“We do not believe any group of men adequate enough or wise enough to operate without scrutiny or without criticism. We know that the only way to avoid error is to detect it, that the only way to detect it is to be free to inquire. We know that in secrecy error undetected will flourish and subvert.” –J. Robert Oppenheimer
The above image of a vintage Rolodex is courtesy of CSA Images via Google Images.
Health Friday is a series devoted to information about Big Pharma, vaccines, general health, and associated topics. As today’s post speaks to the disaster of COVID-19 (the COVID-19 virus itself, and the COVID-19 “vaccines”), Yours Truly dedicates it to the memory of all persons, of whatever age or location, who have passed away from the negative effects of these lab-created bioweapons.
There are Important Wolf Moon Notifications; the Rules of our late, good Wheatie; and, certain caveats from Yours Truly, of which readers should be aware. They are linked here.
And now, Part Two of the COVID-19 Information File:
BOOKS: One: Cancer Care, Second Edition. By Dr. Paul E. Marik, MD, FCCM, FCCP (Dr. Marik is a co-founder of the FLCCC Alliance). This book is found on https://www.amazon.com/.
Two: The Doctors Book of Home Remedies, by the editors of Prevention Health Magazine Books, 1990 edition. This book is available online as used copies.
WEBSITE NAME CHANGES:
The FLCCC Alliance (formerly https://covid19criticalcare.com, also called FLCCC Alliance) is now Independent Medical Alliance: https://imahealth.org/.
COVID-19 VIRUS and COVID-19 “VACCINES” DETOX / MITIGATION PROTOCOLS:
https://imahealth.org/ (Independent Medical Alliance, formerly FLCCC); https://americasfrontlinedoctors.org/ (AFLDS); https://www.mercola.com/ (Dr. Joseph Mercola, MD; must sign up to access); https://www.americaoutloud.com/ (Dr. Peter McCullough, MD’s, Wellness Company site.) Note: this is not an exhaustive list, and does not include herbal medicine, naturopathic medicine, homeopathic medicine, Ayurvedic medicine, Traditional Chinese Medicine, or other allopathic / osteopathic websites.
THE YALE “LISTEN” STUDY PAPER:
Yours Truly has written on the main discussion thread several times regarding this groundbreaking paper (the “Iwasaki et al. paper”) about COVID-19 “vaccine”-induced injuries presenting as long as 709 days after “vaccination.” Here is Steve Kirsch’s take on the paper: https://kirschsubstack.com/p/covid-vaccine-injury-study-published, “COVID vaccine injury study published on preprint server because the mainstream medical journals refused to publish it”, 19 February 2025. HOWEVER, Yours Truly has found that the original preprint paper has already been reissued in a “new” preprint version. The original version is found here: https://www.medrxiv.org/content/10.1101/2025.02.18.25322379v1, “Immunological and Antigenic Signatures Associated with Chronic Illnesses after COVID-19 Vaccination”, Akiko Iwasaki, et al., dated 18 February 2025. The “new” preprint version is found here: https://www.medrxiv.org/content/10.1101/2025.02.18.25322379v2.full, same title, Akiko Iwasaki, et al., dated 25 February 2025. Meanwhile, Dr. Pierre Kory, MD, has written a blog post regarding how the LISTEN study may be used as legal support for persons with COVID-19 “vaccine”-induced issues in lawsuits: https://pierrekorymedicalmusings.com/p/new-study-provides-legal-support, “New Study Provides Legal Support For The Vaccine Injured”, 21 February 2025. Dr. Kory has coined the term, “Post Covid Vaccination Syndrome”, or PVS, to describe the conditions and issues that COVID-19 “vaccinated” patients in his practice present.
