These mRNA vaccines are corrupting and destroying our innate immune systems

Let's kick off with a basic explanation of why the COVID-19 vaccines are more or less useless at preventing infection.

There are two major categories of antibodies:

1. Secretory IgA, which is produced by immune cells (lymphocytes) located directly underneath the mucous membranes that line the respiratory and intestinal tract. The antibodies produced by these lymphocytes are secreted through and to the surface of the mucous membranes. These antibodies are thus on site to meet air-borne viruses, and they may be able to prevent viral binding and infection of the cells.

2. IgG and circulating IgA, which occur in the bloodstream. These antibodies protect the internal organs of the body from infectious agents that try to spread via the bloodstream.

Vaccines that are injected into the muscle will only induce IgG and circulating IgA, not secretory IgA, so they cannot and will not effectively protect the mucous membranes from infection by SARS-CoV-2.

How are these vaccines harming people?

The mRNA in these vaccines is entering the bloodstream, going to your vital organs and telling the cells there – and throughout your body - to produce the toxic spike protein. Your killer lymphocytes are then attacking these cells that are producing the pathogen, resulting in damage to the heart, lungs, kidneys, etc.

Prof. Sucharit Bhakdi, Professor Emeritus of Medical Microbiology and Immunology,

former Chair, Institute of Medical Microbiology and Hygiene,

Johannes Gutenberg University of Mainz.

From the video above:

Autopsies were carried out on 17 individuals aged between 28 and 95, whose deaths were apparently unrelated to the vaccine, and nothing was found - the organs appeared normal.

Professor Doctor Arne Burkhardt, professor of pathology, looked at these organs and in 90% he found clear evidence for auto-immune self-attack by killer lymphocytes on the tissues, the main ones being the heart and the lung. (Summary of findings)

Although it can’t be definitively proved that it was due to the vaccines, that was the only common denominator in all the deceased.

Of all the infectious agents that are sleeping in the bodies of billions of people around the world, the number one is tuberculosis. Our lymphocytes keep all the potentially harmful bacteria and infectious agents sleeping in our bodies at bay. But if some of these lymphocytes take up the mRNA and start expressing the spike, their fellow lymphocytes will attack and kill them, which will lead to a weakening – and potential eventual destruction – of the natural/innate immune system.

New study shows that 90 days after vaccination you’re MORE likely to be infected with Omicron than the unvaccinated

From a Danish study carried out on almost all PCR cases in the country between 20th Nov and 12th Dec.

Found VE in first months after second dose:

- Pfizer 55.2%

- Moderna 36.7%

VE declines rapidly over just a few months. After being boosted with Pfizer, VE goes up to 54.6% - i.e. slightly lower than after initial vaccination.

The study concludes: ‘In light of the exponential rise in Omicron cases, these findings highlight the need for massive rollout of vaccinations and booster vaccinations.’ Right.

But look at the data for VE beyond 3 months. Minus 76.5% for Pfizer and minus 39.3% for Moderna. That means you’re that much more likely to be infected with Omicron!!

From Steve Kirsch’s newsletter on 24th Dec 2021:

‘If people don’t get boosted as required, they will be MORE vulnerable than if they weren’t vaccinated. That’s what NEGATIVE vaccine efficacy means. It doesn’t mean the protection wears off (like we were told). It means the OPPOSITE of what you were told: it means the vaccines helps the virus to infect you (by suppressing your immune system). It means we were lied to.

This isn’t a vaccine at all. This is basically stimulating your immune system so it is already “geared up” to fight the virus. That’s not what a vaccine is supposed to do.

Furthermore, the negative VE after 90 days means you are hooked for life and I would guess that we will need shorter and shorter dosing intervals for every booster (since it kills off your immune system every time).'

If you want to know more about the way the mucosal and systemic parts of the immune system work, this is a really interesting conversaiton between Dr John Campbell, a nurse teacher for more than 25 years, and Emeritus Professor Robert Clancy, expert in mucosal immunology:

And an interesting article by Dr Jessica Rose (BSc in Applied Mathematics, MSc in Immunology from Memorial University of Newfoundland) on a study from the Netherlands, entitled: 'The BNT162b2 mRNA vaccine against SARS-CoV-2 reprograms both adaptive and innate immune responses'.

'These COVID-19 mRNA injectable products are causing, immune system dysregulation - and not just in the context of the adaptive system, but in the context of the innate system.

The bottom line here is this. We know that innate responses are vital to a healthy and optimally-functioning immune system. We also know that something is very, very wrong with these COVID-19 injectable products with regards to persistent hyperinflammation and a plethora of systemic and physiologically-comprehensive adverse events including death from micro-emboli formation and clotting.

We also know that [there is] evidence to support that these COVID-19 injectable products are modulating innate responses and that this isn’t limited to problems with COVID-19. Problems with fungi, other viruses and bacteria can be anticipated. VAERS has hundreds of thousands of reports of adverse events related to fungal infections, plagues of herpes zoster (shingles) occurrences indicating weakened immunity, cancers coming out of remission, and the list goes on.'

Read the full article here.