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01 Oct 2017
Home
File List, RICO
1988 Steere says Lyme is like a B cell leukemia
Assoc Blogs-n-Webs:
TruthCures.org
badlymeattitude.com/
immune2lies.com/
researchfraud.com/
may12.org
meadvocacy.org/
truthbetoldx81
lymecryme
CrymeDiseaseNorway
crymedisease
theothersideofthestretcher
rjspiritualityandtuth
LymeTruthSite
JC-LilnkedIn
KD-Linkedin.com
LD-LinkedIn
JC-academia.edu
KD-academia.edu
CDC "SPIDER"
Fungal Exosomes Inhibit Apoptosis
IDSA:
"Vaccines serve the mfgs, not their victims"
RICO_filed_USDOJ
BlumenthalAntiTrust Lawsuit
Exosomes, Blebs
Spirochetal_Dementia
PDFs
CDC Admits Fraud, 2016
Dattwyler, 1988
Golightly, 1988
Dressler,
1994
BarbourFish, 1993
Dearborn,
1994
BarbourFishpdf.pdf
Pathogenic Fungi
Bush's warcrimes, Oct 2000
Trainer
170708 |
| |
Free 200+ page scientific book on the various fraud crimes committed by CDC
and Yale employees.
Includes information on how the pediatric vaccines
fail
by giving the children the very
brain damage these viruses these vaccines were intended to prevent
(particularly the MMR), according to
IDSA,
NYU's Stanley Plotkin, and Johns Hopkins' Paul
Auwaerter.
Also included are details about how the University of Connecticut
"assaulted" Czech children with a non-vaccine (LYMErix) that they knew
would do those children no good. There was NO chance that
vaccine would have prevented Lyme, not only because OspA is pam3cys, a
triacyl-, fungal lipoprotein which causes immunosuppression, but because
there is none of the USA Borrelia strain B31 OspA in Europe.
We show that Allen Steere published in 1988 that Lyme caused a B cell
mutation (lymphoma-like) that rendered them incompetent and that that's
actually the disease IDSA, the CDC, Yale and UConn deny exists and wrote out
of the "case definition" because that immunosuppression disease was also
caused by LYMErix and they knew this in 1993 - before the Dearborn
stunt (where the CDC falsified the testing for Lyme, 1994).
We show NIAID's "Director" Anthony Fauci even has a patented treatment for
fungal immunosuppression diseases, yet he claimed on national TV (Lou Dobbs)
that "We have a scientifically validated Lyme vaccine, but it's not well
used" - 1.5 years after it was ordered off the market by the FDA via
ultimatum, in February, 2002.
We show that Simon Wessely, et al, while finding that Gulf War Illness was
associated with the vaccines, later claimed the Veterans were just cowardly
airy-fairies and are using "brain magic" (like telekinesis) to fake their
scientifically valid illness signs. (Yes. That is what
"somatoform" technically means.)
This is the crazy whacked-out, pervert "government" the world is supposed to
respect as "Exceptional." They can't handle a thing. They lie
about everything. They commit war crimes #ALLDAY, betray each other
(Cheney and Plame), and blame the victim, no matter what the situation.
The Lord, God, in Heaven and the Jesus Gang do not respect the liars and the
cowardly. In fact it works the other way around. He "removes His
Grace."
Remember, people, when all USA
institutions fail (and they have, as Winston Churchill predicted in 1932), that's a
power vacuum. When your credibility on all matters is a
negative number, no one listens to you. Other countries will have
conversations between themselves without you. You're not taken
seriously. Nations, institutions, and societies go elsewhere for the
Truth and subsequently, insight into the future of civilization and the
planet to go forward.
Churchill: "Projects
undreamed-of by past generations will absorb our immediate descendants;
forces terrific and devastating will be in their hands; comforts,
activities, amenities, pleasures will crowd upon them, but their hearts
will ache, their lives will be barren, if they have not a vision above
material things. And with the hopes and powers will come dangers out of
all proportion to the growth of man’s intellect, to
the strength of his character or to the efficacy of his institutions.
Once more the choice is offered between Blessing and Cursing. Never was
the answer that will be given harder to foretell."
http://teachingamericanhistory.org/library/document/fifty-years-hence/
And if the US Govt employees were the least bit
intelligent, they would see the loss of credibility as a threat. But those US Govt
employees are all too busy serving themselves, according to the
erroneous Freudian theory that ME-Love is GOOD!! because of the statistical
frequency of such debauched, un-virtuous behavior.
The dumbasses dont know they have created not just a USA power vacuum, but a
global one. The Theory of Me does not scale up from the individual to
society, so I hate to tell you but the pop psychology theories were never
real or valid. They're short-sighted. Imbecilic.
The reason the
CDC, Yale, and ALDF.com
criminals
dont want "Lyme" (or any other borreliosis) treated or
even
identified
is because it becomes more about the secondary opportunistics and you dont
treat the herpesviruses with antibiotics.
ILADS is not aware of any of this, which is why they're so
famous. They know zero about the mechanisms of disease;
they're "doctors," not scientists.
I wish people understood the very big difference.
People maybe dont know this, but during the VietNam war, the
USA lowered the medical school requirements, admitting the likes of
psychology or philosophy or English literature undergraduates.
At the present time, the first picks for entry into USA
medical schools - and you can look this up since it is a real fact - depends
on how much
the applicants'
parents donated to the medical school. These factors contribute to a lowered
cognitive standard, overall, in "doctors." Two primary factors
contribute to the growth in dumb "doctors":
mainly only rich kids get into medical school,
and they dont need a science background.
Allen Steere chose Rheumatology to get out of VietNam; how
many old ladies who need aspirin are going to be deployed to VietNam?
Eugene Shapiro was an English Literature major.
Being a "doctor" is
not about talent and it's not about wanting to be a healer.
It's a money-making *business.* That was why the only times
any medical associations sued Big Insurance was over their own
reimbursements, NOT about how Insurance interferes in medicine or diagnostic
and treatment guidelines. They interfere with everything, not just Lyme;
they RAISED the bar on the diagnostic standard for Lupus, changing the name
to "anti-phospholipid syndrome" and you are only allowed to have it
(and therefore be entitled to "treatment"), if you have a certain
high level of anti-phospholipid antibodies.
Besides the scientists and "doctors" we quote in the
Occam's Razor and other reports, what "doctors"
are talking about how OspA alone caused a form of post-sepsis?
In the world. Think....
You MUST understand this about "doctors," they are only to be
laughed at.
Pharma advertises directly to consumers now.
The CDC throws out data it does not like all the time, re:
vaccines.
That means all this - Medicine - is a free-for-all.
NO ONE is demanding science or scientific validity or even the
scientific method.
Even the NIH says they dont know what OspA is.
They told me
so.
Fauci's office told me
and
Francis Collins' office told me they dont know
what OspA is (this is basic science: "what is the molecule, so we can guess
what it does").
Paul Auwaerter's office told me they dont know (then he
later said "I am no mycologist" just a few weeks ago), the CDC said they do
not know, and YALE told me they do not know what OspA is, in March 2012.
Think about what it would mean if these entities openly said
OspA was Pam3Cys.
CHANGE how you think about "doctors." You cant educate
them into treating you. They do not listen.
They have the hard core arrogance that comes from
being a fraud. They dont HEAR, or READ, because in their own minds, they are
superior to it all.
You exist to serve them.
You are raw meat, they operate the hamburger-maker.
You are PROCESSED.