MORE INFORMATION ON HOW THE COVID-19 “VACCINES” INCREASE THE IgG4 “TOLERATE BUT NEVER CLEAR” IMMUNE SYSTEM CELLS IN THE “VACCINATED” PERSON’S BODY:
The following screenshot is from the 2015 FDA guidance document on gene therapies:
The following screenshots are via FOIA information that Judicial Watch sued the FDA for and won regarding the Pfizer-BioNTech “flagship” modRNA COVID-19 “vaccine”, BNT162b2:
COVID-19 BTI (Bioweapon Toxin Injections, aka the “vaccines”) AND ORAL COVID-19 “VACCINE” NEWS:
One: The European Commission has just approved the use of the self-amplifying RNA (saRNA) COVID-19 “vaccine”, KOSTAIVE, for use in the European Union / Scandinavia. Please see: https://defender.substack.com/p/europe-approval-self-amplifying-covid-mrna-vaccine-no-long-term-safety-data, “Inhumane, Reckless: Critics Weigh in on Europe’s Approval of Self-Amplifying COVID mRNA Vaccines”, by Suzanne Burdick, PhD, 23 February 2025. KOSTAIVE is the brand name of the injectable called ARCT-154, by Arcturus Therapeutics. This product was approved in Japan in November 2024 and is in use there. Below are two screenshots from the Defender article:
Please re-read the sentence above from Dr. Jablonowski regarding how an saRNA COVID-19 “vaccine” is “like being vaccinated every day for the rest of your life.” (Italics mine)
One of the blogs that Yours Truly reads regularly is that of Walter M Chesnut: https://wmcresearch.substack.com/. Mr. Chesnut has been performing solid research into the mechanisms of the spike protein of the SARS-CoV-2 (COVID-19) virus itself for over 3 years. While it is not known for absolute certainty the actual ingredients of the lab-created bioweapon called the SARS-CoV-2 virus, Mr. Chesnut continues to find possible pieces of this puzzle. Here are two recent such blog articles of his. The first: https://wmcresearch.substack.com/p/turbocancers-a-secondary-manifestation, “Turbocancers: A Secondary Manifestation of the Extracellular Matrix (ECM)?” The second: https://wmcresearch.substack.com/p/the-spike-protein-and-iib3-understanding, “The Spike Protein and [alpha]IIb[beta]3: Understanding the Fibrous Clots from an Integrin-Mediated Perspective”, 24 February 2025. A screenshot from this article is below:
The point here is that the COVID-19 virus itself it NOT “just another virus.” It is a lab-created bioweapon that, in and of itself, can damage the infected person’s body. Combined with the “enhanced” ingredients found in the COVID-19 “vaccines” (lipid nanoparticles and N1-methylpseudouridine), this “foundational” bioweapon virus becomes extremely dangerous or even deadly. (NOTE: Yours Truly apologizes for the [alpha] and the [beta] in the title of the Chesnut article cited above. She is still in the WP “learning curve.”)
FLASH! UPDATE 6 MARCH: REGARDING THE “DISCOVERY” OF THE “NEW” BAT CORONAVIRUS, HKU5-CoV-2:
This “new” bat coronavirus was supposedly “discovered” by the Wuhan Institute of Virology. The first question this raises is: How many OTHER bat (or other) coronaviruses are in the “storage vaults” of the WIV to be “discovered” at some point? There is speculation all over the internet regarding HKU5-CoV-2 and if / when, it could infect humans. This “new” coronavirus apparently can use the same types of entry methods into the human body that SARS-CoV-2 and MERS do.
Two: But wait, there’s more! Another question is raised: What did / does, Pfizer-BioNTech know about HKU5-CoV-2? Because this company has been Phase 1 testing an “experimental” modRNA “Pandemic Influenza vaccine” since December 2023. The study is NCT06179446 (https://clinicaltrials.gov/study/NCT06179446), begun on 13 December 2023 and scheduled to finish the Phase 1 clinical trial on 26 August 2025. This “experimental” modRNA prophylactic “Pandemic Influenza vaccine” is called pdmFlu. The Pfizer-BioNTech product identifier number is PF-07985819, and the Study Identifier number is C5561001. According to the “Researcher View” of the Clinical Trials entry, as many as eight different formulas and/or dosage amounts will be given to the study participants (there are 160 registered study participants.) NCT06179446 has two separate “control groups”: One “control group” will receive injections of a “licensed influenza vaccine”; the other “control group” will receive a placebo.
