reSee.it - Related Video Feed

Speaker 1 claims that no vaccines, including the COVID vaccine, have been properly tested. They assert that no childhood vaccine has undergone a placebo-controlled clinical trial of sufficient duration and power to assess its safety before being injected into millions of children in America. Speaker 1 states this is not just their opinion, but can be verified by anyone who examines the FDA website, specifically the package inserts and underlying clinical trial documents.

Twenty percent of Americans did not take the COVID vaccine because it was not safe enough. The mRNA in the Pfizer and Moderna vaccines has been chemically modified to resist breakdown by enzymes. The mRNA and spike protein are found in the heart and brain, and the spike protein circulates in the blood for six to nine months post-vaccination. The speaker claims the lethal part of the virus circulates in the blood of vaccinated individuals, especially after boosters, and that it is a killer protein. The speaker asserts safety trumps efficacy and objects to claims that vaccines, specifically the COVID-19 vaccine, saved millions of lives. They state that consent forms do not guarantee the vaccine will save lives and that there has never been a prospective, randomized, double-blind, placebo-controlled trial showing that COVID-19 vaccines reduce mortality or hospitalization.

Speaker 0 argues that the myth that vaccines are safe and necessary and that they eradicated childhood disease is false. He claims vaccines have never been tested for safety and that there are no placebo-controlled trials; in trials, the control group is given the immunogens that are in the vaccine, making the comparison deceptive. He emphasizes that vaccines typically contain a protein plus an accompanying substance—the adjuvant or immunogen—that stimulates an immune response, and that these adjuvants (such as aluminum or other substances) by themselves are dangerous. When the control group receives these adjuvants along with the experimental group, he says the side effects are similar, describing this as a “slight hand trick” and “extremely deceptive.” He notes that for the last forty years people have been shouting that there has not been a true placebo-controlled trial with saline. He then argues that if one looks at the history of all the childhood illnesses that vaccines target, they were almost all nearly eradicated before the introduction of the vaccine. He claims that the impression vaccines stop childhood illnesses is not true; almost all illnesses had reduced to extremely low levels due to sanitation and hygiene, development, and some antibiotics. Regarding the vaccines themselves, he states that the true data and history of these vaccines are “really horrible.” He mentions a history of lack of safety and relates it to sudden infant death syndrome, asserting that it “suddenly came out of nowhere as we suspended the schedule” and asks when death occurs. He asserts that sudden infant death syndrome is reproducible in that it occurs at two months, four months, and six months, and that most of those deaths occur within days to a couple of weeks of the vaccine. He concludes with a strong personal stance: if he had his young children today, he would not give them a single vaccine.

Speaker 0 asserts that there is no safe vaccine on the childhood schedule and labels themselves an anti-vaxxer because no vaccine has been properly tested for safety. They state that, in the book Vax Facts, you are more likely to die from the vaccine than from the disease for which there is a vaccine, and that this is true for every single vaccine on the childhood schedule. They acknowledge that death from the vaccine is still a death and “super rare,” but claim you are much more likely to die from the vaccine. They ask which do you want: a greater chance of dying from the vaccine or a lesser chance of dying from the disease, noting that for many of these diseases, the risk is zero.

According to the speaker, most vaccines have never been tested in a randomized, placebo-controlled trial to evaluate their safety. The speaker claims that vaccines contain aluminum compounds because many dead vaccines don't mount an immune response without them. The speaker alleges that in a Gardasil vaccine study, the placebo group received an aluminum adjuvant instead of a true placebo, resulting in similar side effect profiles between the active vaccine and placebo groups. The speaker asserts that Merck used a novel aluminum compound and that data suggests aluminum in vaccines is profoundly toxic. The speaker states that the only true randomized controlled trial involving a vaccine was conducted on sheep with blue tongue disease. The results allegedly showed that the aluminum in the vaccine was toxic, causing the sheep to become sick, unsociable, and, in some cases, die. The speaker concludes that the assumption that aluminum adjuvants in vaccines are safe is unfounded and has never been tested.

