by an mRNA therapeutic, not a vaccine, and highlights issues with lipid nanoparticles and synthetic mRNA, which can persist for hundreds of days. They claim that instructing cells to produce a protein that presents on the cell surface can trigger autoimmune disorders. The speaker states that the spike protein itself is biologically active, causing cells to grow and divide inappropriately, and was known to damage the placenta and lungs. They assert they knew early on that the shot didn't stay in the arm. They cite 2005 research showing the SARS-CoV-1 spike protein alone could harm animals. The speaker references 2015 gain-of-function research at UNC, NIH, and Wuhan labs, where a more lethal and transmissible SARS virus was created. A traditional vaccine attempt for this virus caused harm and lethality in animals, with pathology slides showing similar vascular lung damage seen with SARS-CoV-2. The speaker concludes that "they" knew about these risks but still rolled out the vaccine, profiting from it while falsely claiming it was safe and effective.

The speakers describe a study in which gene expression profiles are compared across several groups to assess the impact of mRNA injury. The comparison set includes a healthy control group that was observed before the COVID-19 era, individuals classified as mRNA injured, a subset of three individuals with cancer, and a smaller number of participants who exhibited neurological and cardiovascular adverse events. The central finding reported is that, in the mRNA-injured group, thousands of gene expressions become dysfunctional. The dysfunction spans several critical cellular and biological processes, notably mitochondrial function, immune function, and protein production. The speakers indicate that these alterations include the production of abnormal proteins as a consequence of the disrupted gene expression patterns. In addition to widespread dysfunction in metabolic and cellular pathways, the speakers note that genes involved in cancer surveillance are turned off in the mRNA-injured group. Specific genes named are p53, KRAS, and BRCA, with their expression or regulatory activity described as being suppressed or deactivated. The implication conveyed is that the disruption of cancer surveillance mechanisms accompanies the broader profile of gene expression changes observed in response to the mRNA injury. The overall conclusion presented by the speakers is that flooding the body with synthetic messenger RNA is associated with unleashing biochemical havoc, which they characterize as having severe consequences. The framing suggests a causal or strongly associative link between exposure to synthetic mRNA and the observed downstream effects on gene expression, including mitochondrial and immune dysfunction, abnormal protein production, and the suppression of key cancer-related surveillance genes. The narrative emphasizes the magnitude of the molecular disturbances, noting that thousands of gene expressions become dysfunctional and that critical safeguards against cancer may be compromised in the mRNA-injured group.

The speaker states: "We found circulating Pfizer mRNA in his exosomes three point six years after his last shot, and we also found plasmid DNA from the manufacturing process SV40 ORI segments, as well as the spike expression segments in his skin, in his Grover's disease area. He developed this skin disease after the shots." They add: "We also found vaccine spike protein and no nucleocapsid in this skin area as well." The speaker emphasizes timing: "Three point six years after his last shot, he suffered from myocarditis, pulmonary embolism, multisystem vaccination syndrome, neurological adverse events as well." They conclude: "And so the fact that we are finding this material forty three months after the last shot means we were lied to completely." The speaker claims: "We were told it would stay in the arm, it would degrade within weeks, that was wrong and we expect lawsuits to begin to flood in."

Speaker 0 describes what he claims is the strongest case report ever done on vaccine injury, specifically mRNA vaccine injury. The subject is a 51-year-old man who developed myocarditis, pulmonary embolism, neurological disturbances, and skin disturbances, constituting multisystem long vaccine syndrome. The key findings are said to be detected 3.6 years after his last shot. Exosomes circulating in his body allegedly contain Pfizer mRNA, and this mRNA is still present in those exosomes years after vaccination. The same mRNA is reportedly also found in his skin. In addition, plasmid DNA from the manufacturing process is claimed to be present in his skin, again 3.6 years after vaccination. Specifically, the plasmid DNA allegedly includes the SV40 segment, the spike expression cassette, and the open reading frame region, with all components of the plasmids in the Grover's disease–affected skin area. Microscopic analysis of the Grover’s disease area allegedly showed staining for SARS-CoV-2 spike or vaccine spike, indicating the presence of spike protein in that skin region. This staining for spike protein is reported as occurring 3.6 years after the shot. Overall, the speaker asserts that all vaccine components—mRNA, plasmid DNA with defined segments, and spike protein—remain in the body for multiple years, with findings in exosomes and skin indicating long-lasting presence. The speaker also asserts that this represents a situation in which “we were completely lied to.”