It does not matter to them how you turn out, as
long as in their records
("defensive medicine"), you were put through the machine.
The machine does not change, either.
Patient comes in, they walk out poorer and with some
prescription.
Done.
If you dont fit into that machine, you have to go into the
incinerator.
You are foul.
Waste.
Unusable.
These people, "doctors,"
have no creative intelligence
(that's a very dangerous sign).
They did not design the machine. They're just operators of it.
When it's broken, they do not know how to fix it.
This is America; everything is broken.
Incompetent criminals and losers dot NIH
dot gov lament a reduced budget for their non-endeavors and incompetent
"science," LMAO
We Love Russia!!!
This is not my country any more. The USA
rejects, trashes, and destroys its own people.
New updates to the Common Mechanisms charge sheet (see links below
on this webpage to download) reveal that the CDC and BigPharma are
throwing out the vaccine failure data
from "safety and efficacy" calculations where the children who are getting
those brain damaging viruses from the vaccines (confirmed at autopsies)
and are blaming the parents.
They're saying the children are getting those brain damaging viruses from
the environment - from being exposed to other people with active mumps,
measles or rubella.
Do you see ~1:60 people walking around with measles mumps and
rubella, assuming a 1:1 contact rate between the baby vaccinee and
someone they are exposed to with active MMR viruses?
That's the most ridiculous lie the CDC has told to date.
New Website with all the new, updated criminal charge
sheets >>
http://www.truthcures.org/charge-sheets
We think you're going to enjoy
Johns Hopkins' Paul Auwaerter talking
about how the pediatric Autism vaccines fail by giving the children those
actual vaccine viruses which are all brain damaging. That was the
reason we had proposed for the abuse and neglect of the 20-30 milion of us
with Post-Sepsis Syndrome, otherwise known as "Chronic Lyme," "Chronic
Fatigue syndrome," Fibromyalgia, etc. There is no NIIID (National
Institute of Immunosuppression and Infectious Diseases), there is only the
opposite, the tip of the iceberg, NIAID.
What's Paul Auwaerter doing claiming he is
an expert in only 2 things on on his webpage? Lyme and Epstein-Barr?
Why is his job, now, apparently to trash Lyme victims? Hmmm. Let
me think...
He's
an expert on why the MMR vaccines fail and give children the very
viruses the vaccines were meant to prevent via vaccinating immunosuppressed
children, and vaccinating children with mycoplasmally/other contaminated
viruses. It's the same thing with
Gulf War Illness.
All this slander and libel (Deprivation
of Rights under Color of Law) against sick people because the truth
about Lyme and ME/CFS is that they are in the "immune system failure" class
with vaccines induced autism and cancer. Additionally, a
stealth
bioweapon "overwhelms" the immune
system, while leaving no antibody trace of the original infection.
That is why there is no NIIID.
The charges are also linked from here, if you find it easier to copy and
paste from a webpage than a pdf. >>
Navigation.htm
Good thing Sweeg and Durland were such
harassholes. We never would
have discovered what was the source of the Autism pandemic from
vaccines. We have to say, "Thanks for OspA."
And Merck is not going to be
too happy with Auwaerter's several reports about how their vaccines
brain damage babies. We have more than
this.
The Criminal Charges Sheets - this is
actually a book:
Updated --
1. ALDF-CDC "Enterprise" (read
"RICO") Conspires to Defraud USA in
Dearborn-Vaccine Scam; see how next, in the subsequent charge sheet
on patents, the very people who falsified the testing are the ones
who own the patents for the bogus vaccines and test kit products:
Updated -- 2. Lyme Disease Patents owned by the Dearborn scammers, CDC
officers, Yale in association with Corixa, Mayo Clinic and Imugen.
Leaving OspA and B out of the Dearborn standard was intended to
facilitate a monopoly on post-LYMErix approval on blood testing for
all vectior-borne disease:
Updated --
3. Lyme Disease
Biomarkers, as compared to scientifically
invalid psychiatric check lists. These biomarkers were identified by
the very people who later said Lyme was not even a disease, and who
are the same people who own the vaccine patents and falsified the
testing at Dearborn:
Updated --
4. The Primers (DNA, RNA) Shell Game; the very people who own all the
patents and falsified the testing for Lyme in order to falsify the
outcomes of those bogus products, use the wrong DNA to not-find Lyme
or other spirochetes in humans, while using the correct DNA to
patent borrelia-specific DNA; no biofilms.
Updated --
5.)
Occam's Razor If it
quacks like a duck, it must be Epstein-Barr/post-sepsis syndrome (as the
REAL "Great Imitator"):
Updated --
6. The Common Mechanisms of Fungal-Viral Damage in CFIDS,
Vaccines-Autism, and "Chronic Lyme"/ New Great Imitator, per the CDC,
NIH and IDSA; This paper reveals the CDC's own data on what Lyme and
CFIDS are, and how immunosuppression-via-fungal contamination also
explains the failed childhood vaccines, giving children the very
viruses the vaccines are intended to prevent (with resultant
encephalitis):
Updated --
7. Simon Wessely and the abuse of Gulf War veterans, Justina
Pelletier and 21st century witch trials; with scientifically valid
evidence for real illness, a vast majority of post-sepsis and
vaccine injured are slandered and libeled with invalid psychiatric
terminology:
Updated --
8. The State of Connecticut and Yale
Assaulted Czech Children
with a known fake vaccine (OspA or LYMErix) just to see how serious
would be the adverse events:
All in one pdf,
HERE
170131: Steere says "seronegative Lyme is a conflict in terms when talking about arthritis" meaning that after the Dearborn conference,
"Lyme Disease" officially became the arthritis, only (in the Munchausen's/Schoen lies book here (1998)>>
http://www.amazon.com/Lyme-Disease-Key-Diseases-Series/dp/0943126584/ref=sr_1_fkmr0_2?ie=UTF8&qid=1341914626&sr=8-2-fkmr0&keywords=lyme+disease+rhan+and+evans
Seronegative Lyme disease is a subtle, attenuated illness, says Steere, in 1998. He means "low antibody concentration" - see the Western Blots
in the RICO complaint to see the difference: http://www.actionlyme.org/USDOJ_COMPLAINT_RICO.htm The NeuroLyme patients are immunosuppression or Post-Sepsis Syndrome patients, with the variety show of illness signs. The cryme is that these patients were excluded from the case definition in the first step at the cryme scene of Dearborn, where Steere added the ELISA, which screened out Neurologic Lyme cases, and only kept the HLA-linked hypersensitivity outcomes (bad-knees). The reason they did this is because the early Phase I and Phase II trials of OspA as vaccines were underway, as revealed by CDC officer Alan Barbour and Yale's Durland Fish in this libelous, derogatory, misogynistic 1993 report.
161219 - Lyme Crooks Wormser and Steere - and even the "CDC
officer" criminal Paul Mead -
finally
admit Late Lyme and LYMErix diseases are immunosuppression outcomes.
'Say the "TLR2/1 agonism" (immunosuppression) is probably the "more
important" driver of the disease outcome.
