They lied about masks, about vaccines, about the origin of Covid. In fact they lied about everything….and now they want to be in charge of global pandemic responses. What could possibly go wrong?
Oh SH*T, Bill Gates next pandemic plan just SCREWED all of us | Redacted with Clayton Morris Redacted (32 min)
The NYT: Mask Mandates Did NOTHING AT ALL – Covid Update (12 min)
Antibody class switch in vaccinated – video update 79
The war on eggs…..
1./ Now I understand the war on eggs…https://t.co/BnzZt2sQrV
— Elijah (@CherithElijah) February 3, 2023
3./ I lost one of my chooks this week (suddenly died) but will be replacing the poor thing soon. Do you like the makeover I gave my coup. pic.twitter.com/mYPc5CsBGJ
— Elijah (@CherithElijah) February 3, 2023
@Tishbite_redux Geert exposes himself and flashes his rude (controlled ops) bits pic.twitter.com/tF2O2cdlgs
— Elijah (@CherithElijah) November 7, 2022
Geert made some good points at the start of the pandemic which established his credibility but now he is being wheeled out as damage control. He is never going to say…..we killed and injured people with the vaccine. He does no talks on excess deaths. We are on 17% in Australia. He says give them to the elderly but not to children. He even condemns the bivalent vaccine. Those are just concessions to the obvious. The bivalent vaccine and the injection of Children is a moot point because uptake is extremely low (except for retards) and will never get higher. However,they need to protect the legacy of this “wonderful” new technology. The legacy is….”see the vaccines worked” and cut the severity of the disease. We had some problems because some of the antibodies were not fully neutralizing (leaving the door open for improvements). We can use this new vaccine mRNA technology to power our (Fourth Industrial) medical revolution. According to Geert the non-neutralizing antibodies prevent severe disease (while still creating ADE go figure) but he never mentions that it is T cells aimed at non-structural proteins that prevent severe disease. His job is to keep you focused on the SPIKE and ANTIBODIES and nothing else. I seem to remember the virologist expert rancid yellow (Vincent Racaniello) stating that, “there is no correlate of immunity with antibodies”. Other experts have said the same. All antibodies tell you is that at some point you had X disease. After a while even the antibodies disappear. But the Tcells have long memories. The Tcells don’t forget. Moreover his astonishment at the “rapid evolution” of the variants is suspicious. Apparently thousands of years of mutations have suddenly sped up and produced a plethora of variants. Quell surprise. Even if the appearance and sequencing of these new variants is 100% correct might it have something to do with constantly jabbing people (with who knows what different formulations?) thereby forcing viral evolution by running it through different populations. The shedding alone will create differentiated viral quasi swarms. We need to stop vaccinating and we need to hunt these people down and prosecute them.
Geert needs to be asked these questions:
1. Do you think we should continue developing mRNA vaccine (transfection) technology?
2. Was the pandemic man made or natural?
3. Does anyone need to be prosecuted for crimes against humanity?
Put him on the spot and watch the vaccionologist squirm. There are very few of them not playing some roll in this global pantomime.
Synthetic clones can be made by the truckload and purified mRNA will code for pathogenic viruses but burn out easily. Such viruses do not have the adaptability of a quasi-swarm and therefore harm will be contained (but shocking to anyone on the receiving end). They used this technique coupled with a psychological campaign, manipulated death numbers and a rigged PCR test to get us to inject.
It was all about the “vaccines”….they needed billions of test subjects…shooting us full of who knows what….and feeding the results into A.I. so as to discover how to make us transcendent humans. Instead they created zombies.
1:01 – Synthetic clone (2008)https://t.co/3gAOvpJTdN pic.twitter.com/F1LlnhoJvM
— Elijah (@CherithElijah) November 7, 2022
This is the Twitch version:
Office Hours GEERT ON NARRATIVE: Gigaohm Biological High Resistance Low Noise Information Brief (2:21)
On Odysee:
Watching this as I type this blog. Look at 32 minutes at the Vaccine Conference in Italy a junket for Virologists. J.C. shows how they emphasize “antibodies” at the expense of everything else. Where are the T cells, B cells etc. And how come no one mentions the HUGE mountain of excess deaths? These people DISGUST me. The slides have GSK logo.
GlaxoSmithKline (GSK) consolidates Pfizer consumer brands under Publicis Media specialty unit. GlaxoSmithKline has awarded Publicis Media and its bespoke platformGSK more business, adding the former Pfizer Consumer Healthcare brands to its portfolio. Pfizer owns a 32% equity stake in the joint venture and GSK owns 68%. The combined business, which will operate globally as GSK Consumer Healthcare, will be led by CEO Brian McNamara.