The discussion centers on the credibility of vaccine safety claims made by various health organizations and the FDA. One speaker argues that vaccines undergo rigorous testing, while the other contends that no vaccine has ever completed a long-term placebo-controlled trial before being licensed. They express distrust in the FDA, citing past issues with drugs like Vioxx and opioids, suggesting that the FDA misled doctors and the public about their safety. The speaker believes that pharmaceutical companies influence these agencies, leading to misinformation about vaccine safety. The goal is to address and rectify this perceived corruption.

The speaker argues that looking up “FDA licensed vaccines” and reviewing “6.1” in vaccine inserts on the FDA website shows that placebo trials “never” occurred, including for childhood vaccines. The speaker claims that these placebo trial details are contained in insert text that was “wrapped around a vaccine” but allegedly not shown to people due to lack of “informed consent,” and that experts may cite studies that the speaker says did not exist. The speaker further alleges that Tony Fauci lied about “six foot distancing,” and that “everyone at the CDC and the regulatory agencies” lied. The speaker also claims that Robert Kennedy Jr. stated that COVID vaccine efficacy claims about stopping transmission were lied about, referencing Rachel Maddow’s claim that if you take the vaccine “it stops with you,” and the speaker asserts “the virus stops with you bull crap” and “it does. And you heard that here,” followed by a claim that it “does not” based on what “we know.” The speaker says that FDA “has already admitted” these points and emphasizes a call to “start asking people to show their work” and to “see the evidence,” saying “Do not trust experts any longer” because “we’ve been lied to long enough.” The speaker expresses hope that a documentary will not be the last made and claims they do interviews by giving their opinions directly and not worrying about being edited “to make me look crazy,” arguing that audiences will decide for themselves. The speaker then discusses the “vaxxed versus unvaxxed” study, saying they worked to build a relationship with someone who wanted to “prove me wrong.” The speaker claims they took a risk and promised to trust whatever the study shows if it is published, and asserts that the study results will show “how bad it is when you do this study the right way.” The speaker claims the CDC has “done this study a thousand times” trying to prove vaccinated people are healthier and that it “can’t” be done, and that doing it “the right way” will reveal worse outcomes. Finally, the speaker frames the “inconvenient” study as inconvenient for panels, for the pharmaceutical industry that allegedly owns television stations, and for CDC and HHS leadership, concluding that they “aren’t going to take it anymore” and claiming “evidence like they have never, ever had before.”

Vaccine recommendations typically come from the Advisory Committee of Immunization Practices (an outside consulting committee at CDC) and VRBPAC (within FDA), which recommends vaccine licensure. These committees only adopted evidence-based medicine about twelve years ago. The speaker states that during their administration, they want safety studies prior to vaccine licensure and recommendation. They claim vaccines are exempt from pre-licensing safety testing, and the COVID vaccine was the only one tested in a full placebo trial. They assert that the other 76 shots children receive between birth and 18 have not been safety tested against a placebo, meaning the risk profile is not understood. The speaker intends to remedy this.

The speaker claims that no double-blind, placebo-controlled safety trials have been conducted on any childhood vaccines currently on the market. The speaker states that they have searched for such trials and been unable to find any. According to the speaker, Anthony Fauci and Francis Collins allegedly admitted that placebo-controlled safety trials are not performed on childhood vaccines because it would be unethical to test products administered to children. The speaker challenges news agencies to provide evidence of a double-blind, placebo-controlled trial done prior to licensure for any childhood vaccine, asserting that it doesn't exist.

None of the 72 vaccines for children have been tested against a placebo. The speaker sued HHS in 2016 to find placebo studies for vaccines, but none were found. The safety testing for the polio vaccine was only 48 hours, while the hepatitis b vaccines were tested for 4-5 days. This means that any adverse events occurring after that time period were not considered. Without placebo testing, the risk profile of current vaccines is unknown, and it cannot be determined if vaccines cause more harm than good. The speaker questions the ethics of mandating medical products with unknown risks for children.