Abstract (published Dec 15, 2016):
https://www.ncbi.nlm.nih.gov/pubmed/27976670
Full Text:
http://www.actionlyme.org/Steere_Wormser_Admit_Immunosuppression.2016_Dec_15.pdf
Mario Philipp has long been the guy who says Borrelia and OspA causes
immunosuppression, so look at all of his reports:
https://www.ncbi.nlm.nih.gov/pubmed/?term=Philipp+and+borrelia
Ref 79, above, (Mario Philipp): Interleukin-10
anti-inflammatory response to Borrelia burgdorferi, the agent of Lyme
disease: a possible role for suppressors of cytokine signaling 1 and 3.
https://www.ncbi.nlm.nih.gov/pubmed/16988256
The crooks report above, saying the more serious disease outcome may be
due to its fungal-ish agonism of TLR2/1, is a little bit of a screwed up way
of saying it, but they, the CDC and the Lyme criminals, finally admitted
their whole Lyme story was a lie.
Notice that ILADS has NEVER said what
Late Chronic Lyme was. They lost
their opportunity to be the ones to bring the truth forward as I had
predicted, also.
The next reports show
your "Post-Lyme disease" is actually "Post-Septic Shock
Syndrome," and depends on how much
OspA-ish antigens (triacyl/fungal lipoproteins) have ruined your immune
system. Whoever says "inflammation" or "autoimmunity" about Lyme in the same
sentence is a fraud (unless they're talking about autoimmunity to the
secondary infections, like MS or Lupus).
If people don't
believe me, they might as well believe Gary Wormser and take these 2 reports
to their "doctors" for a cure for post-sepsis syndrome (there isn't). Or at
least to help you get Social Security Disability.
The immunosuppression from a tick bite is a well known thing - from
the experiments trying to make a vaccine out of fungal lipoproteins for
Tuberculosis. They all failed the same way LYMErix failed (see the
Occam's Razor) - they made people
sicker and "more susceptible
to other infections."
https://crymedisease.wordpress.com/2016/03/20/gary-wormser-reports-global-immunosuppression-from-ospaborrelia/
Other people who say the CDC, ALDF.com, NYMC,
Harvard, Tufts, etc are criminal frauds on Lyme and LYMErix disease, and
that Lyme and LYMErix are diseases of immunosuppression and not the
opposite, inflammation or HLA-linked bad-knees:
Latov
Marks
Luft & Dattwyler (SUNY-SB - 1988 !!)
NIH (Fauci, Martin, Marques)
Cadavid
Persing and Schoen (Mayo, Yale)
Duray (US Army, & Yale)
Baumgarth and Barthold (UC Davis)
(Medvedev, Harding, Redmond, Philipp, etc)
---
2) Norman Latov
 Norman Latov
on how OspA vaccination caused the same disease as chronic Lyme:
Neuropathy and cognitive impairment following vaccination with the OspA protein
of Borrelia burgdorferi.
“Neurological syndromes that follow vaccination or infection are often
attributed to autoimmune mechanisms. We report six patients who
developed neuropathy or cognitive impairment, within several days to 2
months, following vaccination with the OspA antigen of Borrelia
burgdorferi. Two of the patients developed cognitive impairment, one
chronic inflammatory demyelinating polyneuropathy (CIDP), one multifocal
motor neuropathy, one both cognitive impairment and CIDP, and one
cognitive impairment and sensory axonal neuropathy. The patients with
cognitive impairment had T2 hyperintense white matter lesions on
magnetic resonance imaging. The similarity between the neurological
sequelae observed in the OspA-vaccinated patients and those with chronic
Lyme disease suggests a possible role for immune mechanisms in some of
the manifestations of chronic Lyme disease that are resistant to
antibiotic treatment.” http://www.ncbi.nlm.nih.gov/pubmed/15363064
3) Donald Marks
 Donald
H. Marks - an OspA vaccine trial administrator -
on how LYMErix caused the same disease as chronic Lyme:
Neurological complications of vaccination with outer surface protein A (OspA).
”A
wide range of neurological complications have been reported via the
medical literature and the VAERS system after vaccination with
recombinant outer surface protein A (OspA)
of Borrelia. To explore this issue, 24 patients reporting neurological
adverse events (AE) after vaccination with Lymerix, out of a group of 94
patients reporting adverse events after Lymerix vaccination, were
examined for causation. Five reports of cerebral ischemia, two transient
Ischemic attacks, five demyelinating events, two optic neuritis, two
reports of transverse myelitis, and one non-specific demyelinating
condition are evaluated in this paper. Caution is raised on not actively
looking for neurologic AE, and for not considering causation when the
incidence rate is too low to raise a calculable difference to natural
occurrence.”
http://www.ncbi.nlm.nih.gov/pubmed/21673416
[It's not “Autoimmune.”
It’s Subimmune. This Subimmunity represents the
entire class of the DSM's VooDoo
Somatoformia – as well as cancer. Cancer
is in the Subimmune class, at the other end of the immunity spectrum
from Autoimmunity. This fact or condition completely flips the entire
medical paradigm where you have to have a biomarker that is above-, or
more-than- the normal range. Lyme is not an inflammatory disease.
There are always negative correlations to biomarkers of autoimmunity or
illness or infection except when using sophisticated DNA techniques
using spinal fluid, in particular in these chronic, waste-basket
diseases. Henceforth, Autoimmunity will be an
obsolete word that connotes the previous Medical Establishment where BigPharma
is going to “block” something with their drugs. They are dinosaurs.
You can’t block a mechanism that is already permanently blocked and you
can’t unblock it.
It
could be that a person has an HLA-linked outcome to one of the secondary
infections like Epstein-Barr or HHV-6, reactivated by the AIDS-like Lyme
and LYMErix. Those people would for instance have the official,
hypersensitivity outcomes of MS or Lupus or whatever. But they are not
also called Incompetent Incantation-ators and they are not mistreated by
the entire universe (family, friends, Social Security, “doctors,”
everyone, including ILADS and the non profits).]
Who else says OspA alone is responsible for the immunosuppression with brain inflammation that is characteristic of "Chronic Lyme?"
4) Ben Luft SUNY-SB
 Ben Luft at the 1998 FDA Vaccine Meeting on LYMErix:
"The
point that I wanted to make in regard to the study is that there is very
heavy dependence on serologic confirmation. And when we start thinking
about the adverse events, ***
it was stated originally when we got the overview of the disease that
the disease is really quite protean. And actually the adverse events are
very similar to what the disease manifestations are.**** And if you
start to, as I think Dr. Hall was eluding to -- if you start to kind of
say well how often do you actually become seropositive, you can start to
have a different take on when someone has an adverse event or whether it
is disease specific or infection specific versus vaccine specific. And I
think that that is an important issue that we have to deal with. ..." http://www.fda.gov/ohrms/dockets/ac/98/transcpt/3422t1.rtf
5.)
Dattwyler and
Luft in 1989, in IDSA's own "journal," saying "treatment
fails in half the cases." And the OspA vaccine caused the same
systemic disease, say the crooks, themselves. See the
Occam's Razor report for who says so.
Steere was at this 1994 FDA meeting:
DATTWYLER: "-- the ones that (sic) failed to mount a vigrous immune response tended to do worse. So, there is an inverse correlation between the degree of serologic response and the outcome.
"So, individuals with a poor immune response tend to have worse disease."
1994 FDA Meeting Transcripts where Ray Dattwyler tells the FDA Vaccine Committee that the
patients with low or no antibodies are the sickest: http://www.actionlyme.org/Dattwyler_Luft_DNA_in_CSF.htm
Ray Dattwyler (SUNY-SB) says in 1988 that exposure to Lyme or even just its supernatants (OspA-like molecules) turn off the NK cell activity (or is immunosuppressive):
Effect of B burgdorferi Culture on Normal PBL
"...when lymphocytes are cultured in the presence of growing Bb there is
a marked inhibition ( p < .0005 ) of NK activity on days 3, 5, and 7 when compared to lymphocytes cultured in BSKII media in the absence of spirochetes. This effect is not due to a selective depletion or or toxicity to endogenous NK since viability studies and monoclonal antibodies demonstrate no significant changes after culture with the organism.