WHAT DID / DOES, PFIZER-BIONTECH KNOW ABOUT HKU5-CoV-2?
Three: And, by the way — RALPH BARIC has been experimenting with HKU5-CoV-2 SINCE AT LEAST 2014, funded by the NIH. One of his papers is here: https://pmc.ncbi.nlm.nih.gov.articles/PMC7022341/, “Trypsin Treatment Unlocks Barrier for Zoonotic Bat Coronavirus Infection”, Ralph S. Baric, et al., 14 February 2020.
WHAT DOES / DID RALPH BARIC KNOW ABOUT HKU5-CoV-2?
The above image of lab equipment is courtesy of Google Images and Public Domain Pictures.
Today’s offering for Health Friday concerns what is called self-amplifying RNA (saRNA.) As the presentation includes discussion of saRNA COVID-19 “vaccines”, this post is dedicated to the memory of Yours Truly’s cousin Bill, who “died suddenly and unexpectedly” in September 2023.
Readers already know about the Important Wolf Moon Notifications, the importance of Civil Discussion, the Rules of our late, good Wheatie, and the caveats regarding Health Friday posts by Yours Truly. Links to these items can be found here. NOTE: Since this post is detailed and there are multiple areas to cover, Yours Truly has added Summaries of certain sections, and a General Summary at the end.
Before one begins: It is well known that the modRNA and the viral vector COVID-19 “vaccines” currently in use have been, and are, a disaster on multiple fronts. Not only do they induce literally thousands of negative medical and psychological effects in the bodies of those who took them and who take them now; these “vaccines” also cause death. The numbers of COVID-19 “vaccinated” persons presenting with COVID-19 “vaccine”-induced illnesses, injuries, disabilities, or “died suddenly and unexpectedly” are increasing by the month. Nobody knows exactly how long, or in what amount, the elements and mechanisms of the COVID-19 “vaccines” work in the “vaccinated” person’s body: what IS known, is that whatever “protection” is conferred by these “vaccines” is short-lived, while, at the same time, the “vaccine” mechanisms linger on in the body for an indeterminate period of time. Yours Truly has written extensively for this board regarding this situation. For further information, please see websites such as these: https://kirschsubstack.com/ (Steve Kirsch); https://petermcculloughmd.substack.com/ (Peter McCullough, MD); and, https://phinancetechnologies.com/HumanityProjects/Projects.htm#Nav_ExcessDeaths (Ed Dowd, statistician.)
At the same time, the development of new types of COVID-19 “vaccines”, as well as new types of “vaccine delivery” (intranasal, oral, and aerosol, for examples) goes on apace. One of the “newest” types of COVID-19 “vaccines” uses what is called self-amplifying RNA, or saRNA.
The concept of saRNA is the use of a small amount of RNA (or mRNA) in an injectable. Once introduced into the body of the patient, the saRNA theoretically goes to work, “re-creating itself.” (Think RNA or mRNA being turned into a “Xerox copier” inside the “vaccinated” person’s body.) The “goal” of saRNA is for the agent to “re-create itself” inside the “vaccinated” person’s body for a certain amount of time and in some amount. The patient’s body is “instructed” by the saRNA to “recognize” and produce antibodies against certain “enemies”, such as viruses. The theory is that a smaller amount of saRNA initially introduced into the body, followed by the “Xerox copier effect”, then followed by “instructing” the body to “recognize” and fight off certain “enemies”, will make saRNA a “more effective use” of mRNA in injectables.
Basically,saRNA COVID-19 “vaccines” turn the “vaccinated” person’s body into a “Xerox copier” (which, apparently, the “vaccinated” person’s body CANNOT stop, slow down, or mitigate) for the ingredients (and, by extension, the mechanisms) of the saRNA “vaccine.” Today’s post is a primer about saRNA COVID-19 “vaccines.”