The speaker claims that searching the FDA website for “FDA licensed vaccines” and checking section 6.1 on vaccine insert documents will show that placebo trials “never did” occur, including for childhood vaccines. They argue that placebo trial details are included in insert materials for vaccines where the public “never got to see” certain information due to lack of informed consent, and they say experts would claim those studies were done because they rely on what the insert language indicates or what they assert based on expert testimony. The speaker further asserts that Tony Fauci lied about six-foot distancing and that “Everyone at the CDC and the regulatory agencies” lied about COVID-19 vaccine efficacy, specifically claiming the vaccine “would stop transmission” was false and that if vaccinated people contract and transmit the virus, “the virus stops with you” and they claim it “does not” stop with you. They say the FDA has “already admitted it,” and they call for people to “start asking people to show their work,” to seek evidence, and to “not trust experts any longer,” stating they have been lied to “long enough.” They express that they hope a documentary is not the last one and say they take interviews without concern about edits that could make them look “crazy,” because they believe viewers will agree. The speaker then discusses the “vaxxed versus unvaxxed study,” saying they have been addressing it “forever” and that they took a risk by agreeing to trust the study’s results if the other party published them. They say the CDC has “done this study a thousand times” in ways meant to prove vaccinators are healthier and “they can’t do it,” and they claim that results become “bad” when the study is done “the right way.” They describe an “inconvenient study” that they say is inconvenient for panelists, for the pharmaceutical industry that they say owns television stations, and for CDC leadership and HHS officials they claim were involved in “covering up the real science.” They conclude that people will “not take it anymore” and that they now have evidence “like they have never, ever had before.”