"you were two to four times more likely to suffer serious harm from taking the COVID vaccine than you were to be hospitalized with COVID." "what is more better described as a gene therapy than as a vaccine." "$500,000,000 worth of investments in the mRNA technology for vaccines." "mega analysis of all the data." "Hundreds of studies, peer reviewed studies showing the harms of the mRNA vaccine." "the side effects of this gene therapy was so enormous and progressive, it was difficult to fathom." "The millions of molecules of mRNA entering the cell is creating biochemical havoc." "It's disrupting protein metabolism." "It's interfering with tumor suppressor genes." "In other words, it may be a risk factor for cancer." "it's highly likely that the COVID vaccines have been a factor, a significant factor in the cancer of members of the royal family."

"Unfortunately, the mRNA platform, though it is brilliant in its conception, is fatally flawed." "the myocarditis and pericarditis that showed up as a result of COVID vaccinations are inherent to the platform, not to the messenger RNA that was delivered inside these shots." "the design of this platform is to induce your own cells to make a foreign protein which gets displayed on the surface of those cells." "there's no targeting mechanism to lead it to happen only in certain tissues, it can happen haphazardly around the body, including in places like your heart." "And what that triggers is your own immune system to see those foreign proteins and conclude the only thing they can, which is that those cells have been virally infected." "the right response, the response, the natural response of the body is to take virally infected cells and destroy them."

The speaker presents a set of dramatic pathological observations and a charged political critique. They show the myocardium of a man who died from unknown causes after the third vaccine injection, describing heart muscle as red with yellow islands identified as dead cells or scars. They claim that in a 77-year-old who had no prior heart history, the muscle was simply bedridden with scars, and that these scars were microscopic and would not have been seen unless the heart had been opened and examined. The speaker questions how the scars could have formed, asserting that the damp vaccine had been injected into the man’s blood, caused the vessels to become leaky, and allowed the vaccine to seep into the muscles. They describe the muscle tissue as red with islands of what they call “normal muscle” that were not normal, and refer to Michael Mertz as having found dead and dying heart muscle cells in these normal islands, specifically mentioning “numbers three and four.” They urge the audience to consult a publication that they claim is now available to everyone and describe it as “damning, so damning.” They challenge others to stop talking about the issue and to halt “this madness, this criminality.” They then name political and health authorities—“Biden,” the FDA, the CDC, and the WHO—and assert that these entities are killing millions and soon billions of people on the planet because they claim there is an effort to introduce mRNA vaccines for everything, listing measles, mumps, hepatitis, flu, and “you name it, you have it.” In sum, the transcript alleges that: - A man died after the third vaccine injection, with pathological cardiac findings described as red myocardium containing microscopic scars and islands of dead cells. - In a 77-year-old with no prior heart disease, the heart muscle supposedly carried microscopic scars and was bedridden, with the scars attributed to the vaccine entering the bloodstream and causing leaky vessels that allowed seepage into the muscles. - Michael Mertz is cited as having found dead and dying heart muscle cells within what appeared to be “normal” muscle tissue. - A publication is claimed to exist and be readily accessible, described as damning. - The speaker calls for stopping political and health authorities (Biden, FDA, CDC, WHO) and asserts that the introduction of mRNA vaccines for widespread use is leading toward mass and eventually billions of deaths.

