SASHA LATYPOVA'S clarion call, her cry out (with a French colleague Helene Banoun) to Protect Babies from the Injection of Beyfortus (RSV monoclonal) is word the read! injection of Beyfortus
(nirsevimab, a monoclonal antibody against bronchiolitis caused by RSV) is recommended for all newborns from maternity ward. not been tested on newborns, but on children aged between 3 months- 2 years
Start Sasha here:
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Here are changes that were made to the CDC childhood vaccination schedule for 2024:
Helene Banoun is a pharmacist-biologist, former INSERM researcher, based in France.
She writes in an email:
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Since December 6, when I alerted the public about the French government's uncontrolled clinical trial, Twitter France has made me invisible. In France, the injection of Beyfortus (nirsevimab, a monoclonal antibody against bronchiolitis caused by RSV) is recommended for all newborns from the maternity ward. This treatment has not been tested on newborns, but on children aged between 3 months and 2 years!
French whistleblower calculations demonstrate the existence of a very significant increase in the number of deaths of babies aged two to six days, two months in a row, exactly since the introduction of this “preventive monoclonal therapy against bronchiolitis” (Beyfortus®) which has never really been tested in newborns.
It seems that Twitter has activated the "hide Hélène Banoun's tweets" feature for many subscribers https://twitter.com/BanounHelene
“The unpleasant surprises of RSV bronchiolitis vaccines and preventive therapies.”
by Helene on Researchgate here.
Some excerpts from the paper [numbered references are in the linked paper]:
Monoclonal antibody preventive therapies?
A new concept is emerging in the fight against bronchiolitis: preventive therapy involving direct injection of antibodies. In collaboration with Astra-Zeneca, Sanofi is marketing a monoclonal antibody against RSV, Beyfortus, for preventive injections in newborns. One of the clinical trials [1] showed serious adverse reactions to the vaccine, with 3 deaths in the vaccinated group versus 0 in the placebo group. According to the ritual formula, "deaths are not attributed to the vaccine by the investigator".
The FDA recorded 12 deaths in all trials of this monoclonal antibody [2]: 4 cardiac deaths, 2 gastroenteritis, 2 sudden deaths, 1 cancer, 1 Covid, 1 fracture, 1 pneumonia, but no deaths were linked to treatment.
The EMA recorded 3 deaths in the placebo groups and 11 deaths in the treatment groups. EMA conclusion: the benefit/risk balance is positive...[3].
The HAS (Haute Autorité de Santé, High Health Authority, France) also stresses the absence of any data to support a possible impact on reducing hospitalization times or mortality, and also notes deaths as a possible adverse effect [4].
Let's not forget that this whole bronchiolitis "prevention" campaign is supposed to avoid overcrowding hospitals with babies suffering from this disease: if this product doesn't significantly reduce hospitalizations, what's the point?
In its September 2022 report [3], the EMA reminds us of the fiasco of RSV vaccine trials in the past: children died of severe bronchiolitis in the vaccinated groups and none in the control groups.
This is yet another manifestation of the ADE (antibody-mediated facilitation/aggravation of infection) described for Dengue fever [5]. This ADE is due to the deleterious effect of antibodies which, instead of neutralizing the virus, facilitate its entry into the cell via the receptor of the Fc fragment of immunoglobulins.
And it's precisely this Fc region of Nirsevimab (the generic name for Beyfortus) that industry has seen fit to modify: the Fc of this antibody has a higher affinity for the neonatal Fc receptor, in order to extend its lifespan.
Note - how coincidental! Very similar design approach was taken simultaneously by ALL covid vax manufacturers: select the most toxic component of the target “pathogen” to make it the design element of their product. It appears to be the new-new fashionable trend in drug development. Let’s make it REALLY dangerous.
The EMA reminds us that the role of this Fc fragment in "protection" against the RSV virus cannot be ruled out. As I explained [6], different names are given to the same phenomenon, depending on whether it's considered beneficial (ADCD, ADNKA, ADCP, ADNP) or deleterious (ADE): it's always an entry of the virus into the cell facilitated by the Fc fragment of the antibody. Manufacturers are looking for the beneficial effects of this phenomenon and are wary of deleterious effects, which is why they have investigated the risk of ADE with Beyfortus in animal models. They claim not to have detected it, but the EMA points out, unmoved, that no histopathological evaluation of rats was carried out after treatment and infection with RSV: this is the only recognized marker of ADE.