"The inhibition is directly attributable to the organism or its
supernatants from the organism also inhibit NK without prior exposure (data
not shown)."
Full Text:
Golightly,
1988.pdf
From: Modulation of natural killer cell activity by Borrelia
burgdorferi.
Golightly M,
Thomas J,
Volkman D,
Dattwyler R.
Department of Pathology, State University of New York, Stony
Brook 11794.
PMID: 3056196 [PubMed - indexed for
MEDLINE]
Ann N Y Acad Sci. 1988;539:103-11.
http://www.actionlyme.org/DATTWYLER_NK_SUPPRESSION.htm
Dattwyler on Seronegative Lyme and how that is like fungal diseases:
DOWNLOAD THE FULL TEXT of Dattwyler talking about seronegative, neuroLyme,
HERE:
dattwyler1988 (1).pdf
Lyme is like Jeopardy! Ask the right question: "Something that
causes a 'multi-system disease' and is
IDSA's own 'New Great Imitator.'"
The answer is, "What is OspA?"
6) Dave Persing, Mayo Clinic, Robert Schoen, Yale
Dave Persing who together with Yale’s Robert Schoen
developed this test in 1994 or 1995 says this about the similarities
between Lyme and LYMErix disease (you cant tell them apart):
"Additional uncertainty may arise if the vaccines are not completely
protective; vaccinated patients with multisystem complaints
characteristic of later presentations of Lyme disease may be difficult to
distinguish from patients with vaccine failure..."
http://patft1.uspto.gov/netacgi/nph-Parser?Sect1=PTO1&Sect2=HITOFF&d=PALL&p=1&u=/netahtml/PTO/srchnum.htm&r=1&f=G&l=50&s1=6045804.PN.&OS=PN/6045804&RS=PN/6045804
7.) THE NIH (Martin and Marques):
Borrelia
burgdorferi Induces TLR1 and TLR2 in human microglia and peripheral
blood monocytes but differentially regulates HLA-class II expression
(2006).
"The
spirochete Borrelia burgdorferi is the agent of Lyme disease, which causes
central nervous system manifestations in up to 20% of patients. We
investigated the response of human brain microglial cells, glial
progenitors, neurons, astrocytes, as well as peripheral blood monocytes to
stimulation with B. burgdorferi. We used oligoarrays to detect changes in
the expression of genes important for shaping adaptive and innate immune
responses. We found that stimulation with B. burgdorferi lysate increased
the expression of Toll-like receptors (TLRs) 1 and 2 in all cell types
except neurons. However, despite similarities in global gene profiles of
monocytes and microglia, only microglial cells responded to the stimulation
with a robust increase in HLA-DR, HLA-DQ, and also coexpressed CD11-c, a
dendritic cell marker. In contrast, a large number of HLA-related molecules
were repressed at both the RNA and the protein levels in stimulated
monocytes, whereas secretion of IL-10 and TNF-alpha was strongly induced.
These results show that signaling through TLR1/2 in response to B.
burgdorferi can elicit opposite immunoregulatory effects in blood and in
brain immune cells, which could play a role in the different susceptibility
of these compartments to infection."
http://www.ncbi.nlm.nih.gov/pubmed/16783164
The NIH-RML patent
explaining how Lyme causes LYMErix-disease (“stealth bomber”):
"The
invention relates to novel antigens associated with Borrelia burgdorferi
which are exported
(or shed) in vivo and
whose detection is a means of diagnosing Lyme disease. The antigens are
extracellular membrane vesicles
and other bioproducts including the major extracellular protein antigen.
Another object of the invention is to provide antibodies, monoclonal
and/or polyclonal, labeled and/or unlabeled, that are raised against the
antigens. A further object of the invention is to provide a method of
diagnosing Lyme disease by detecting the antigens in a biological sample
taken from a host using the antibodies in conventional immunoassay
formats. Another object of the invention is to provide kits, for the
diagnosis of Lyme disease, comprising the antibodies and ancillary
reagents. The advantage of the antibodies used in the invention is that
they react with the antigens from geographically diverse strains of
Borrelia burgdorferi, but do not react with antigens from related
Borrelia spirochetes."
http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO1&Sect2=HITOFF&d=PALL&p=1&u=%2Fnetahtml%2FPTO%2Fsrchnum.htm&r=1&f=G&l=50&s1=5,217,872.PN.&OS=PN/5,217,872&RS=PN/5,217,872
The shed blebs (or exosomes
or vesicles) have LYMErix on them (delayed fuse or “time bomb”):
Characterization of
multiprotein complexes of the Borrelia burgdorferi outer membrane
vesicles.
"Although we uncovered the existence of at least 10 distinct OM
complexes harboring several unique subunits, the complexome is dominated
by the frequent occurrence of a limited diversity of membrane proteins,
most notably P13, outer surface protein (Osp) A, -B, -C, and -D
and Lp6.6."
http://www.ncbi.nlm.nih.gov/pubmed/21875077
UCSF says Lyme and LYMErix-Disease are a diseases of
immunosuppression, and they say that half the Lyme/tick bite victims
remain ill and are not cured with antibiotics
Feb 12, 2016:
“Early Lyme disease prior to antibiotic therapy was characterized by marked
upregulation of Toll-like receptor signaling but lack of activation of
the inflammatory T-cell apoptotic and B-cell developmental pathways seen in
other acute infectious syndromes,” wrote the study’s authors. “Six
months after completion of therapy, Lyme disease patients were found to have
31 to 60% of their pathways in common with three different immune-mediated
chronic diseases. No differential gene expression signature was observed
between Lyme disease patients with resolved illness to those with persistent
symptoms at six months post-treatment.”
"Six months after treatment, 15 of the 29 patients in the study had
fully recovered, while 13 had persistent symptoms, and one had dropped
out."
http://www.genengnews.com/gen-news-highlights/lyme-disease-may-be-diagnosable-via-transcriptome-signature/81252365/
8.) BAUMGARTH and BARTHOLD
See more below from UC Davis, and in the
Occam's Razor report. The Great
Imitator is EBV, the Great Initiator is the fungal antigen OspA, shed by
spirochetes - their own phylum, and not regular "bacteria" -
on blebs, says the NIH.
America is a really stupid country, when you consider that nearly every
disease is an outcome of the first immune disordered step - inhibition of
apoptosis of infected B cells.
Look at the experience of Lewis Bull, East Lyme, CT,
back in the OspA "vaccines" trials days (late 1990s) to see exactly what
these evil bastards of the CDC (Barbour, Johnson, Steere) had planned from
the beginning to do with LYMErix - "multisystem
(read: "sepsis")," Chronic Fatigue Syndrome-like - outcomes.
'Says it all.
University of California, Davis, says the
CDC, Allen
Steere, Gary Wormser, Edward McSweegan, et al
must be lying their faces off:
Lyme
and LYMErix cause permanent immunosuppression or is like a B cell AIDS.
http://www.ccm.ucdavis.edu/our-science/lyme-disease
Lyme is not an "inflammatory," "autoimmune disease," it is the
Great Initiator of latent viruses, as
a fungal antigen shedder, SPIROCHETE (its own phylum). Fungal antigens
like triacyl lipopeptides (OspA) have always been known to cause
immunosuppression. The complete opposite of an "autoimmune" or
"inflammatory" disease. The only
biomarkers
will be signs of nerve and brain degradation in the cerebral spinal fluid;
no antibodies in the blood.