"a systematic review of autopsy findings and deaths after COVID nineteen vaccination, actually proved a causal link between these mRNA shots and death." "A study by Alessandro and colleagues found a thirty seven percent life expectancy reduction in those who received two or more doses." "The first one, ninety nine million people in it. They found, five hundred percent increased risks of myocarditis, about two hundred, three hundred percent increased risks of spinal cord inflammation." "The second largest study with eighty five million people, and it just came out. They found three hundred percent increased risks, heart attacks, strokes, arrhythmias, and coronary artery disease." "And then we had another study last week that came out that showed people with strokes who got mRNA shots are producing spike protein in their cerebral arteries, so in their brains, for up to seventeen months."

The discussion reports a comparative analysis of gene expression profiles among four groups: a healthy control group pre-COVID, individuals who were injured by mRNA, and subgroups including three individuals with cancer and a few with neurological and cardiovascular adverse events. The study found that in the mRNA injured group, thousands of gene expressions become dysfunctional, affecting mitochondrial function, immune function, and protein production, leading to the creation of abnormal proteins. It also notes that cancer surveillance genes are literally turned off, specifically mentioning p53 and KRAS, as well as BRCA. The overall claim is that flooding the body with synthetic messenger RNA unleashes biochemical havoc, with severe consequences.

We have multiple studies now indicating severe behavioral changes in those who receive mRNA shots. a study by Oten colleagues that found the mRNA, vaccine mRNA, and spike protein was being produced in cerebral arteries of stroke patients. the mRNA shot's based on the second largest COVID vaccine safety study ever conducted with eighty five million people in it. They found two hundred percent increased risk of stroke in after dose two of mRNA shots. They actually identified 86 neuropsychiatric safety signals for these COVID shots, including homicide, homicidal tendencies, psychosis, schizophrenia, Alzheimer's, cognitive impairment, violent behavior. All of this stuff was found to be in far exceedance of what was reported with the flu vaccinations. We clearly now know based on the peer reviewed evidence, it damages the brain, causes brain damage resulting in neuropsychiatric conditions.

First, the mRNA is injected within lipid nanoparticles in your arm. It travels through every organ system, including the heart. Crosson found mRNA directly in the heart of deceased mRNA recipients. So we know it reaches the heart. Baumeyer found the spike protein directly in the heart in biopsies of patients with vaccine induced myocarditis. So we know the vaccine mRNA and lipid nanoparticles get into the heart, translate into spike proteins, so your cardiomyocytes begin to produce a toxic non human protein and your own body attacks the heart resulting in inflammation and cardiac scarring including micro scars which are undetectable with imaging. And so once you have this scarring, you're going to have cardiac electrical abnormalities, electrical conduction abnormalities, and your heart's not going to beat properly. And that's why we saw a lot of sudden deaths among athletes back in 2021.

