Posted on 03/29/2020 1:40:58 PM PDT by Uber-Eng
I am originally from MI, so I’ll bite.
We will beat this thing, but here is an OS glimpse of CV-19, largely taken from another MI native, which I posted on another thread —
Some Interesting “down in the weeds” info!
Efforts began a year and a half before, and *multiple labs were involved, but in 2010, RUS/CCP Bio were successful in genetically taking the most virulent parts of the original “bat/SARS-Lk” virus, and adding it to the most virulent parts of “SARS” virus, in the Wuhan P4 genome manipulation, in which they did successfully created a NEW GENOME.
This is pages of summarized complexity by itself.
It is from thus new engineered genome VV-19 derives, and late in 2014 and in 2015, really bad stuff happened. Very quietly, RUS actually rapidly dumped significant resources into cv19 vaccine, calling it a “flu” vaccine, and for ing it on most of the population. It was generally not believed they were successful.
Already at this point, there is near impossible zoological complex union.
Analysis also reveals there was also restrictive enzyme manipulation of the HIV S component proteins, taken from glycoprotein 120 (GP120), with 4 confirmed inserts. One insert was taken from HIV-1 Gag (attached to the HIV capsid, or “nodule”), of which most bio engineers don’t understand the purpose of its insertion, and most yet believe to be mostly inert or failed. So, focus was on the other 3 HIV protein inserts. These inserts act through the CV-19 protein “spikes”, which initially look for and “plug into” the ACE-2 receptor.
However, keep in mind, the CV-19 virus is an RNA virus, and is not HIV.
That being said, it is believed the HIV S protein inserts (added/inserted to the CV-19 “nodule” spike proteins), likely serve to “fake out” the human immune system, (which doesn’t know it’s under attack), and initially even *reduces the production of *white blood cells*, enabling exponential unchecked viral growth or “load”. This means once a person really knows they are sick, and the body is trying to respond, the CV-19 virus has already been very active, and the onset of additional symptoms can be rapid.
As well, at least 35 different sequenced strands of Wuhan CV-19 have been identified around the world. One of these is known to have branched off and is called R18/G13. It is still referred to as Wuhan homogeneous, but the HIV Gag proteins are more broken down.
For now, the main receptor the CV-19 ((meaning a person has transitioned from SARS-CoV-2 into SARS/CoV-19)) RNA virus is attacking, is the Angiotensin Enzyme 2 (ACE2) recepter, (which is a Renin Aldosterone (RA) pathway), **which helps control a persons bloodpressure**!
So the CV-19 is not just attacking the lungs, it is attacking the heart, even before significantly reducing lung efficiency.
So the first steps of CV-19 virus are designed to initially attach to the ACE2 receptor, *fake out the immune system, and through cellular endocytosis exponentially replicate, while going after the RA pathway.
However, it’s not just the Wuhan Strand and the ACE2 receptor being attacked.
There are cases where CV-19 is attacking the GRP78 receptor, and the CD147 receptor.
So the spike protein on the CV-19 virus “nodule”, does already does not need to mutate, to go after other receptors. But it does have the stronger attraction or “infinity” for the bloodpressure regulating ACE2 receptor. At the same time, it can attack both GRP78 and CD147. If there is a wave 2 and wave 3, GRP78 and CD147 receptors may well be main mutated CV-19 targets.
CV-19 is likened to pre 1918 Spanish Flu in virulence, but it is not at all an influenza virus. As such while CV-19 may be 45X more virulent and robust (3 day viral life on non-porous surfaces), than H1N1, it is still not an influenza virus, and for that reason, and many other modern reasons, it is wrong to say it will kill the same percentages of people as the “Spanish Influenza”.
Part of the reason for the virulence —we have the protease called furin in our cells, and when CV-19 protein spikes have attached to an ACE2 receptor with furin near the surface, the CV-19 virus goes crazy, or “supercharged”, and this is when the CV-19 becomes roughly 1000X times as virulent.
What is written here, is largely taken from this Open Source vid — https://youtu.be/J6VEYzwSdZU
Any more than that, and increase the risk of a few people in trouble. Even in this vid, as intense as it sounds, Dr. Cottrel is being a bit careful not to get himself in trouble, so not to lose his “accesses”.
I am so on board with the hydroxychloroquine, as I have had to take much stronger related malarial drugs on deployments where up to 5 different types of malaria were present at once — As well as the use of other antibiotic therapies in the effort to reduce and even eliminate CV-19.
I am originally from MI, so I’ll bite.