****** Summary: In other words, saRNA injectables **may**, at some point down the road, have **some** benefits. In the meantime — NONE of these types of injectables (GEMCOVAC, Kostaive) have been SUFFICIENTLY AND THOROUGHLY INVESTIGATED AND TESTED FOR USE ON HUMANS. But they are being approved ANYWAY, and are being injected into the bodies of unsuspecting persons who buy into the “Look, this shot has less mRNA than the ones you took before, and it’ll work better!” hype.
****** Look closely at the above graphic. It appears that the basic schema of saRNA is a “double-layer” of saRNA “replicons” that create a “subgenomic RNA.” This, in turn, creates the “Xerox copier” response which forces the body of the saRNA “vaccinated” person to endlessly produce immune system response— and for “at least” as long as 28 days after such “vaccination.”
Please see this paper regarding a discussion of saRNA “vaccine” design: https://doi.org/10.1016/j.tibtech.2023.05.007, “Rise of the RNA machines — self-amplification in RNA vaccine design”, Jerome D.G. Comes, et al., 14 June 2023. Below is the Abstract of this paper:
Note the language about “,…at least in theory” advantage of saRNA “vaccines.” Also note the last sentence — saRNA can “persist for a month.” In fact,nobody really knows how long saRNA elements will “persist” in the body of the person who takes this type of “vaccine” — NO long-term clinical trial or study has been performed using this technology.
On 28 November 2023, the Japanese Government approved the use of the saRNA COVID-19 “vaccine”, ARCT-154 (also called LUNAR-COVID-19 and Kostaive) for “active immunization” (translation: “prevention”) against COVID-19 for persons age 18 and older. Kostaive was developed by CSL / Arcturus (remember this company? Yours Truly took the lid off it here: www.theqtree.com/2024/08/02/the-hhs-gave-the-go-ahead-to-use-an-h5n1-vaccine-but-the-ama-just-issued-new-cpt-codes-for-an-h5n8-vaccine/.) This “vaccine” was to have supplies ready for administration by physicians or hospitals by mid-December 2023.
CSL / Arcturus, the Japanese government, and media outlets were quick to herald this “first-ever saRNA COVID-19 “vaccine.” Except — there already was an saRNA COVID-19 “vaccine” approved and in use, since 2022, in India: GEMCOVAC. Perhaps what CSL / Arcturus, the Japanese government, and media outlets should have mentioned the fact that Kostaive is modRNA-based from the J.1. Omicron SARS-CoV-2 variant (along with other “familiar” manufacturing methods, see below in today’s post); whereas GEMCOVAC based on an “ancestral variant” (in other words, the Beta variant) of the original Wuhan Hu1 SARS-CoV-2 virus.
Before Yours Truly presents information on Kostaive, she will first discuss GEMOCOVAC. This is in order to present further background information on saRNA technology as applied in COVID-19 “vaccines.” Stay with me — this is all germane to the situation:
Looking at GEMCOVAC, one can get the beginning of a picture of how saRNA COVID-19 “vaccines” work. The “latest version” of this “vaccine” is called GEMCOVAC-OM. Below is a portion of the SmPC pdf for this product (https://gemcovac.com; scroll down the page to GEMCOVAC-OM SmPC (pdf) and click “Download”):
The BA.1. Omicron variant of SARS-Co-V-2 is the basis for this “vaccine.” It is not strictly modRNA (however, recall that ALL of the “descendant variants” of the original Wuhan Hu1 SARS-CoV-2 virus contain elements of that original lab-created virus).
Of the excipients (in other words, the adjuvants): per Wikipedia, DOTAP (1,2-Dioleoyl-3-trimethylammonium propane) is a chemical used in fabric softeners, but also is used as a lipid nanoparticle in vaccines. Squalene: below is Page 1 of the FisherScientific MSDS Safety Data Sheet for this chemical (www.fishersci.com/):
Continuing: for polysorbate 80, again from Fisher Scientific, Page 1 of the MSDS Safety Data Sheet:
And, here is the Mechanism of Action for GEMCOVAC-OM, from the Package Insert (see the link above):
Note the language, “…which is reported to interact with host cells receptors (ACE-2.)” (Italics mine.) The developer and manufacturer (GENNOVA) of this “vaccine” can’t exactly quantify how the product works.