The EMA reassures us that no signs of ADE have been observed in clinical trials: really? However, bronchiolitis was reported as the cause of death in infants in the treated groups; these deaths were not attributed to the treatment by the investigator. To be able to confirm this, these poor babies would have had to be autopsied and checked for histopathological phenomena in the lungs: this was not done, and the EMA was careful not to ask for it. It is therefore to be feared that this monoclonal antibody, whose Fc fragment has been modified, could cause this dangerous ADE effect in certain infants, which would explain the imbalance in deaths in the treated group compared to placebo, but also the same imbalance compared to the group treated with Synagis (palivizumab), the former equivalent drug which did not have this modification of the Fc fragment [7]!
An article in French press (auto translation to English available) “The Beyfortus train has already derailed.” Shows the following grim statistics:
The blue curve represents, for each month (from 2018 to October 2023), the mortality rates of 2 to 6 days of life, of the native babies of the month in question.
The horizontal green line represents the reference rate, calculated over the years 2018-2019. This rate is 0.69 deaths per 1,000 births.
The blue dotted lines represent the’ confidence interval of the mortality rates at 95 %.
The red dotted lines represent the’ confidence interval of the mortality rates at 99.8 %.
As of September 2023, there are 54 infant deaths between 2 and 6 days of life out of 55,489 births, what gives a mortality rate of 0.97 deaths per 1,000 births.
White House Confirms 230,000 Additional RSV Immunization Doses for Infants Next Month.
France is the world's testing ground for this product, which will now be distributed in the USA! Beyfortus injected into newborns in maternity wards since September 15 50% increase in infant deaths between 2 and 6 days of age. Main adverse effect = bronchiolitis = facilitation of infection by monoclonal antibody.
RSV is a scam:
Let’s also not forget - RSV is a completely made up, non-issue in health. A rebranded common cold that never threatened lives of babies. Please do not fall for this garbage. Do not inject your babies with toxic biological concoctions.
Moerna’s RSV Vaccine has no efficacy (and IMO, none is expected form transfection of cells with genetic material for a made up respiratory virus):
There is a severe risk exposure from transfecting your cells with genetic and other poisons (IMO, “prevention of cases” is a fairy tale made by highly paid statisticians trained in faking it):
Art for today: Sophia and Moomin, oil on linen.’
Once you realize we are dealing with a real manifestation of evil in this cult of death,
you are not surprised by anything that goes down, their words and actions, represent the evil that this death cult stands for. Killing babies, pregnant woman, anyone and everyone is a target for the death cult.
The day they are all executed will be a wondrous day.
Until that day resist and refuse to comply in every way possible. Do not be afraid.
We will be guided and protected by our awareness, and its connection to the pulse of life.
What do you expect from these copulating illegitimati (fuxing bastards)? They abort babies from the time of conception past birth, so killing a few babies with a neonatal injection, giving a few more autism, damaging their innate immunity, giving a bunch of them original antigenic sin, a few more of them who knows what autoimmune disease (e.g. Type 1 diabetes--which will shorten their lifespan in the best of scenarios, complicate their lives with injections, finger sticks, blood and urine tests & doctor visits;, lead to multiple complications , multiple hospitalizations, blind many of them, lead to lower limb loss from limb ulcers due to diabetic foot ulcers, early heart disease, stroke, and chronic kidney disease (dialysis and/or kidney transplant).
Whats not to like for the medical industrial complex?
Even if it is effective, RSV is in general a mild transient respiratory infection, y no vale la pena (Spanish for not worth the costs or risks.) (Hat tip a Sñra Menocal, mi profesora de Español en escuela secundario)
Like I said flucking bastards, no, fucking bastards, no: FUCKING BASTARDS; NO: GODDAMN FUCKING BASTARDS!!!!
(I have really been spending too much time reading Dr. Paul Anderson's posts.