RECENT
The following is the ammo by which Big Pharma can be
brought to its knees, and the holocaust of autoimmune diseases and cancer in
people and in pets stopped at last. I ask you to circulate it widely.
It is time for you to DEMAND that those promoting mercury as the cause of
autism respond to what I have written below. If the true intention of
these people is to stop this epidemic in our children, then they should let go
of their egos and admit that I have figured out the true cause. Let me
first encourage of all you to go to http://thelightofdayradioshow.com/archives/RBN-BACKUP/the_big_picture.jpg; you will see that
I have ALWAYS said it is the BIG PICTURE of assaults to our immune systems (and
mercury is there) which combine to cause disease, including autism. But it
is the corruption of the immune system caused by the inoculation of viruses
which is the root cause of all autoimmune diseases and cancer...and once this
information is in the hands of a critical mass of the people, we will put a stop
to the biggest epidemic the world has ever known...VIDS (Vaccine Induced
Diseases). And the individuals who continue to promote mercury as the root cause
in the face of this information will be exposed for being INTENTIONAL
disinformers.
Below is a verbatim copy of the US Government concession
filed in November of 2007 in a Court of Federal Claims case brought by
neurologist Dr. Jon Poling and his wife claiming that vaccines were the
cause of their daughter Hannah's autism. This decision is posted on David
Kirby's blog at http://www.huffingtonpost.com/david-kirby/the-vaccineautism-court-_b_88558.html.
David Kirby, author of "Evidence of Harm", is one of the individuals
who is distracting the public that autism is "all about the thimerosol".
The take home message therefore is that if the mercury is removed,
vaccines will be safe. A BIGGER LIE HAS NEVER BEEN TOLD; and my document
"Inoculations the True Weapons of Mass Destruction" posted on http://www.drcarley.com/
describes the corruption of the immune system caused by the injection of viruses
directly into the body, bypassing secretory IgA (an antibody in the upper GI and
respiratory tracts critical for the processing of germs by the immune system for
natural immunity to occur).
I was a guest with David Kirby on a radio
show which is posted on my website at http://thelightofdayradioshow.com/archives/RBN-BACKUP/kirby_vs_carley_autism.mp3, on which I
confronted him with the fact that autism is actually a non-fatal case of
subacute sclerosing panencephalitis caused by demyelination following vaccine
induced encephalitis, and that the name of the condition was changed to autism
to hide this self evident fact. I have sent Mr. Kirby copies of the
documents on my website, and asked him multiple times to be a guest on one of my
internet shows to discuss the "mercury vs demyelination" theories of autism.
He will not do so.
What is truly amazing is that he is now
mentioning live viruses amongst a plethora of other potential problems (see # 6
at http://www.huffingtonpost.com/david-kirby/government-concedes-vacci_b_88323.html)....but ). But is he discussing the live viruses
bypassing secretory IgA, causing vaccine induced encephalitis and subsequent
demyelination? NO...he is mentioning live viruses as a cause of
mitochondrial damage. So once again, we will now be distracted with this
genetic mitochondrial defect...perhaps develop a test to find the children with
this problem before they are vaccinated, when in fact genetic defects can also
be caused by vaccines. More confusion and distraction...rather than
admitting that there is no such thing as a safe vaccine...and the practice
should be abandoned altogether, with attention instead placed on strengthening
the immune system. Of course, since population reduction is the true
agenda of the powers that be, not only will the vaccine push continue...but
viruses are being developed to cause cancer under the Special Virus
Cancer Program. The mad scientists have to be stopped...and this WILL
happen once enough people have opened their eyes to the true purpose of
vaccines.
I urge all of you to carefully read this decision dated
11/9/07, in which this young girl won her case claiming vaccines caused her
autism. Note these important points:
1. 2 days after multiple
vaccines (which included the MMR, which has NEVER had mercury), she developed a
high fever, high pitched screaming, and was lethargic and
irritable. These are symptoms of VACCINE INDUCED ENCEPHALITIS, an
inflammation of the brain caused by injection of LIVE VIRUSES (not from
mercury).
2. She also began to arch her back when she cried (a
sign of vaccine induced encephalitis, NOT mercury poisoning).
3.