Yours Truly now turns to Kostaive, (ARCT-154) the saRNA COVID-19 “vaccine” that was approved by the Japanese government in November 2023.
Note the language in the above regarding “…the potential for extended duration of protection while using lower doses of mRNA compared to existing mRNA vaccines.” (Italics mine) Again, nobody knows exactly how long this “extended duration” period is; nobody knows exactly how much “Xerox copying” of the altered mRNA in Kostaive occurs during this period in the “vaccinated” person’s body; and, nobody knows exactly what effects this “Xerox copying” of the altered mRNA in Kostaive will have in the “vaccinated” person’s body. In other words, anyone who takes Kostaive, or any saRNA “vaccine”, in Yours Truly’s opinion, is being used a “human lab rat” — just as people were used / are still being used, as “human lab rats” for the modRNA COVID-19 “vaccines.”
And, here is the Report of the Deliberation Results (which contains the information about Kostaive that led to its approval) from the Japanese Ministry of Health, Labour, and Welfare: www.pmda.go.jp/files/000269813.pdf. This report is an interesting read. There are numerous “blacked-out” areas, reminding one of the blacked-out areas in certain publicly-released Pfizer-BioNTech reports that the company gave to the FDA regarding that company’s modRNA COVID-19 “vaccine” BNT162b2. HOWEVER, section 2.1 Active Substance for Kostaive states that this saRNA “vaccine” contains elements from the original Wuhan Hu1 SARS-CoV-2 virus, plus elements from the Omicron variant strain. More information on this is found on Page 4 of the document. Below is a portion of this page:
Looking at the above, starting with the D614G mutation, the Abstract from the Zhang, et al. paper on this (https://doi.org/10.1038/s41467-020-19808-4, “SARS-CoV-2 spike-protein D614G mutation increases virion spike density and infectivity”, Lizhou Zhang, et al., 26 November 2020. The paper was researched and published before any COVID-19 “vaccine” was authorized for use):
In other words, the D614G element causes the SARS-CoV-2 virus to be more infective.
Looking at V987P, part of the section Full-Length S Glycoprotein Vaccines from this paper: https://doi.org/10.3389/fimmu.2021/701501, “SARs-CoV-2 Vaccines Based on the Spike Glycoprotein and Implications of New Viral Variants”, Daniel Martinez-Flores, et al., 11 July 2021):
In other words, if V987P was “good enough” for Pfizer-BioNTech and for Moderna to use in their modRNA COVID-19 “vaccines”, it apparently was “good enough” to be used in Kostaive.
The K986P protein used in Kostaive: please see here: www.rcsb.org/structure/6zp1. This viral protein, along with V987P above, are BOTH on the Arg S1/S2 cleavage site on the SARS-CoV-2 virus genome. (FURIN CLEAVAGE SITE, anyone?)
The R682G, R683S, and R685S proteins used in Kostaive: please see here: https://doi.org/10.1038/s41467-022-32665-7, “Omicron SARS-CoV-2 mutations stabilize spike-up RBD conformation and lead to a non-RBM-binding monoclonal antibody escape”, Zhennan Zhao, et al., 24 August 2022. If appears that these proteins help to create a “one-RBD-up conformation.” Below is a portion of the Abstract of this paper:
In other words, these proteins increase the immune system attack from the Omicron SARS-CoV-2 variants by making Omicron “stick better” to the ACE2 receptor cells in the human body.
****** Summary: It appears, then, that Kostaive contains one protein from the original Wuhan Hu1 SARS-CoV-2 virus genome (D614G); two proteins from the “ancestral line” of the SARS-CoV-2 virus (K986P and V987P); and three proteins of the Omicron SARS-CoV-2 variant (R682G, R683S, and R685S.) See below in the post for more information on these items.