Nicholas Holcher, an epidemiologist and foundation administrator at the McCullough Foundation, appears on the WiderWake Media Podcast to discuss what he calls harms from the mRNA COVID vaccines and to critique mainstream approaches to the pandemic and public health policy. - Vaccine definitions and mRNA technology - Pre-2000 definition: a vaccine is an injectable or oral product that introduces a killed part of a virus or an inactivated form to the body so that encountering a wild-type version would not infect or would cause a less severe illness. - He asserts that mRNA injections are not vaccines: they are a gene transfer platform using modified messenger RNA with long persistence in the body (via N1-methylpseudouridine), delivered in lipid nanoparticles. He claims these bubbles distribute systemically, including to the brain, heart, bone marrow, and reproductive system, and that they instruct cells to produce a spike protein, effectively turning organs into “toxic spike protein production factories.” He says this leads to autoimmune attack on those tissues and contributes to adverse events, including myocarditis, strokes, immune destruction, and “turbo cancers.” - History and purpose of mRNA in vaccines - According to Holcher, work on this technology existed for decades but animals testing showed high mortality or sterilization in ferrets and mice, preventing approval except under a declared global emergency. He contends the COVID-19 crisis enabled emergency use authorization across Western countries, with ulterior aims to inject the globe with mRNA technology. - Global impact and uptake - He estimates about 70% of the global population received at least one COVID-19 injection (mRNA or viral vector). He notes Eastern countries used non-mRNA platforms (e.g., AstraZeneca/J&J in some places; Sinovac elsewhere) but that uptake in the West was high. - Harms and evidence - Excess deaths: cites a study by Dennis Brancourt et al. estimating around 17 million deaths worldwide as a result of COVID injections (as of September 2023); he claims US deaths could be in the hundreds of thousands to millions. - Turbo cancers: cites multiple studies in 2023 showing increased risk of seven cancer types (colorectal, bladder, breast, thyroid, prostate, etc.) in vaccinated groups; cites a major cancer journal, OncoTarget, reporting hundreds of turbo cancer cases across 27 countries, with Pfizer contributing most cases. Holcher also mentions his own group’s work with Neo7 Bioscience documenting genomic integration of vaccine-derived mRNA in a stage IV bladder cancer patient (31-year-old woman) with a segment of mRNA found in circulating tumor DNA on chromosome 19; another study reported thousands of dysregulated genes in post-vaccine cancers, including p53, KRAS, and BRCA. - Definition of turbo cancer: per Merrick et al., rapid, aggressive tumor progression with sudden onset and early metastasis, often in younger individuals, and resistant to treatment. - Fertility, pregnancy, and autism - Fertility: cites studies suggesting fertility impacts, including Karaman et al. finding depletion of primordial follicles in rats after mRNA vaccination; Manichi et al. reporting 33% lower conception rates in vaccinated women in Denmark; a study indicating a ~20% drop in sperm concentration and motility with no recovery over five months. - Autism: asserts a large body of evidence linking vaccines to neurodevelopmental disorders, citing a 136-study review with 107 studies finding positive associations between vaccines and neurodevelopmental issues, including autism, attributed to toxicity and immune system disruption, particularly in children with high vaccine exposure and reduced detox capacity (CYP450 impairment). - Other topics tied to vaccines and public response - The COVID-19 period and vaccine skepticism: claims the pandemic catalyzed a large anti-vaccine movement because people were compelled to take an experimental gene therapy product. - Sam Altman and gene editing: discusses Altman’s Preventive venture with the aim to reduce heritable diseases via in utero gene editing but warns of the path to designer babies and the potential for harm in early-iteration edits, citing prior CRISPR experiments on human embryos that produced deformed offspring or nonviable results. - AI, workers, and future society: predicts two-tier society with implanted or enhanced individuals and a replacement of human labor by robots and AI systems; discusses military and surveillance ambitions in gene editing and AI augmentation. - Mental health and digital life: references a randomized trial showing that turning off mobile Internet improved depression scores and well-being to an extent comparable to or greater than antidepressants. - World Health Organization (WHO): notes the US has pulled out of the WHO, arguing this is good for the US but potentially harmful for others still in the organization; expresses concerns about the pandemic treaty and ongoing global health governance, including vaccine passport-style surveillance. - FDA and public health policy: acknowledges some shifts (e.g., cutting doses from the childhood schedule) but argues the FDA remains compromised and too aligned with vaccine industry interests; criticizes the removal of a potential black box warning for vaccines and calls for more accountability. - Resources and contact - Holcher invites listeners to follow him on X (Twitter) at @nichulsher and to read their work on focalpoints.com and through McCullough’s network. Note: The transcript presents Holcher’s claims and interpretations about vaccines, turbo cancers, autism, fertility, and policy changes. The summary reproduces these points without endorsement or evaluation.

Lipid nanoparticles, not intended for human or veterinary use, were administered to billions of people worldwide. Synthetic RNA and spike proteins from the vaccines were found to persist in the body for months, accumulating in the brain, peripheral nerves, liver, and other organs. Autoimmune diseases, myocarditis, renal gland damage, and reproductive harms were also observed. The spike protein affected the immune system, weakened the body's response to other infections, and caused damage to blood vessels, including the coronary vessels. It also led to the accumulation of abnormal proteins in the blood and impaired tumor surveillance. The potential impact on cancer was highlighted as a significant concern.