She developed a POST-VARICELLA VACCINATION RASH (which proves that
the vaccination GAVE HER THAT DISEASE). As explained in the quotes from
Harrison's Principles of Medicine, 6th edition, p. 943 posted in my response
to the CDC on http://www.drcarley.com/, "RARELY IS PREVENTION OF
INFECTION PER SE CONSIDERED TO BE AN IMPORTANT GOAL OF VACCINATION. In
fact, asymptomatic infection after vaccination can serve to enhance and
prolong the immune response."
4. She was
diagnosed with vaccine induced ENCEPHALOPATHY (degenerative disease of the
brain)...as you will see below, mercury is involved in causing the degenerative
disease Alzheimer's, NOT autism).
5. She developed a SEIZURE
DISORDER later on (go to the CDC website at http://www.cdc.gov/vaccines/pubs/vis/downloads/vis-mmr.pdf)
and read the vaccine information statement on the MMR vaccine (which has never
had mercury), and you will see that one of the side effects is LONG TERM
SEIZURES.
6. You will also note that they did genetic testing of
the child and found that she has a genetic defect in her cellular energetics
(note that vaccines are known to cause GENETIC MUTATION due to insertion of
plasmids of DNA from the viruses or tissues used to culture them; in fact, this
is the whole basis on which DNA vaccines are designed). You can read how
DNA vaccines cause genetic mutations at http://sciamdigital.com/index.cfm?fa=Search.ViewSearchForItemResultList
(you will have to pay $7.95 to access this 1999 article from Scientific
American; put "genetic vaccines" in the search engine at that site to find the
article, and especially see p. 52 of the article). Of course, they are
purporting that this is a GOOD thing...and do not reveal that "regular" vaccines
can do the same thing. VACCINES ARE THE SOURCE OF MOST GENETIC MUTATIONS IN
PEOPLE AND IN PETS; and once these mutations have occurred, they are then passed
on to future generations. Thus, this insane practice has the potential of
causing the extinction of humanity itself.
7. You will
notice that although the white coat treating Hannah Poling went as far as to do
genetic testing in this child, there were NO ANTI-MYELIN OR ANTI-NEURONAL
FILAMENT LEVELS DONE; this IS the test that demonstrates demyelination before it
is massive enough to show up on MRI's; and this IS the test that would prove
that autism is actually a non-fatal form of subacute sclerosing panencephalitis
(which is why this test is almost never done). However, it is a known fact
that the measles virus has similar proteins to myelin basic protein, and thus
through molecular mimicry, the anti-measles antibody itself can cause
demyelination; and, as quoted from Harrison's above, this production of
anti-measles (and possibly anti-myelin and anti-neuronal filament antibodies
formed by injection of tissue culture on which the viruses are grown) is
prolonged because a chronic infection results.
Here
is the decision (but please be sure to also read what I have written after
it)...
IN THE UNITED STATES COURT OF FEDERAL
CLAIMS
OFFICE OF SPECIAL MASTERS
CHILD
[Hannah Poling], a minor,
by her Parents and Natural
Guardians [Dr. & Mrs. Jon Poling],
Petitioners,
v.
SECRETARY OF
HEALTH AND HUMAN SERVICES,
Respondent.
RESPONDENT'S RULE 4(c) REPORT
In accordance with RCFC,
Appendix B, Vaccine Rule 4(c), the Secretary of Health and Human Services
submits the following response to the petition for compensation filed in this
case.
FACTS
CHILD ("CHILD") was born on
December --, 1998, and weighed eight pounds, ten ounces. Petitioners' Exhibit
("Pet. Ex.") 54 at 13. The pregnancy was complicated by gestational diabetes.
From January 26, 1999 through June 28, 1999, CHILD
visited the
Vaccine Dates Administered
Hep
B 12/27/98; 1/26/99
IPV 3/12/99; 4/27/99
Hib 3/12/99; 4/27/99; 6/28/99
DTaP 3/12/99; 4/27/99;
6/28/99
At seven months
of age, CHILD was diagnosed with bilateral otitis media. Pet. Ex. 31 at 20. In
the subsequent months between July 1999 and January 2000, she had frequent bouts
of otitis media, which doctors treated with multiple antibiotics. Pet. Ex. 2 at
4. On December 3,1999, CHILD was seen by Karl Diehn, M.D., at Ear, Nose, and
Throat Associates of the Greater Baltimore Medical Center ("ENT Associates").