One more ingredient of Kostaive, mRNA-2105: This ingredient is derived from the Venezuelan Equine Encephalitis virus (VEEV.) Below is section 4.R.1. of the Deliberations Results document discussing this:
The question that immediately occurs regarding the above: How can Arcturus (the manufacturer of Kostaive) state that mRNA-2105 cannot be “incorporated into host cell DNA”? How is Arcturus absolutely sure that there is zero reverse transcription potential or ability in Kostaive? This is similar to the same statements from Pfizer-BioNTech about BNT162b2 “cannot change the DNA of the vaccinated individual” — which has been proven to be false (please see: here, Slide 14.)
****** Summary of the above: What Yours Truly is getting at here is that Kostaive appears to be the end-product of: ONE: a lab-created mixture of the dangerous D614G element from the original Wuhan Hu1 SARS-CoV-2 virus, plus, various elements of earlier SARS-CoV-2 mutations; TWO: NO long-term clinical trials, NO safety studies for Toxicity, use on pregnant women, etc.; THREE: the “Process 2”-type manufacturing method (“culturing” the lab-enhanced mRNA for the “vaccine” in a “bath” of E. coli); FOUR: using lipid nanoparticles, one of which (ATX-126) has never been used before in an injectable); FIVE: what appears to be a “pro-forma” Deliberation Results document on Kostaive that raises more questions than it answers; and, SIX: approval by the Japanese government for use on humans without a thorough investigation of the above. Related to point SIX: below is the list of Approval Conditions that were imposed along the approval of Kostaive for use in Japan, from the Deliberations Results document:
By the way, these Approval Conditions read very much like the ones that the FDA imposed on Pfizer-BioNTech along with that agency’s EUA for BNT162b2.
Regarding Kostaive itself, more particulars:
The ingredients of Kostaive are listed in section 2.2 Vaccine Product of the report. A screenshot of this section is below:
Kostaive contains at least three separate types of LNPs (lipid nanoparticles): ATX-126; DSPC; and, PEG2000-DMG. Below is a portion of the MSDS Safety Data Sheet for ATX-126:
Section 2.2.3 of the Deliberation Results document for Kostaive discusses the manufacturing process for Kostaive. It appears that Kostaive ALSO “switched” from a “Process A” manufacturing method over to a “Process B” manufacturing method. (Recall that the Pfizer-BioNTech BNT162b2 was “switched” from its “Process 1” manufacturing method over to a “Process 2” manufacturing method):
One more item from the Deliberation Results document for Kostaive, again on the ATX-126 lipid nanoparticle used in this “vaccine.” It confirms that this “novel excipient” (adjuvant) has not been used before in a “vaccine.”
Yours Truly will again emphasize that other sections of the DeliberationResults document on Kostaive make it clear that NO studies were performed for numerous items, such as Toxicity, potential for impairment of reproduction, and so on. By the way, buried in the document is a “passing reference mention” that the “Process B” manufacturing method for this “vaccine” uses E. coli as the “culturing medium” for the “enhanced” mRNA in the product. (The “Process 2” manufacturing method for BNT162b2 and its “descendant” COVID-19 “vaccines” also uses E. coli.) It also appears that the use of Kostaive on pregnant women in clinical trials was “inconclusive”; this “vaccine” should be taken by pregnant women only if the situation so warrants.
Also: Kostaive is to be taken as a “primary series” of two separate injections, 28 days apart; with a “booster” taken about three months later. The question that arises is: If it is true that the saRNA in Kostaive is active, including installing numberless “Xerox copiers” of itself in the “vaccinated” person’s body for AT LEAST 28 days AFTER the initial injection, WHY is there a need for ANOTHER injection around Day 28? And a “booster” after that?