Senator Ron Johnson introduces Aaron Siri at the Kennedy Center, praising Siri as a highly consequential attorney and highlighting Siri’s work since the COVID era. Johnson recounts how his own oversight role in Congress evolved to rely on the adversarial legal process to extract information from a large government, noting that enforcement power rests in the courts. He frames Siri as someone who, through litigation and testimony, has exposed what he views as flaws in vaccine science, regulation, and safety oversight. Johnson describes Siri’s rise to prominence during the COVID period, beginning with public hearings on vaccine injuries in Milwaukee (June 2021) and Washington, DC (November 2021). He notes that Siri represented Dr. Patricia Lee, a physician who publicly discussed vaccine injection injuries and medical treatment obstacles, illustrating how federal health agencies and the CDC/FDA were perceived to respond to reports of injury. Siri’s testimony is credited with exposing calls to his practice from vaccine-injured doctors seeking treatment and the CDC/FDA officials’ defense of VAERS. Johnson highlights Siri’s 2022 and 2025 hearings, including the release of the VAERS data via the v-safe system, which Siri reportedly showed indicated higher rates of medical care sought and activity impairment among the vaccinated. Siri’s deposition of Stanley Plotkin and other experts is cited as foundational to his arguments about safety science, conflicts of interest, and the integrity of the vaccine schedule. Johnson points to the Institute of Medicine’s (IOM) conclusions as being insufficient to prove vaccine safety for the entire childhood schedule, and to Siri’s presentation of the Henry Ford study (vaccinated vs. unvaccinated children) showing higher rates of chronic illness among the vaccinated. A central claim Johnson attributes to Siri is that vaccines have immunity from liability, due to the National Childhood Vaccine Injury Act of 1986 (NCVIA). Siri’s summary is that vaccines are the only product in America with blanket liability protection for manufacturers and administrators, preempting design-defect claims via the Supreme Court interpretation that “the National Childhood Vaccine Injury Act preempts all design defect claims.” Siri argues this immunity removes the market incentive to develop safer vaccines and leaves safety oversight to federal health authorities (HHS agencies: NIH, CDC, FDA) rather than to private manufacturers. Siri’s account of the 1986 act is that it created a mandate for safer childhood vaccines, with three provisions: (1) the general rule placing the secretary of HHS in charge of vaccine safety; (2) a task force of NIH, CDC, and FDA to make safety recommendations to the secretary; and (3) a biannual report to Congress on actions to improve vaccine safety. Siri contends that the biannual reports have never been submitted, and the task force produced only one report (in 1998) before disbanding, with Secretary Kennedy recently reinstating the task force. Siri’s firm ICANN has filed FOIA requests and submitted recommendations to HHS about how to improve vaccine safety, asserting that the current safety framework is not adequate. Siri then surveys the landscape across federal agencies. He asserts that the absence of liability incentives undermines safety, citing industry-pricing and trial designs, and he presents specific examples of licensure trials for routine vaccines that he claims were inadequate by design. Examples include: - Hepatitis B vaccines (Recombivax HB and Engerix B): five days of safety monitoring in trials with 147 participants, according to package inserts and FDA reports he obtained; he notes a lack of long-term safety data and questions the adequacy of control groups. - Prevnar 7 and Prevnar 13 (pneumococcal vaccines): uses Prevnar 7 as a control for Prevnar 13; safety data show notable serious adverse events but are deemed acceptable for licensure; subsequent trials used Prevnar 13 as control for Prevnar 15 with continued concerns about safety signals. - DTaP vs DTP: claims DTP served as control and that DTP itself was not licensed on placebo-controlled trials; cites a Guinea-Bissau study showing higher mortality with DTP vaccination and other studies suggesting increased overall mortality with DTP. - Dengue vaccine: notes long-term, placebo-controlled data showing increased severe harm and death in certain age groups; argues that non-placebo, ethically problematic trial designs can mask safety issues. Siri asserts a categorical claim based on FDA licensure documents: not a single routine neonatal vaccine on the CDC schedule has been licensed based on a placebo-controlled trial; when another vaccine served as control, that control was never a placebo. He presents this as evidence that safety assessments were compromised, especially for early-life vaccines administered in the first six months. Regarding autism, Siri frames it as a litmus test for vaccine safety studies. He recounts IOM findings that were inconclusive about DTaP (and related vaccines) causing autism, citing the lack of sufficient studies and the absence of unvaccinated comparison groups in many analyses. He describes ICANN’s FOIA drive to obtain CDC studies showing vaccines do not cause autism, asserting that most of the CDC’s own 20-study list did not address the vaccines in question. In deposition clips, Siri indicates that the IOM and CDC have not produced adequate evidence to rule out a causal link for several injuries, and that the only mainstream “no autism” position has come under legal scrutiny when the agencies faced court-ordered settlements and deposition testimony. Siri concludes with reform recommendations across agencies: - FDA: remove conflicted personnel from vaccine safety reviews, require clear licensure standards, mandate proper controls and longer safety monitoring, require practitioner notification of trial details, and post pre-registered study protocols; regain transparency of de-identified health data. - CDC/HRSA: align vaccine injury compensation with statutory requirements; expand the VICP to cover more injuries; ensure the CICP is reformed and funded to reflect safety concerns; reduce conflicts of interest; promote alternative, non-pharmaceutical approaches for root causes of chronic illness. - NIH: limit pharma involvement in vaccine development, focus taxpayer-funded research on root causes and replication, and avoid patent-related partnerships that create conflicts. - CMS/HHS-wide: require automated VAERS reporting and public access to de-identified health data; ensure religious exemptions are preserved; depoliticize vaccines and end mandates as political tools; end chronic disease by addressing vaccines as a contributing factor to immune dysregulation. Siri closes by insisting that mandating vaccines is a political act that undermines informed consent, arguing that safety should be decoupled from politics and that safety and efficacy claims should be grounded in rigorous, transparent science. He emphasizes that informed consent, not mandates, should govern medical decisions.

The speaker challenges someone to debate vaccines, clarifying that they are not anti-vaccine but believe in safety testing. They criticize the lack of accountability for vaccine manufacturers and the exemption from safety testing. They argue that none of the 72 mandated vaccines have been tested against a placebo, making it uncertain if the benefits outweigh the risks. The Institute of Medicine has criticized the CDC for not conducting safety testing. The speaker highlights the increase in chronic diseases like autism and food allergies and questions the source if not vaccines. They conclude by urging people to look at vaccine inserts for information on epidemic diseases in children.