Pet. Ex. 31 at 44. Dr. Diehn recommend that CHILD receive PE tubes for her
"recurrent otitis media and serious otitis." Id. CHILD received PE tubes in
January 2000. Pet. Ex. 24 at 7. Due to CHILD's otitis media, her mother did not
allow CHILD to receive the standard 12 and 15 month childhood immunizations.
Pet. Ex. 2 at 4.
According to the medical records, CHILD
consistently met her developmental milestones during the first eighteen months
of her life. The record of an October 5, 1999 visit to the
At a July 19,
2000 pediatric visit, the pediatrician observed that CHILD "spoke well" and was
"alert and active." Pet. Ex. 31 at 11. CHILD's mother reported that CHILD had
regular bowel movements and slept through the night.
According to her mother's affidavit, CHILD developed a
fever of 102.3 degrees two days after her immunizations and was lethargic,
irritable, and cried for long periods of time. Pet. Ex. 2 at 6. She exhibited
intermittent, high-pitched screaming and a decreased response to stimuli. Id.
MOM spoke with the pediatrician, who told her that CHILD was having a normal
reaction to her immunizations.
On July 31, 2000,
CHILD presented to the
Two months later, on September 26, 2000, CHILD returned to the
CHILD was evaluated at
the Howard County Infants and Toddlers Program, on November 17, 2000, and
November 28, 2000, due to concerns about her language development. Pet. Ex. 19
at 2, 7. The assessment team observed deficits in CHILD's communication and
social development.
On December 21,
2000, CHILD returned to ENT Associates because of an obstruction in her right
ear and fussiness. Pet. Ex. 31 at 39. Dr. Grace Matesic identified a middle ear
effusion and recorded that CHILD was having some balance issues and not
progressing with her speech.
Dr. Andrew Zimmerman,
a pediatric neurologist, evaluated CHILD at the Kennedy Krieger Children's
Hospital Neurology Clinic ("Krieger Institute"), on February 8, 2001. Pet. Ex.
25 at 1. Dr. Zimmerman reported that after CHILD's immunizations of July 19,
2000, an "encephalopathy progressed to persistent loss of previously acquired
language, eye contact, and relatedness."
would not make eye contact.
Dr. Zimmerman referred
CHILD to the Krieger Institute's Occupational Therapy Clinic and the Center for
Autism and Related Disorders ("CARDS"). Pet. Ex. 25 at 40. She was evaluated at
the Occupational Therapy Clinic by Stacey Merenstein, OTR/L, on February 23,
2001.
CHILD returned
to Dr. Zimmerman, on May 17, 2001, for a follow-up consultation. Pet. Ex. 25 at
4. An overnight EEG, performed on April 6, 2001, showed no seizure discharges.
Dr. Zimmerman referred CHILD for a neurogenetics consultation to evaluate
her abnormal metabolic test results. Pet. Ex. 25 at 8. CHILD met with Dr.
Richard Kelley, a specialist in neurogenetics, on May 22, 2001, at the Krieger
Institute.
On October 4, 2001, Dr. John Schoffner, at Horizon Molecular Medicine in
nal myofiber with reduced cytochrome c
oxidase activity.
CHILD returned to the Krieger Institute, on July 7, 2004, for a follow-up
evaluation with Dr. Zimmerman. Pet. Ex. 57 at 9. He reported CHILD "had done
very well" with treatment for a mitochondrial dysfunction. Dr. Zimmerman
concluded that CHILD would continue to require services in speech, occupational,
physical, and behavioral therapy.
On April 14, 2006,
CHILD was brought by ambulance to
showed "rhythmic epileptiform discharges in the right
temporal region and then focal slowing during a witnessed clinical seizure."
ANALYSIS
Medical personnel at the Division of Vaccine
Injury Compensation, Department of Health and Human Services (DVIC) have
reviewed the facts of this case, as presented by the petition, medical records,
and affidavits. After a thorough review, DVIC has concluded that compensation is
appropriate in this case.
In sum, DVIC has concluded that
the facts of this case meet the statutory criteria for demonstrating that the
vaccinations CHILD received on July 19, 2000, significantly aggravated an
underlying mitochondrial disorder, which predisposed her to deficits in cellular
energy metabolism, and manifested as a regressive encephalopathy with features
of autism spectrum disorder. Therefore, respondent recommends that compensation
be awarded to petitioners in accordance with 42 U.S.C. §
300aa-11(c)(1)(C)(ii).