We will beat this thing, but here is an OS glimpse of CV-19, largely taken from another MI native, which I posted on another thread —
Some Interesting “down in the weeds” info!
Efforts began a year and a half before, and *multiple labs were involved, but in 2010, RUS/CCP Bio were successful in genetically taking the most virulent parts of the original “bat/SARS-Lk” virus, and adding it to the most virulent parts of “SARS” virus, in the Wuhan P4 genome manipulation, in which they did successfully created a NEW GENOME.
This is pages of summarized complexity by itself.
It is from thus new engineered genome VV-19 derives, and late in 2014 and in 2015, really bad stuff happened. Very quietly, RUS actually rapidly dumped significant resources into cv19 vaccine, calling it a “flu” vaccine, and for ing it on most of the population. It was generally not believed they were successful.
Already at this point, there is near impossible zoological complex union.
Analysis also reveals there was also restrictive enzyme manipulation of the HIV S component proteins, taken from glycoprotein 120 (GP120), with 4 confirmed inserts. One insert was taken from HIV-1 Gag (attached to the HIV capsid, or “nodule”), of which most bio engineers don’t understand the purpose of its insertion, and most yet believe to be mostly inert or failed. So, focus was on the other 3 HIV protein inserts. These inserts act through the CV-19 protein “spikes”, which initially look for and “plug into” the ACE-2 receptor.
However, keep in mind, the CV-19 virus is an RNA virus, and is not HIV.
That being said, it is believed the HIV S protein inserts (added/inserted to the CV-19 “nodule” spike proteins), likely serve to “fake out” the human immune system, (which doesn’t know it’s under attack), and initially even *reduces the production of *white blood cells*, enabling exponential unchecked viral growth or “load”. This means once a person really knows they are sick, and the body is trying to respond, the CV-19 virus has already been very active, and the onset of additional symptoms can be rapid.
As well, at least 35 different sequenced strands of Wuhan CV-19 have been identified around the world. One of these is known to have branched off and is called R18/G13. It is still referred to as Wuhan homogeneous, but the HIV Gag proteins are more broken down.
For now, the main receptor the CV-19 ((meaning a person has transitioned from SARS-CoV-2 into SARS/CoV-19)) RNA virus is attacking, is the Angiotensin Enzyme 2 (ACE2) recepter, (which is a Renin Aldosterone (RA) pathway), **which helps control a persons bloodpressure**!
So the CV-19 is not just attacking the lungs, it is attacking the heart, even before significantly reducing lung efficiency.
So the first steps of CV-19 virus are designed to initially attach to the ACE2 receptor, *fake out the immune system, and through cellular endocytosis exponentially replicate, while going after the RA pathway.
However, it’s not just the Wuhan Strand and the ACE2 receptor being attacked.
There are cases where CV-19 is attacking the GRP78 receptor, and the CD147 receptor.
So the spike protein on the CV-19 virus “nodule”, does already does not need to mutate, to go after other receptors. But it does have the stronger attraction or “infinity” for the bloodpressure regulating ACE2 receptor. At the same time, it can attack both GRP78 and CD147. If there is a wave 2 and wave 3, GRP78 and CD147 receptors may well be main mutated CV-19 targets.
CV-19 is likened to pre 1918 Spanish Flu in virulence, but it is not at all an influenza virus. As such while CV-19 may be 45X more virulent and robust (3 day viral life on non-porous surfaces), than H1N1, it is still not an influenza virus, and for that reason, and many other modern reasons, it is wrong to say it will kill the same percentages of people as the “Spanish Influenza”.
Part of the reason for the virulence —we have the protease called furin in our cells, and when CV-19 protein spikes have attached to an ACE2 receptor with furin near the surface, the CV-19 virus goes crazy, or “supercharged”, and this is when the CV-19 becomes roughly 1000X times as virulent.
What is written here, is largely taken from this Open Source vid — https://youtu.be/J6VEYzwSdZU
Any more than that, and increase the risk of a few people in trouble. Even in this vid, as intense as it sounds, Dr. Cottrel is being a bit careful not to get himself in trouble, so not to lose his “accesses”.