When will people wake u to the danger? We have been warning for two years. Catch the paper on childhood vaccines at 58 min. And Linked Recognition at exactly one hour (1:00)
Linked Recognition pic.twitter.com/Aw3Uyuy3oH
— The Tishbite (@Tishbite_redux) September 14, 2022
Apoptosis is a type of cell death in which a series of molecular steps in a cell lead to its death. This is one method the body uses to get rid of unneeded or abnormal cells. It “explodes” and clears the contents which include viruses, virus fragments and proteins and mRNA that has been methylated to for the more stable pseudouridine (Ψ ). The natural immune response is therefore NOT Triggered. It interferes with your interferon (IFNs) response and this was already known in 2016. This probably explains why the most deaths and illness occur in the first two weeks after the jab. Infection is not recapitulated by IM (Intra Muscular) transfection!
Interferons (IFNs), cytokines produced by nearly all cell types during viral and other microbial infections, play crucial roles regulating immune response. mRNA vaccines incorporate Ψ or m1Ψ to evade host cell foreign RNA sensing and enhance mRNA translation.
Linked Recognition: Gigaohm Biological High Resistance Low Noise Information Brief (1:56)
This is very interesting because it goes right back to March 2020 and sees what the likes of Bret Weinstein was saying in his podcast back then. How times have changed. The experts back then were WRONG. The likes of Johnathan Couey and Dr Kevin McCairn were correct more than two years ago and I am pleased to say that I brought you the correct information from the start.
A Fan Dedication to Darkhorse: Gigaohm Biological High Resistance Low Noise Information Brief (2:18)
Not watched either of these yet.
National Immunomythology Update: Gigaohm Biological High Resistance Low Noise Information Brief (2:49)
History of Virology: Gigaohm Biological High Resistance Low Noise Information Brief (3:04)
Recommended
Two great quotes by Walter:
"I would rather have Questions that cannot be answered rather than answers that cannot be questioned" "Do everything that helps and nothing that hurts"
Another cracking show. Walter and Johnathan are starting to connect all the dots.CD147 or Basigin is a novel receptor on red blood cells and augments NF-κB -dependent inflammation in monocytes (= a type of white blood cell called leukocytes). Not only ACE 2 but also CD147 helps the virus enter the cell Recent studies suggests CD147 as SARS-CoV-2 entry receptor of platelets and megakaryocytes, leading to hyperactivation and thrombosis. CD147 plays an important role in human immunodeficiency virus type 1, hepatitis C virus, hepatitis B virus, Kaposi’s sarcoma-associated herpesvirus, and severe acute respiratory syndrome coronavirus infections. CD147 (Basigin) has been shown to be an essential receptor on red blood cells for the human malaria parasite, Plasmodium falciparum. Does this explain why HCQ might be effective?
Walter Chesnut LIVE : Gigaohm Biological High Resistance Low Noise Information Brief (2:15)
00:00 Intro
16:00 Jessica and spike reaction on hemoglobin
17:00 Walter Chestnut interview
24:00 CD147 and blood cancers
27:00 CD147 and Diabetes
28:00 Cat disease and CD147
35:00 Neurotoxic amyloidogenic peptides in the proteome of SARS-COV2
42:00 Antiphospholipid Syndrome ..a mechanism for Recurrent Thrombosis?
45:00 Waldenström macroglobulinemia
01:11 https://wmcresearch.org/
01:13 Obesity
01:18 This to shall pass?
01:20 Letter to the editor
01:22 Injection techniques
01:24 End of interview with Walter
01:25 Jessica’s sub stack post
01:26 Monocyte CD147
01:32 They changed the way we think about the immune system:
Antibodies provide no corelate of immunity pic.twitter.com/gSmd9E3c1i
— The Tishbite (@Tishbite_redux) August 14, 2022
01:39 Antibodies do clean-up they come last
01.42 No corelate of protection. Antibodies do not equal immunity
01.47 Deepak fraud
01:50 Bill Gates carbon zero
01:54 The elite think they are Beekeepers
01:56 Albright challenged
02:00 What have we learned?
02:05 Gay
02:10 Outro
Another excellent presentation with Walter Chestnut discussing his latest findings, also commenting on a Robert Malone video who warns about the LNP delivery mechanism causing problems such as PEG micelles stimulating production of anti-PEG IgM, which led to accelerated clearance of subsequently administered PEGylated liposomes. According to A review on phospholipids and their main applications in drug delivery systems, Phoshpholipid–PE–PEG mixtures could form micelles rather than liposomes if PE–PEG content exceeds certain critical limit. Of course the PEG interests me because it is used along with surfactants for micelle formation in polymerisations. I never thought something like that would be injected into people (lolz). Below is actually a good resource on Lipids (have a look at all the pages very informative):
Phospholipids are major plasma membrane constituents that comprise cells’ outermost layer.https://t.co/9dr94NaRtQ pic.twitter.com/uWzqe5FXC6
— The Tishbite (@Tishbite_redux) July 28, 2022
Heavy metals play a role in neurodegeneration but lipids are important as Anticardiolipin and other antiphospholipid antibodies (are found) in critically ill COVID-19 positive and negative patients Antiphospholipid antibodies (APLAs) are biomarkers of a spectrum of clinical features observed in antiphospholipid syndrome (APS).1 Features of APS include venous and arterial thrombosis involving multiple organs and having various presentations. Positive APLA serology was associated with more severe disease regardless of COVID-19 status. Moreover, Persistent lgG anticardiolipin autoantibodies are associated with post-COVID syndrome. Persistence of various symptoms in patients who have recovered from coronavirus disease 2019 (COVID-1 9) was recently defined as ‘long COVID’ or ‘post-COVID syndrome’ (PCS). They conclude that Immunoglobulin G (lgG) anticardiolipin autoantibodies (aCL) are associated with the severity of COVID-19. In other words an allergic or inflammatory reaction to lipid (in the heart) but also “…persistence of the virus, especially in the nervous system, could be suggested with a post-infectious inflammatory or autoimmune reaction”. Might this have something to do with pumping the body full of phoshpholipids and mRNA spikes? What do I know? (I am just a bucket chemist who used to mix this stuff in buckets not in human bodies).