DVIC has concluded that CHILD's
complex partial seizure disorder, with an onset of almost six years after her
July 19, 2000 vaccinations, is not related to a vaccine-injury.
Respectfully submitted,
PETER D. KEISLER
Assistant Attorney General
TIMOTHY P. GARREN
Director
Torts Branch, Civil Division
MARK W. ROGERS
Deputy Director
Torts
Branch, Civil Division
VINCENT J. MATANOSKI
Assistant Director
Torts Branch, Civil
Division
s/ Linda S. Renzi by s/ Lynn E.
Ricciardella
LINDA S. RENZI
Senior Trial
Counsel
Torts Branch, Civil Division
U.S.
Department of Justice
P.O. Box 146
Benjamin
Franklin Station
Washington, D.C. 20044
(202)
616-4133
DATE: November 9, 2007
PS: On Friday,
February 22, HHS conceded that this child's complex partial seizure disorder was
also caused by her vaccines. Now we the taxpayers will award this family
compensation to finance her seizure medication. Surely ALL decent people can
agree that is a good thing.
By the way, it''s worth noting that her
seizures did not begin until six years after the date of vaccination, yet the
government acknowledges they were, indeed, linked to the immunizations of July,
2000, - David Kirby
Now I am going to prove to you, BEYOND A
SHADOW OF A DOUBT, that mercury is a distraction in the case of
autism:
Please go to http://healthtruthrevealed.com/audio-interviews.php, click on
"inoculations the true weapons of mass destruction", and listen to the interview
I did on this very subject on 3/4/08. You will hear interviewer Greg Ciola
mention research done at the
Now, go to http://www.youtube.com/watch?v=85tgwh3HpsM; this is CRITICAL.
You will hear and see the effect of mercury on brain neurons demonstrated
by the
I also encourage you to go to http://video.google.com/videoplay?docid=1803137818942286763,
and hear Dr Boyd Haley discuss autism & thimerosol (be sure to watch all 4
videos in this series). Dr Haley blames thimerosol for Gulf War Syndrome
(GWS) as well as autism. I have done many shows on GWS, which has many factors;
Gulf War PLAGUE (the infectious component of the SYNDROME) is due to mycoplasma
incognitas which was in the vaccines given to the soldiers. (In fact, this
pathogenic mycoplasma has actually been PATENTED by Dr. Shyn Ching Lo of the
American Registry of Pathology in
Dr. Haley brings up the work of Dr Andrew Wakefield,
whose medical license was attacked because he demonstrated measles virus in the
lymphoid patches in the guts of autistic children. DR. BOYD ADMITS HE DID
NOT EVEN STUDY THE MEASLES VIRUS. Although Dr Wakefield did not realize
that these viruses' significance as a chronic infection is that this leads to a
constant production of anti-measles antibody which, through molecular mimicry,
then attacks the myelin sheath (causing demyelination), Dr. Wakefield is being
persecuted because his work supports my work; especially since the MMR has NEVER
HAD MERCURY. Dr. Haley's work reinforces the notion that if you take
mercury out of vaccines, they will be safe. My work proves there is NO
SUCH THING as a safe vaccine, due to the corruption of the immune system caused
by injection of live viruses.
Dr. Haley also discusses how antibiotics
further accelerate the damage in these children. The question he does
not address is why are the vaccinated children on antibiotics?
Answer...because they have chronic infection caused by inoculation of live
bacteria & viruses; as quoted from Harrison's principles of medicine in my
response to the CDC (also on my website), "RARELY IS PREVENTION OF INFECTION PER
SE CONSIDERED TO BE AN IMPORTANT GOAL OF VACCINATION. In fact,
asymptomatic infection after vaccination can serve to enhance and prolong the
immune response". (And this prolonged immune response IS prolonged
production of anti-measles antibody which then continue to attack the myelin
sheath, causing demyelination). I also quote from
Dr. Haley also discusses how mercury
is more toxic in children with immune disorders. Where did these immune
disorders come from? From the corruption of the immune system caused by
the inoculation of live viruses. He also discusses that mercury can cause
toxicity which affects genetics by decreased methylation of DNA & RNA.
However, no mention is made of the genetic mutations caused by injection
of plasmids of DNA from the organisms themselves and the tissues that the
viruses are cultured on, which is the whole basis of DNA vaccines. That is
why this court case focuses on the fact that the child had a genetic defect
which caused mitochondrial dysfunction, and states that the child has "a
regressive encephalopathy with features of autism spectrum disorder".