The speaker claims that no childhood vaccine has ever undergone a safety trial using a double-blind, placebo-based study. They assert that this type of study, involving a saline injection as a placebo, is the only way to determine the safety of a pharmaceutical product. Furthermore, the speaker states that there has never been a study comparing the health outcomes of children who receive the full schedule of 72 (or potentially up to 90) vaccines to those who receive none. Because of the lack of safety studies and comparative data, the speaker chooses not to inject themselves or their children with vaccines. They want evidence that vaccines are safe and make people healthier.

We couldn't find any prelicensing safety trials for the 72 vaccines doses that are recommended for American children. Unlike other medications, vaccines were exempt from conducting safety trials that compare health outcomes between a placebo group and a vaccine group. This lack of safety trials is concerning considering the widespread use of these vaccines.

We couldn't find a prelicensing safety trial for any of the 72 vaccines doses recommended for American children. Unlike other medications, vaccines were exempt from conducting safety trials that compare health outcomes between a placebo group and a vaccine group.

Big problem with trusting the science is not the science part, it's who's behind the science part, primarily in the area of vaccines for children. Normally, when you study a drug, you compare it with a placebo, so that way you can truly test the side effects on something, but that is not how they test children's vaccines. This so called placebo control is not really a true placebo control because it's not inert. It's an active vaccine with something called an adjuvant. The big one that they've been using for a long time is aluminum. My question is, how can you really truly test the safety and effectiveness of something if you're looking at the relative safety of an active vaccine to another active vaccine with adjuvants. That just muddies the water to this whole safe and effective claim that you keep hearing over and over and over.

Speaker 0: They argue that because the vaccine is classified as such, they don’t have to worry about being sued. They claim immunity from liability is dependent on there being no fraud, and there clearly was fraud. Speaker 1: They say there is fraud. They note that immunity from liability depends on fraud, and in light of that, it matters. They explain that there was fraud. Speaker 0: Expresses surprise and asks for caveats about fraud. Acknowledges there were caveats. Speaker 1: Confirms there is fraud and says it makes the situation more interesting. Speaker 0: Asks how fraud is defined, noting that drugs were sold with multiple studies and only one was good. Speaker 1: Responds with a point about safety testing for the mRNA vaccines. States that the insufficient safety testing was done before release, and that the product injected into billions of people involved DNA plasmids. There is massive contamination in the shots actually delivered, including the SV40 promoter from simian virus 40. The point is that safety testing for one drug was completed, but people were injected with something different that had other components that were not tested, which is described as fraudulent. Speaker 0: Requests an explanation of the SV40 issue for the audience. Speaker 1: Describes production techniques used to generate the product. Explains that a plasmid, a circular piece of DNA, was used to produce the product in vats, with bacteria performing the production, later coated in lipid nanoparticle. There is a requirement to purify DNA and set standards for DNA contamination, with limits that cannot be exceeded. In this case, the problem isn’t only poor quality control but that there was a more painstaking way to produce the same product that did not involve DNA plasmids at all. Consequently, leftover material in vials injected into people contained DNA contamination across the board. Kevin McKernan tested vials, finding DNA contamination in the samples. Speaker 1: Explains that the DNA left over includes the SV40 promoter, a genetic trigger from simian virus 40, which is known to be carcinogenic. Since this promoter is left in the vials from injections given to people, it challenges the claim that the mRNA shots could not integrate into the genome. While acknowledging that there are cellular processes such as reverse transcription, the speaker asserts that even the claim of “no DNA” is false because there is DNA in the vials, specifically DNA with the SV40 promoter, a genetic engineering tool with carcinogenic potential. The speaker concludes that this appears to be fraud: injecting a different product into the public on the basis of safety testing that was conducted with a product produced by a different process. Speaker 0: Reiterates the conclusion: you can’t inject a different product into the public on the basis of safety testing that was done with something produced by a different process.

The speaker states they searched for years for a pre-licensing safety trial of the 72 vaccine doses effectively mandated for American children. They claim that every other medication requires a safety trial comparing health outcomes in a placebo group versus a vaccine group before FDA licensing. The speaker assumed this was also done for vaccines. They state they found out that vaccines were exempt from this requirement.