So what
exactly is OspA?
“I did not get the vaccine so this does not concern me.” Oh,
yes, you got the vaccine. Everyone with Lyme got LYMErix. Here is what
LYMErix is, and how this "vaccine-was-the-disease" works:
This is image is of Pam3Cys
or OspA. What is variable is the protein end "("peptide"), but what is
immunogenic (seen as an invader to the immune system) are the fatty acids or
acyl groups and the very electronegative cysteine core:
Pam3Cys is a triacylated lipoprotein, the degree of acylation is
equated with its toxicity. So what is acylation? It’s the zig-zaggy
lines that mean Carbon-Carbon-Carbon, yes, hydrocarbons, like margarine
or octane. Exactly, the name just refers to the number of carbons in
each carboxyl or acyl group. Palmitic (the Pam in Pam3Cys) has X number
of carbons, gasoline, 8, linoleic acids, like 14. Look up what are
alkanes then add a COOH group and you have one of these fatty acids.
Something highly acylated like this (3 or more fatty acids hanging off)
are managed by Toll-like Receptor (TLR) 2 and TLR1, together.
Therefore a “TLR2/1-agonist” is another term that generally refers to
lipoproteins like those from Borrelia, mycoplasma, mycobacteria, and
others like Brucella. (But they can manage other compounds.)
This thing, Pam3Cys and fungal lipid molecules like it, is shed with the
blebs. In other words, like this:
The
likes of OspA is on these blebs. They go to the brain, inflame it, get
eaten up by immune cells - which renders them incompetent-, they go to
the kidneys (LUAT), etc. You will find this to be so in an NIH-owned
patent (5,217,872) and elsewhere.
So, the fungal antigens are on the shed blebs and they go everywhere and
they render the immune cells incompetent, resulting in an AIDS-like
disease. Everyone who has Lyme disease also has LYMErix disease.
9 .)
Cadavid and the NIH say these shed
vesicles or blebs go to the brain and
inflame it:
http://www.ncbi.nlm.nih.gov/pubmed/?term=Cadavid+and+borrelia+and+brain
In other words, the NIH is saying that thanks to exposure to shed blebs
with TLR2/1 agonists like OspA on them, the HLA molecules will be
downregulated and that you will make no antibodies. This
mechanism is mimicked elsewhere, in other fungal diseases models. It
is also CALLED endotoxin tolerance.
Endotoxin Tolerance Inhibits
Lyn and c-Src Phosphorylation and Association with Toll-Like Receptor 4
but Increases Expression and Activity of Protein Phosphatases.
“Endotoxin tolerance protects
the host by limiting excessive 'cytokine storm' during sepsis, but
compromises the ability to counteract infections in septic shock
survivors.
It reprograms Toll-like receptor (TLR) 4 responses by attenuating the
expression of proinflammatory cytokines without suppressing
anti-inflammatory and antimicrobial mediators, but the mechanisms of
reprogramming remain unclear. In this study, we demonstrate that the
induction of endotoxin tolerance in
human monocytes, THP-1 and MonoMac-6 cells inhibited lipopolysaccharide
(LPS)-mediated phosphorylation of Lyn, c-Src and their recruitment to
TLR4, but increased total protein phosphatase (PP) activity and the
expression of protein tyrosine phosphatase (PTP) 1B, PP2A, PTP
nonreceptor type (PTPN) 22 and mitogen-activated protein kinase
phosphatase (MKP)-1. Chemical PP inhibitors, okadaic acid, dephostatin
and cantharidic acid markedly decreased or completely abolished LPS tolerance,
indicating the importance of phosphatases in endotoxin tolerization.
Overexpression of PTPN22 decreased LPS-mediated nuclear factor
(NF)-x03BA;B activation, p38 phosphorylation and CXCL8 gene expression,
while PTPN22 ablation upregulated LPS-induced p65 NF-x03BA;B and p38
phosphorylation and the expression of TNF-α and pro-IL-1β mRNA,
indicating PTPN22 as an inhibitor of TLR4 signaling. Thus, LPS tolerance interferes
with TLR4 signaling by inhibiting Lyn and c-Src phosphorylation and
their recruitment to TLR4, while increasing the phosphatase activity and
expression of PP2A, PTPN22, PTP1B and MKP1.
http://www.ncbi.nlm.nih.gov/pubmed/26457672
10)
Anthony Fauci:
NIAID.gov Director Anthony Fauci actually owns a patent for the treatment
of immunosuppression diseases like
Lyme,
other fungal diseases, like inhalation crypto-mold and Tuberculosis.
"Doctors" don't know what are the
diagnostic
codes for post-sepsis syndrome, so they cant really help you get
Disability, and that is why none can help you in any way. See the
link, below, to the "Big Picture"/Fauci page for that data.
We can tell you what the disease *is,*
but we cant tell you how to train your "doctors" to help you.
Sorry.
We're at a total loss if people with "MD" after
their names cant see the obvious. That is the thing
about cults, like cop cults and jail guard cults and government employee
cults. The cult protects itself, first, that is one
of the primary characteristics of a cult. The second it that the cult
leaders tell the cult members that there is something SPECIAL !! about them,
or that they are UNIQUE !! or owners of SPECIAL, SECRET KNOWLEDGE !!
(appealing to vanity).
The best example I can think of it psychiatry: The head of NIMH said it
was all bogus, invalid, and crazy bullshit (Thomas
Insel) but few to none of the rest of them say it. In
fact, there is a push on now to get more psychiatrists to literally drug
more children. Yes, that was their claim. They
need more non-valid, non-scientific "MDs"
to sell the brain-damaging psych drugs to children. And
this is while the head of the NIMH said none of this DSM bullshit was real.
There is no National Institute of Immunosuppression outcomes to
Infectious Diseases (NIIID), there is only the opposite, *ALLERGY,* or "too
many antibodies" or "autoimmune diseases" - of which ANTHONY FAUCI is the
head (NIAID). Yet, you can see here that Fauci knows
all about the immunosuppression/opportunistics (EBV) outcomes of fungal
diseases like Lyme and other infections that cause chronic
fatiguing/dementia-causing post-sepsis syndrome, here (he has a patent for
the treatment of it).
Why, you may ask, does the HHS.gov abuse us? We suggest reasons in the
article linked below, and they're even more sinister than the
abuse of tick bite sepsis victims that you have seen so far.
https://crymedisease.wordpress.com/2016/12/11/big-picture-and-fauci/
See more at:
http://www.actionlyme.org/151026_OCCAMS_RAZOR.htm
OspA or the
LYMErix vaccine was Pam3Cys; here we find it loosens the blood brain
barrier permanently, as part of the damage:
https://www.ncbi.nlm.nih.gov/pubmed/27493242
OspA or the LYMErix vaccine or the fungal triacyl lipopeptide causes
immunosuppression and permanent brain damage, but the US Govt only tortured
us instead of thanked us for blowing the whistle on it and forcing it off
the market.
Where are our heroism or public service medals? Not gonna
happen, why?
COWARDICE.
Cryme Disease. Here is how it works:
B cells eat OspA-ish, fungal-ish antigens (highly lipidated) and then go
limp (no longer do their jobs; this is called tolerance, there are no
antibodies being produced).