Where this mitochondrial defect originated is not discussed...injection of
foreign DNA in prior vaccines in either Hannah or one of her parents, if this
defect was inherited. (However, if one of Hannah's parents has this
mitochondrial defect, then why don't they have autism?)
Lastly, Dr. Haley
also states that oral vaccines would be safer, but does not say this is because
of the secretory IgA causing proper handling of the germ and its subsequent
elimination from the body (as also explained in my inoculation paper), leading
to life long NATURAL immunity. Of course, if all vaccines were made into
oral forms, people may then ask the hard question...SO WHY ISN'T NATURAL
EXPOSURE TO THESE VIRUSES THE BEST WAY TO GO? This question would stop
vaccine production altogether, which would stop the creation of all autoimmune
diseases and cancer, which would shut down Big Pharma. THAT IS THE
POTENTIAL OF MY INFORMATION; which is why the medical mafia has gone as far as
taking my only child, not just my medical license as they tried with Dr.
Wakefield in an attempt to shut me down.
I also sent this document to Dr. Paul Offit at offit@email.chop.edu. Dr. Offit has a huge conflict of interest in promoting vaccines, as he developed the rotavirus vaccine which had to be taken off the market as it sent so many children into the operating room with the life threatening condition called intussussception, where the bowel telescopes in on itself. This is what I stated to Dr. Offit: “I am anxious to hear you present your evidence that autism is not a non fatal form of subacute sclerosing panencephalitis, since the only evidence you presented in your recent book Vaccinated praising Maurice Hilleman was that SSPE is always fatal.” No response from Dr. Offit, who has also publicly made the insane statement that “children can handle 10,000 vaccines at one time.”
If you want to learn how the post encephalitic syndrome caused by vaccines causes changes in the brain that lead to violence and criminal behavior, please go to http://www.thinktwice.com/ and order the highly referenced book Vaccinations, Social Violence and Criminality by Harris Coulter, PhD. Do you now see how vaccines contribute to the ever increasing violence being seen in our young people; not to mention how many children are subsequently put on psychiatric drugs after sustaining neurological vaccine damage leading to ADD, ADHD, etc. As Big Pharma has even started to admit, these drugs have a side effect of homicide and suicide.
Are you beginning to realize how important it is to stop this
insane practice of inoculating our children with disease, and instead give them
natural supplements to boost their natural immunity?
Can you handle knowing the fact
that all this is being done to the children ON PURPOSE? Then go to http://www.republicbroadcasting.org/index.php?cmd=archives.month&ProgramID=36&year=8&month=3&backURL=index.php%253Fcmd%253Darchives.getyear%2526ProgramID%253D36%26year%3D8%26backURL%3Dindex.php%253Fcmd%253Darchives
and
listen to the 2nd hour of my interview on 3/5/08 with Dr. True Ott, where he
discusses how the history of MediSIN goes back to the 1600's as detailed in the
Magnum Opus by Jesuit Del Rio, with the creation of amulets by sacrificing
animals and mixing their blood with mercurial compounds TO CAST A SPELL AND
CONTROL THE MINDS OF THE POPULATIONS (Dr Ott discusses this starting at 13
minutes of the 2nd hour of our interview). He explains how the origins of the
word "pharmaceutical" in Latin is "pharmakia", which translates to "SORCERY".
Yes, folks...you have now entered the rabbit hole...because nothing has
changed since the 1600's.
I have been trying for 10 years to stop the
vaccination holocaust on people and pets. I have proven, with the quoted
studies and works of the "mercury causes autism" disinformers themselves, that
it is NOT MERCURY WHICH CAUSES AUTISM. I leave it up to you to
forward this e-mail to all the individuals and groups which promote mercury as
the cause of autism, so you will see for YOURSELVES who is intentionally
misleading you, vs. who was misguided. You will know which is the case by
whether or not they respond. SILENCE IS CONSENT that I am right; and if
they do not join with me to stop this holocaust altogether, you must then ask
yourself WHY. IT IS TIME FOR THOSE WITH HONORABLE INTENTIONS TO JOIN WITH
ME TO STOP THIS EPIDEMIC OF VIDS. I have already sent this document to Dr. Boyd
Haley (behaley@uky.edu) and
David Kirby (brook200@hotmail.com); please do so yourselves.
Let's
roll....
Namaste,
Dr Carley