I am so on board with the hydroxychloroquine, as I have had to take much stronger related malarial drugs on deployments where up to 5 different types of malaria were present at once — As well as the use of other antibiotic therapies in the effort to reduce and even eliminate CV-19.
for some weird reason, they didn’t include this EO from Gov Halfwit on their website:
STATE OF MICHIGAN
GRETCHEN WHITMER
GOVERNOR
DEPARTMENT OF LICENSING AND REGULATORY AFFAIRS
LANSING
ORLENE HAWKS
DIRECTOR
BUREAU OF PROFESSIONAL LICENSING
611 W. OTTAWA • P.O. BOX 30670 • LANSING, MICHIGAN 48909
www.michigan.gov/bpl • 517-241-0199
LARA is an equal opportunity employer/program
March 24, 2020
TO: Licensed Prescribers & Dispensers
RE: Reminder of Appropriate Prescribing and Dispensing
Dear Licensed Prescribers and Dispensers:
The Department of Licensing and Regulatory Affairs has received multiple allegations of
Michigan physicians inappropriately prescribing hydroxychloroquine or chloroquine to
themselves, family, friends, and/or coworkers without a legitimate medical purpose.
Prescribing hydroxychloroquine or chloroquine without further proof of efficacy for treating
COVID-19 or with the intent to stockpile the drug may create a shortage for patients with lupus,
rheumatoid arthritis, or other ailments for which chloroquine and hydroxychloroquine are proven
treatments. Reports of this conduct will be evaluated and may be further investigated for
administrative action. Prescribing any kind of prescription must also be associated with medical
documentation showing proof of the medical necessity and medical condition for which the
patient is being treated. Again, these are drugs that have not been proven scientifically or
medically to treat COVID-19.
Michigan pharmacists may see an increased volume of prescriptions for hydroxychloroquine
and chloroquine and should take special care to evaluate the prescriptions’ legitimacy. Pursuant
to Michigan Administrative Code, R 338.490(2), a pharmacist shall not fill a prescription if the
pharmacist believes the prescription will be used for other than legitimate medical purposes or if
the prescription could cause harm to a patient.
It is also important to be mindful that licensed health professionals are required to report
inappropriate prescribing practices. LARA appreciates all licensed health professionals for their
service and cooperation in assuring compliance in acting responsibly while continuing to provide
the best possible care for Michigan’s citizens during this unprecedented and very challenging
time.
To stay up to date on the latest information regarding the COVID-19 pandemic please go to
www.michigan.gov/Coronavirus and the CDC site at www.CDC.gov.
Sincerely,
Deb Gagliardi, Director
Bureau of Professional Licensing
Forrest Pasanski, Director
Enforcement Division
BUREAU OF PROFESSIONAL LICENSING
611 W. OTTAWA • P.O. BOX 30670 • LANSING, MICHIGAN 48909
www.michigan.gov/bpl • 517-241-0199
LARA is an equal opportunity employer/program
Obviously a few mistakes, as sent from my phone. “VV” = CV
I’m like many Freepers, doing research to learn about the threat and how to protect our families. My question is why can’t the Government be open about the threat?
Thanks for the info.
I agree. The President should allow every American to get a 5 day script for the drugs for each of their family. I reside one county north of Oakland.
So are doctors able to use the drugs? Dr. Zelenko in NY seems to be having success. 699 successful out 703.
I agree on the Bio weapon stuff.
Seems to me that the letter states the drugs are not approved to treat Covid, thus would fall under the unauthorized use clause in the letter effectively outlawing the treatment. But I’m not a lawyer.
“So are doctors able to use the drugs?”
totally ...they’re old drugs, long approved by the FDA ... and any doctor can legally and ethically prescribe any FDA-approved drug for any medical purpose, even for purposes for which it wasn’t originally approved ... that kind of use is called off-lable use and it’s done all the time ...
CDC even has a information about possible doses for treating COVID-19:
“There are no currently available data from Randomized Clinical Trials (RCTs) to inform clinical guidance on the use, dosing, or duration of hydroxychloroquine for prophylaxis or treatment of SARS-CoV-2 infection. Although optimal dosing and duration of hydroxychloroquine for treatment of COVID-19 are unknown, some U.S. clinicians have reported anecdotally different hydroxychloroquine dosing such as: 400mg BID on day one, then daily for 5 days; 400 mg BID on day one, then 200mg BID for 4 days; 600 mg BID on day one, then 400mg daily on days 2-5.”
https://www.cdc.gov/coronavirus/2019-ncov/hcp/therapeutic-options.html
The whole crowd here has become pretty good at “reading between the lines”, no worries on the spelling. And thanks for the breakdown.
Again, anyone that looks at that reddit link sent earlier can see the graph that puts the CV19 well ahead of any flu or SARS with respect to contagiousness.
With your explanation, why do I feel like I’m in a twisted version of “Jurassic Park” and unrestrained DNA manipulation?
Marking to read
Thank you for sharing
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