And so do you, go limp (post-sepsis, or endotoxin tolerance and
cross-tolerance is the same thing as Chronic Fatigue Syndrome or
Fibromyalgia).
The psychopaths who "work" for the CDC and Yale said this OspA fungal
endotoxin was a "vaccine," the opposite.
So, the cryme, saying OspA was a vaccine, is actually the
disease, post-sepsis immunosuppression, with reactivated latent
herpesviruses, etc. It's simple.
They used to put
Thimerosal in vaccines
to prevent fungal growth - or OspA-ish antigens -, because such fungal
antigens cause immunosuppression. (You can't make this up:
Thimerosal was invented to prevent the OspA Lyme "vaccines.")
See more at
Cryme Disease, the movie: https://vimeo.com/180529812
Join us
at:
https://www.facebook.com/groups/OccupyUSDOJ/; ours is the only group
that explains this disease to you, and shows you the current status of the
disease and testing for it. However, it is an activism group whose
goal is to have the CDC and Yale crooks busted by the USDOJ.
We offer no treatment notions, because there really aren't any.
(Please do NOT even ask, that's not what we do.)
UCSF says Lyme and LYMErix-Disease are a diseases of
immunosuppression, and they say that half the Lyme/tick bite victims
remain ill and are not cured with antibiotics
Feb 12, 2016:
“Early Lyme disease prior to antibiotic therapy was characterized by marked
upregulation of Toll-like receptor signaling but lack of activation of
the inflammatory T-cell apoptotic and B-cell developmental pathways seen in
other acute infectious syndromes,” wrote the study’s authors. “Six
months after completion of therapy, Lyme disease patients were found to have
31 to 60% of their pathways in common with three different immune-mediated
chronic diseases. No differential gene expression signature was observed
between Lyme disease patients with resolved illness to those with persistent
symptoms at six months post-treatment.”
"Six months after treatment, 15 of the 29 patients in the study had
fully recovered, while 13 had persistent symptoms, and one had dropped
out."
http://www.genengnews.com/gen-news-highlights/lyme-disease-may-be-diagnosable-via-transcriptome-signature/81252365/
Baumgarth, UCDavis:
"For months after infection, those germinal centers fil to produce the
specific cells -- memory B cells and antibody-producing plasma cells --
that are crucial for production of lasting immunity. In effect, the
bacteria prevent the animal's immune system from forming a "memory" of
the invading bacteria and launching a protective immune response against
future infections.
"The researchers found that following Borrelia burgdorferi infections,
this process even prevented the induction of strong immune responses to
an influenza infection."
https://scienceblog.com/79136/lyme-disease-subverts-immune-system-prevents-future-protection/#hiCzbjF13JBLGgQF.97
Ray Dattwyler, 1989, in IDSA's journal:
http://www.actionlyme.org/IDSA_TMTFAILS.htm
They're obviously all saying the same thing, from 1989 until 2016.
You have a 50% chance of being effed for life if you are bitten by a
tick, because the disease is really about immunosuppression, like AIDS.
ONLY IN the United States of
STUPID could
you see the likes of the
ALDF.com's founders,
Edward McSweegan and
Durland Fish,
not knowing
spirochetes were their own
phylum (are not regular "bacteria"), are relapsing fever
organisms, that the
nature of the relapse
was antigenic variation (vaccines would do no good), and that the
McSweegan-Fish gang never even asked what
OspA
was
(fungal, TLR2/1 agonist, causes permanent immunosuppression, never could have been a
vaccine). The CDC deployed the stupid
and cowardly Allen Steere who
went into
Rheumatology to avoid VietNam
(there are no old ladies who need aspirin among deployed US combat forces),
probably because he was known to be too stupid to ask any questions about
ticks or spirochetes.
What is the simplest way to explain that the
ALDF dot com / Yale / CDC Lyme cabal
threw out of the Dearborn, "2-tiered" "case definition" the
very same disabling, chronic neurologic, "New
Great Imitator" disease that was caused by the
fungal toxin, Pam3Cys or OspA?
They knew OspA vaccination causes
neurologic, immunosuppression disease before the Oct 1994
Dearborn, Michigan fake consensus conference ever took place (chronology
here).
In order for it to be prosecuted as
a
criminal case you have to show they knew ahead of time that there was
this problem with their "vaccine" choice and that they CHANGED the
testing definition after that, such as to leave out the chronic
neurologic Lyme definition - the very disease caused by the fungal OspA vaccines.
This is from June, 1993, by Alan Barbour and
Durland Fish:
http://www.actionlyme.org/BarbourFishpdf.pdf
They said this ˄ BEFORE the CDC's Dearborn-"Let's-Leave-Out-the-Chronic-Neurologic-Form-of-the-Disease-Which-Is-Also-Caused-by-OspA-Injection-Alone"
fake consensus conference took place (Oct, 1994). So, these
criminals would have known there was a problem with OspA injections making
people sick. After all, OspA is a fungal endotoxin, TLR2/1-agonist.
The current, 1994, "Dearborn" case definition only detects the 15% of cases, only the late-, HLA-linked- arthritis cases, no early cases, and then
these CDC (vaccine patent holding) criminals say
this late manifestation needs no treatment. The truth is that chronic
neurologic disease is mainly caused by immunosuppression, reactivated
Epstein-Barr and cross tolerance to other infections, or, technically, is
post-sepsis syndrome or a kind of a B cell AIDS (see the
Occam's Razor).
In this criminal case, you have to show to the
DOJ that they
CHANGED the
diagnostic criteria from an older one that allowed more people to be
diagnosed (the
1990 CDC version).
If the DOJ does not respond, clearly this was a bioweapon accident of some
sort.
The circumstantial scientific,
epidemiological evidence from
Plum Island as the original outbreak area says so. (Do
the Russians know by now? They knew in 2006. The Chinese, a year
later. Site stats.)
The US press cant handle it, and no
one has ever written about it in any book.
Whoever does not know
what Lymerix-disease is, does
not know what Lyme disease is. This includes ILADS dot org and
all the Lyme non-profits. One has to know what the antigen is,
in order to know what it does. Ad it turns out, that Lyme and
Syphilis as "Great Imitators" are really Great Detonators of latent
viruses and general immunosuppression, also known as post-sepsis
syndrome. It turns out that Pam3Cys (OspA) or triacyl
lipopeptides are functional mimics of E. coli's Lipid A, a serious
fungal (TLR2/1-agonist ENDOTOXIN. Think about that. The
CDC wanted to inject everone with several blobs of bathroom scum.
And that's what happens with a tick bite, too.
Baumgarth, UCDavis:
"For months after infection, those germinal centers fil to produce
the specific cells -- memory B cells and antibody-producing plasma
cells -- that are crucial for production of lasting immunity.
In effect, the bacteria prevent the animal's immune system from
forming a "memory" of the invading bacteria and launching a
protective immune response against future infections.
"The researchers found that following Borrelia burgdorferi
infections, this process even prevented the induction of strong
immune responses to an influenza infection."
https://scienceblog.com/79136/lyme-disease-subverts-immune-system-prevents-future-protection/#hiCzbjF13JBLGgQF.97
Cadavid on Septic Spirochetes:
"Finally, spirochetal lipoproteins have more prominant
pro-inflammatory effects compared to other bacterial lipoproteins
and synthetic lipopeptides (28)."
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4075078/
I heard through the grapevine that GSK and others
involved are intending to "throw Allen Steere under the bus" (verbatim) for
this crime of
falsifying the testing.