******BUT — AND THIS IS A HUGE BUT — TAKE ANOTHER LOOK AT SECTION 2.2.1 OF THE DELIBERATION RESULTS DOCUMENT FOR KOSTAIVE:
Look at the “active ingredient” item, “zapomeran.” What is zapomeran? It is a “drug” that contains the RNA of the Venezuelan Equine Encephalitis Virus (VEEV or VEE) in an saRNA form. It is ALSO manufactured by ARCTURUS (CSL.) It is unclear if it is being used in other types of COVID-19 “vaccines” other than Kostaive. Please see: https://synapse.patsnap.com/drug/510bcf7ef75649278b284a94663c69f6. Scroll down the page to R&D Status to see that zapomeran has already been approved in the EU; Norway; Iceland; and Liechtenstein; but in what final form it is used, is also unclear. NOTE 1: It has been impossible to find a complete list of ingredients for zapomeran. One would not be surprised to learn that the names Kostaive and zapomeran may, in some respects, be “interchangeable.” NOTE 2: It is not easy to find information on zapomeran. Yours Truly has encountered “504 Bad Gateway” error messages when going back to recheck a couple of the links to zapomeran in this post.
Looking further into VEEV (or VEE), there is this article: https://ceh.vetmed.ucdavis.edu/health-topics/venezuelan-equine-encephalitis-vee, by Amy Young, 28 August 2020. This virus can affect horses, donkeys, or zebras. VEEV is transmitted to these animals by infected mosquitos that bite them. It can cause severe disease or death by infecting the brain and the central nervous system. Humans who contract VEEV can also become severely ill and can also die from it. Another paper, discussing the RNA of VEEV (VEE),by Sarah E. Hickson and Jennifer L. Hyde, is here.
****** VERY IMPORTANT:The SARS-CoV-2 spike proteins in zapomeran are the same ones that are in Kostaive. These were discussed above in the post. Turning to the nsP proteins (non-structural proteins) in zapomeran (hyperlinks to papers are embedded), as these elements are also apparently contained in Kostaive:
****** SUMMARY:IT APPEARS, THEN, THAT KOSTAIVE CONTAINS ZAPOMERAN, WHICH INCLUDES THE VENEZUELAN EQUINE ENCEPHALITIS RNA; PLUS, SIX LAB-ENHANCED/LAB-ISOLATED GENOME CODES OF SARS-CoV-2; AND, FOUR NON-STRUCTURAL PROTEINS, ONE OF WHICH IS A ROTAVIRUS TOXIN. KOSTAIVE ALSO CONTAINS DANGEROUS LIPID NANOPARTICLES (SUCH AS ATX-126.) THESE ARE ALL PRESENT IN THIS saRNA COVID-19 “VACCINE” PRODUCT. RECALL THAT LIPID NANOPARTICLES WILL HELP TO SPREAD A “VACCINE” THROUGHOUT THE ‘VACCINATED” PERSON’S BODY, INCLUDING CROSSING THE BLOOD-BRAIN BARRIER.
Why on Earth is a COVID-19 “vaccine” that contains the RNA of an equine brain inflammation virus (a virus that comes from infected mosquitos that bite equine animals) being used on humans? A “vaccine” that is engineered to create an unknown number of “Xerox copiers” of the “vaccine” elements into the body of the “vaccinated” person? A “vaccine” that contains six apparently lab-enhanced/lab-isolated genome codes from the SARS-CoV-2 virus or its variants? What does an equine brain inflammation virus have in common with SARS-CoV-2? What if a person who has already taken, say, five or six injections of a modRNA COVID-19 “vaccine” decides to take Kostaive? Could an saRNA COVID-19 “vaccine” somehow “interact” with the modRNA COVID-19 “vaccine” elements already in that person’s body?
****** GENERAL SUMMARY: saRNA “vaccines” for COVID-19 are already being used (GEMCOVAC in India); and are being approved for use (Kostaive in Japan.) The technology for saRNA is not fully developed and not fully tested; the COVID-19 “vaccines” that use saRNA contain “lab-enhanced”/”lab-isolated” genome codes of the SARS-CoV-2 virus or its variants; saRNA COVID-19 “vaccines” contain lipid nanoparticles — and, in the case of Kostaive, an LNP (ATX-126) that has never been used before in an injectable; that no studies have been performed on saRNA COVID-19 “vaccines” regarding Toxicity, the effects on reproductive potential, and so on; and, that Kostaive contains the RNA of the Venezuelan Equine Encephalitis Virus. And yet, these products are being hailed as “the vaccines of the future.” And, the people taking them are again being used as “human lab rats.”