The discussion centers on the claim that SIDS is a “vaccine death.” It states that seventy five percent of all deaths from SIDS happened within seven days of a vaccination. The conversation then shifts to polio. It references “Polio, forty eight hour safety review trial” and says the safety review lasted “forty eight hours, two days.” It also brings up President Roosevelt, described as “famous for having polio in the wheelchair,” and adds that he “had transverse myelitis.” A response rejects the polio framing: “No way. Didn’t have polio.” The speaker disputes trust in doctors’ knowledge of vaccines, saying, “How can you sit here and say doctors don’t know anything about vaccines?” Another claim follows that “a doctor is lucky if they have a half a day education on vaccines,” and that “I have yet to find a pediatrician that can list the ingredients of any vaccines.” The speaker further asserts, “They don’t know anything at all.” A broader argument is made about vaccine testing and timing for children. The speaker claims that “99.5 of our children are getting a product that was tested for five days” and says this product was tested “for a disease they will not come in contact with until they’re an adult.” The speaker adds “and hopefully never,” linking this to a belief about later behavior: “if they were raised correctly, will find themselves sharing heroin needles or sleeping with prostitutes.” The conclusion of the argument is presented as a belief that uncovering these “truth” points will expose broader wrongdoing: “I do believe when people see the truth on this, it will reveal everything that’s corrupt about the world that you live in.”

If regulatory agencies continue to rush products to market without long-term safety trials, the planet is in danger. The speaker questions what would happen if a vaccine wipes out fertility. They state that no childhood vaccines on the schedule have gone through randomized, double-blind, placebo-controlled trials. The speaker finds it alarming that Dr. Martin Macri's statement that no future vaccine will be licensed without a proper randomized controlled placebo trial is shocking to some. They accuse mainstream media of spreading misinformation by denying the absence of placebo trials, then admitting it to avoid delaying vaccine advancement. The speaker asserts the pharmaceutical industry has lied about drugs like Fenben and Vioxx and is now making vaccines. They call for accountability from the industry and the media, warning of grave danger if this does not happen. They disapprove of five-day safety trials with no placebo, especially for products given to healthy children.

According to the speaker, vaccines have never been tested in a randomized, placebo-controlled trial to evaluate their safety. The speaker claims that vaccines contain aluminum compounds because many dead vaccines don't mount an immune response without them. The speaker alleges that in a Gardasil vaccine study, the placebo group received an aluminum adjuvant instead of a true placebo, so the side effect profiles of the active vaccine and placebo groups were the same. The speaker asserts that Merck used a novel aluminum compound and that data shows aluminum in vaccines is toxic. The speaker states that the only completely randomized controlled trial was on sheep using a vaccine for blue tongue disease. The speaker claims the aluminum was toxic, the sheep became sick, their behavior changed, and many died compared to the placebo group. The speaker concludes that the presumption that aluminum as an adjuvant is safe is unfounded and has never been tested.

Speaker 1 states that no vaccines, including the COVID vaccine, have been properly tested. They claim that no childhood vaccine has undergone a placebo-controlled clinical trial of sufficient duration and power to assess its safety before being injected into millions of children in America. Speaker 1 asserts this is not an opinion, but can be verified by anyone reviewing package inserts and clinical trial documents on the FDA website.

Speaker 0 questions Speaker 1 about the lack of clinical trial data for the MMR vaccine. Speaker 1 insists that the vaccine was extensively tested before being licensed and that millions of doses have been used. Speaker 0 asks for proof of pre-licensure clinical trials, but Speaker 1 only refers to a book and mentions studies done in the 1960s. Speaker 0 argues that the data provided is not sufficient and questions the absence of a placebo group. Speaker 1 admits uncertainty about the inclusion of control groups but maintains that safety assessments were conducted. Speaker 0 concludes that no randomized placebo-controlled study exists for the MMR vaccine. Speaker 1 agrees to provide additional information after the deposition.

None of the vaccines, including the COVID vaccine, have undergone proper testing. No childhood vaccine has completed a placebo-controlled clinical trial with sufficient duration and power to confirm its safety before being administered to millions of children in America. This is not an opinion; it can be verified by anyone visiting the FDA website, where the package inserts and clinical trial documents are available for review.