I replied to that insider that that would not be throwing him under
the bus because he really was the one who falsified the testing in Europe
(Germany; why Germany?).
This video, inside this blog post, has done what the non-non-profits have
never been able to do in ~30 years: Explain the crime, and give you
some actionable intelligence - what you can do.
https://badlymeattitude.com/2016/12/04/lyme-math/
Two important bits of news
came out mid-November, 2016.
One was regarding how the
Epstein-Barr virus - and fungal antigens like those shed by spirochetes
- inhibit
apoptosis (search for that term here) of
infected cells, rendering them "immortalized" (you could call them B cell
zombies, really) or "immature" or "Epstein-Barr
transformed" B cells, causing cancer or chronic fatigue syndrome or
"chronic Lyme."
The truth is in the BCL2 class genes,
manipulation of apoptosis. Dysfunction, here, is the first
step in nearly all disease.
And the other was about
the FDA telling Senators Blumenthal, Durbin,
et al, to "Screw Off," that "No," the FDA
"would not be doing their jobs, assuring
Lyme or any other testing is valid."
You
heard it all
here first, folks.
And all along.
The FDA did not even look at the falsified case definition for "Lyme
disease" (1994, Dearborn) when they "approved"
LYMErix, obviously. I did that for them. LYMErix was the
opposite of a vaccine, the case definition was falsified by
Allen Steere in Europe and the CDC at
Dearborn, and the FDA finally ordered it off the market with an ultimatum to
SmithKline after the November 2001 hearing on adverse events that were
not "bad knee" but the
systemic
post-septic shock disease we call "Chronic Lyme, - the very outcome
that was left out of the case definition in 1994 when the CDC falsified it.
Government Welfare. Everyone should have such a Govt job to not
only do nothing, but put out proclamations about how they're not
going to do their jobs even when specifically asked to do so by the
legislators. Good one.
And ILADS.org and the "non-profits" of Lyme? They can't and
haven't told you anything about these 2 phenomena: How
OspA alone causes chronic illness as a
fungal toxin, reactivating Epstein-Barr via immunosuppression, or
how if the FDA was forced to do their jobs,
Yale and the CDC
criminals would be prosecuted for falsifying the case definition to
leave out this very
immunosuppression
and "reactivation of EBV, et al" result.
There it is. No one who alleges to "help" you, can or will.
There it is, from the fake non-profits to the black market "LLMDs," to
blowhard "lawyers" who don't know "data" from "hearsay," to the FDA
either in the past or presently, and who now issue their own demands
about what they're not gonna do from now on... to the CDC,
NIH, to the HHS.gov to the ends of the earth. Exceptional America,
can't or won't do what they claim to be. No how no where not ever.
But they want you to worship them.
You should be shocked. There it all is, right there. ILADS
and the non-profits have made no announcement regarding these 2 news
items that came out this week. We checked. They can't.
You live in one big giant asylum. Put the walls up, Mr. Trump.
Close the ports....
161118; In case you just fell off the
cabbage truck yesterday,
"Lyme disease" is not
even a real thing. Spirochetes ruin your immune system by
shedding fungal antigens, by going directly to and damaging the B cell
germinal centers in the
lymph nodes, and by reverting
to a spheroplast form in hostile environments (antibiotics or spinal fluid).
But the CDC staff members formed a fake non-profit called the
ALDF dot com and held a bogus conference in Dearborn MI,
in 1994 to falsify the diagnostics of this primarily immunosuppression
disease. It was the only way they could sell their own
patented DNA for test kits
and vaccines.
So, "Lyme disease" became only the HLA-linked hypersensitivity outcome or
arthritis (this is
FRAUD and Racketeering).
Fungal-ish antigens shed by spirochetes are more serious endotoxins than the
typical lipopolysaccarides of common bacterial infections. TLR2/1
agonists (fungal-ish, or triacylated lipoproteins) such the
shed Outer Surface Proteins (Osps)
and the Variable Major Proteins (Vmps) of Borreliae cause disease by turning
off the immune system to more than just other fungal antigens. This is
called
cross-tolerance.
And
Yale University said
this dangerous, moldish, bathroom scum-type toxin, a triacyl lipoprotein,
OspA, was a "vaccine"
rather than an immune-suppressing, sepsis-causing toxin.
New, 161118;
Exported Fungal OspA-ish Antigens Also Inhibit Apoptosis and that
is how they cause disease.
You've read about this mechanism in the
Occam's Razor and
elsewhere on ActionLyme since
2004.
http://www.the-scientist.com/?articles.view/articleNo/47548/title/How-Epstein-Barr-Virus-Hijacks-B-Cells-To-Cause-Blood-Cancer/
New: How to Un-Break Americans' Brains:
Keep Hitting them Over the Head With the Obvious. There is no National
Institute of Post-Sepsis or Immunosuppression Diseases (NIIID), because to
do so would betray the source of the Autism pandemic. (Yet you
hear these things every day on the TV commercials.)
"Translational Medicine" - Hilarious:
'Something Rockefeller University
studied and knew about in 1922: that spirochetes are permanent infections
and live in the lymph nodes, destroying immunity,... and we hear about it
again in 2015 by a lady scientist,
Nicole
Baumgarth!!
I would say that was OUTSTANDING "translational" medicine, where all the
words and years in between were lost,... and we had to have the
Craazy Eddie McSweegan gang and a fake
FUNGAL lipoprotein Lyme vaccine. And no one in the ENTIRE
HHS.gov ever asked what OspA was, nor to this day will admit what OspA was (Pam3Cys).
Good translating. Good word-saying, all around. Needs 27
million more dollars....
Go ahead, check it:
https://www.ncbi.nlm.nih.gov/pubmed/?term=spirochetes+and+lymph+nodes+and+rockefeller
University of California, Davis, says the
CDC, Allen
Steere, Gary Wormser, Edward McSweegan, et al
must be lying their faces off:
Lyme
and LYMErix cause permanent immunosuppression or is like a B cell AIDS.
http://www.ccm.ucdavis.edu/our-science/lyme-disease
Great translating from 1922.
'Needs more money because the NIH has not donated enough to that cesspool
called the Ivy League, for them to still not understand what spirochetes
are/do, despite a million new cases of DISABILITY per year in the USA,
alone.
Why doesn't the CDC want you to know that Post-Lyme and
Chronic Fatigue/ME is really
Post-SEPSIS-Syndrome?
http://www.businessinsider.com/flawed-lancet-study-me-cfs-chronic-fatigue-2016-9?r=DE&IR=T
Because the mechanisms of illness - acquired immune deficiency
particularly from the likes of TLR2-agonists or
fungal-antigen-bearing/shedding infections or even contamination of
childhood vaccines with the likes of a fungal antigen like LYMErix -, are
the same in Post-Sepsis and Vaccine-Damage Autism.
The reason the babies are actually
GETTING those live, attenuated, brain-tropic viruses from the vaccine vials
is due to immunosuppression and/or contamination causing the
immunosuppression.
The reason someone came up with the idea for a Rubella vaccine in the first
place was because Rubella causes the
neurodevelopmental brain damage we call
"Autism." Think about it. The kids are GETTING the VIRUSES and
they're all brain-tropic.
The Infectious Diseases Society of America says these vaccines are given too
many, too young, and are not properly vetted -
please see for
yourself, their exact language; the adverse events are a lot like sepsis
events.
http://www.vimeo.com/truthcures <<< See all 3 videos, they are all
related, and you'll see - finally - that this is simple, and regarding
models of disease you know about and have seen before (dual infections and
synergy).