Unfortunately, many of Walter’s hypothesis are proving to be correct. He is an avid reader of the medical literature and a talented dot-connecter with a big picture overview. His sub-stack is highly recommended. In his latest article he shows how amyloid is a double-edged sword. A large build-up will cause problems, but amyloids also serve protective functions – against autoimmune attacks. So, they are symptomatic rather than causal factors.
— The Tishbite (@Tishbite_redux) July 28, 2022
Comment: Repeated infection with covids is not good even for the unjabbed and even if they got over it before. A least the omicrons have the PrP silenced. But the HIV and the other nasties and all the humanized nucleic acid etc tacked into the spike yes, will be immune insults that will catch up with us the older we are. Shortened lifetimes, yes. The younger the less shortened. Of course, the jabbed are the ones who will suffer shortest lives.
More study is needed into the mutagenic properties of the spike-protein. Perhaps this explains Nucleic Acid Acid Based Therapeutics against Respiratory Infections?
— The Tishbite (@Tishbite_redux) July 28, 2022
Comment: The prion promoting sequence in the spike also promotes amyloidosis. They are seeing where there won't be a positive D-dimer test but when they put blood under the scope then you see the amyloid building up. The amyloid is causing the clotting, the heart damage, etc. They look for a test for amyloid in those "rare" pre-jab liver inflammation cases and they find amyloid build up and light chains. The hepatitis victims go on to be found Dx with myloid leukemia (if I have the name correct). The Chinese are making more targeted covid viruses - but it is US research over 25 years that developed those - there is research trail from Baric, Daszak and others and a lot of patents. Baric collaborated with Shi - he trained her! That enrichment is bad news - they did that in the jab for a lot of reasons - it throws off all kinds of cascades along with the defanging IFN-1. IFN-1 has all these cascades which include regulatory ones to down regulate inflammation. But that is all gone because of the jab made to evade being recognized and take IFN-1 out. Enriching with C-G over-glycosylates it possibly more than HIV is so it sails on by more so than the virus construct.
This is very complex and there is so much that we do not know. As someone commented.
Code that codes for multiple things depending happening on how it’s parsed with the folds everybody producing the spikes internally become a mini gain of function study. multiply by a billion consecutive studies running concurrently.
It is not just the structure of the protein but how it folds and polarity as in hydrophilic or hydrophobic nature and charge. Who is to say that the same protein might not fold differently under other circumstances thereby acquiring different properties? Repeat expansions have been proposed to cause disease by both the repeat RNA forming foci that sequester RNA-binding proteins and through toxic dipeptide repeat proteins generated by repeat-associated non-ATG translation discussed in the article G-quadruplex-binding small molecules ameliorate C9orf72 FTD/ALS pathology in vitro and in vivo.
C9orf72 (chromosome 9 open reading frame 72) is a protein which in humans is encoded by the gene C9orf72. The protein is found in many regions of the brain, in the cytoplasm of neurons as well as in presynaptic terminals. The mutations in C9orf72 are significant because it is the first pathogenic mechanism identified to be a genetic link between familial frontotemporal dementia (FTD) and amyotrophic lateral sclerosis (ALS). The mutation of C9ORF72 is a hexanucleotide repeat expansion of the six-letter string of nucleotides GGGGCC.
I wonder, I wonder if pumping the body full of mRNA instructions to make spike proteins will deliver the spike proteins that they want? We know already that the mRNA vaccines are not pure but contain fragments. The start codon of a gene is always “ATG” so repeat associated non-ATG translation means that it does not read the correct starting point, or you could say that it reads through the stop condon (runs the red light). It looks like read-through can cause disease. Is that why the above experiment attempted to improve dementia using small peptides that stick to the G-quadruplex?
Walter Chesnut LIVE: Gigaohm Biological High Resistance Low Noise Information Brief (2:50)
He warns that injecting the children is murder. They will be made more vulnerable to sickness and death.
Pandemic Restarting?! Geert Vanden Bossche takes a unique view (1:21)
LINK: https://streamyard.com/8ik4q75u6p7r
Not had a chance to watch this yet:
Mystery Science Theater 2022: Gigaohm Biological High Resistance Low Noise Information Brief (2:57)