The Autism pandemic is the result of babies getting the actual brain-tropic viruses that are in the vaccine
vials,
either because those children are immunosuppressed or because
the vaccines are contaminated with the likes of fungal antigens like LYMErix.
Yes, the *ENTIRE* HHS.gov is that stupid. Add to that, everyone with
"MD" after their names. YES, ALL OF THEM are THAT
STUPID.
You have seen the MRIs of the heads of the ZIKA
brain damaged children in the news. The scientific literature says
Borna virus is the model for the "neurodevelopmental brain damage" we call
Autism.
The
IDSA says vaccines are given too many, and too young, and none of them are
properly vetted, and this was true since the 1970s. The scientific
literature on those MMR qualifications shows those children were never
followed longer than a few days. The MMR vaccine qualifications were
even more criminal than the LYMErix stunt. Go look for yourself on
Pubmed. You'll do it if you give a sh*t about other people. But
if you don't, you won't bother.
It is the same with activism, in general.
If you are looking for the very simplest explainer
on the Lyme crymes,
see the RICO
complaint already filed with the USDOJ. I was talking to
lawyers after all, so I had to really dumb it down.
Cryme Disease, the movie:
https://vimeo.com/180529812
The fungal-ish OspA vaccine caused the
same
post-sepsis, immunosuppression
disease as the one thrown out of the case definition at
Dearborn.
Steere used a seronegative Lyme assay to assess chronic neuro Lyme, a
disease he later
falsified and now claims
never existed.
Steere recently claimed in a radio interview that (June 14, 2016) he
never knew Lyme caused a chronic neuro outcome. The CDC would
like to throw Allen Steere under the bus,... and Steere is trying to avoid
being thrown under the bus. Obviously not happening.
IF you are the kind of person
who wants a simple one-liner, single model, single, simple general idea
to explain something, this would be it (Dattwyler and Fauci, below).
OspA is a known immune-suppressor, not a "vaccine."
We are not about to prove that OspA is a triacyl lipoprotein also called a
basic Pam3Cys molecule type, is fungal, is a more serious endotoxin than
LPS, a TLR2/TLR1 agonist, and that other spirochetal lipoproteins are
triacylated, if not Pam3Cys exactly. We can assume anyone knows how to use
the National Library of Medicine or else the United States and European
patent databases or even just pull the one arm of one-armed information
bandit named Google and discover that, for instance, State University of New
York, Stony Brook’s, Raymond Dattwyler has a patent for an inhalation form
of OspA.
It, the OspA in Dattwyler’s OspA patent, is intended to attenuate (lessen,
or dampen) any suffocating inflammatory response people might suffer from
the likes of the dual infections of, for example, influenza and pneumonia,
such as what happened in the 1918 Spanish Flu epidemic [FAUCI]. During that
pandemic, the healthy people succumbed to the secondary pneumonia. That is,
the strong, mucus-y inflammatory response is what killed 20+ million people
back then. They choked to death. (One infection invites another, this is
well-known).
Let’s just go ahead and have a look
at what Raymond Dattwyler says about OspA as Pam3Cys and how inhaling a
fungal antigen like this, OspA or Pam3Cys or a triacyl lipoprotein might
tolerize you against the deadly pneumonia part of Pandemic
Flu-moniaâ:
(US20090324638)
LIVE BACTERIAL VACCINE
"A lipidation/processing
reaction has been described for the intact OspA gene of B. burgdorferi. The
primary translation product of the full-length B. burgdorferi OspA gene
contains a hydrophobic N-terminal sequence, of 16 amino acids, which is a
substrate for the attachment of a diacyl glyceryl to the sulflhydryl side
chain of the adjacent cysteine (Cys) residue (at position 17). Following
this attachment, cleavage by signal peptidase II and the attachment of a
third fatty acid to the N-terminus occurs. The completed lipid moiety, a
tripalmitoyl-S-glycerylcysteine modification, is termed Pam3Cys (or is
sometimes referred to herein as Pam(3)Cys or Pam3Cys). It has been suggested
that the lipid modification allows membrane localization of proteins, with
polypeptide portions exposed as immune targets. In addition to serving as
targets for the immune response, Pam3Cys-modified proteins, such as OspA,
have been reported to act as potent inflammatory stimulants though the
toll-like 2 receptor mechanism (TLR2).
http://patentscope.wipo.int/search/en/detail.jsf?docId=US42934470&recNum=9&maxRec=30&office&prevFilter&sortOption=Pub+Date+Desc&queryString=tripalmitoyl+cysteine+or+Pam3Cys+and+Epstein-Barr&tab=NationalBiblio
NIAID's Chief Anthony Fauci on the 'monia part of 1918
Spanish Flumonia®
being what causes people to choke to death -- it was inflammatory response
in the lungs to the fungal-ish pneumonia:
Predominant role of bacterial pneumonia as a cause of death in pandemic influenza:
implications for pandemicinfluenza preparedness.
Abstract
BACKGROUND:
Despite the availability of published data on 4 pandemics that
have occurred over the past 120 years, there is little modern
information on the causes of death associated with influenza pandemics.
METHODS:
We examined
relevant information from the most recent influenza pandemic
that occurred during the era prior to the use of antibiotics,
the 1918-1919 "Spanish flu"
pandemic. We examined lung tissue sections obtained during 58
autopsies and reviewed pathologic and bacteriologic data from
109 published autopsy series that described 8398 individual
autopsy investigations.
RESULTS:
The
postmortem samples we examined from people who died of influenza during
1918-1919 uniformly exhibited severe changes indicative of
bacterial pneumonia. Bacteriologic and histopathologic results
from published autopsy series clearly and consistently
implicated secondary bacterial pneumonia caused by common upper
respiratory-tract bacteria in most influenza fatalities.
CONCLUSIONS:
The majority of deaths in the
1918-1919 influenza pandemic
likely resulted directly from secondary bacterial pneumonia
caused by common upper respiratory-tract bacteria. Less
substantial data from the subsequent 1957 and 1968 pandemics are
consistent with these findings. If severe pandemic influenza is
largely a problem of viral-bacterial copathogenesis, pandemic
planning needs to go beyond addressing the viral cause alone
(e.g., influenza vaccines
and antiviral drugs). Prevention, diagnosis, prophylaxis, and
treatment of secondary bacterial pneumonia, as well as
stockpiling of antibiotics and bacterial vaccines, should also
be high priorities for pandemic planning.
http://www.ncbi.nlm.nih.gov/pubmed/18710327
So, if OspA was obviously something that causes
too-much inflammation-and-then-immunosuppression (endotoxin tolerance), it
could not have been a vaccine. And if OspA was not a vaccine, then
certain people not only lied it onto the market, they falsified the Dearborn
case definition to leave out the 85% of us who do not have a genetic
background for a tendency to have Rheumatoid Arthritis (HLAs).
So, IF you are the kind of person who
wants a simple one-liner, single model, single, general idea to explain
something, this would be it. OspA is a known immune-suppressor, not a
"vaccine." It does the OPPOSITE of what vaccines are intended to do,
which is produce antibodies. It is a more severe endotoxin than LPS.
"TLR2 mediates inflammatory responses to a wide variety of lipidated
microbial components, including bacterial lipoproteins, atypical
lipopolysaccharides, and lipomannans (26–28).
Among these microbial agonists,
bacterial lipoproteins are by far the most potent
(26, 29–31)."
https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3617275/
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