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MYCOPLASMA
The Linking Pathogen in Neurosystemic Diseases
Several strains of mycoplasma have been "engineered" to become more
dangerous. They are now being blamed for AIDS, cancer, CFS, MS, CJD and other
neurosystemic diseases.
Extracted from Nexus Magazine, Volume 8, Number 5 (August-September
2001)
PO Box 30, Mapleton Qld 4560 Australia. editor@nexusmagazine.com
Telephone: +61 (0)7 5442 9280; Fax: +61 (0)7 5442 9381
From our web page at: www.nexusmagazine.com
© by Donald W. Scott, MA, MSc © 2001
President
The Common Cause
Medical Research Foundation
190 Mountain Street, Suite 405
Sudbury, Ontario, Canada P3B 4G2
Tel/fax: +1 (705) 670 0180
PATHOGENIC MYCOPLASMA
A Common Disease Agent Weaponised
There are 200 species of Mycoplasma. Most are innocuous and do no harm;
only four or five are pathogenic. Mycoplasma fermentans (incognitus strain) probably comes
from the nucleus of the Brucella
bacterium. This disease agent is not a bacterium and not a virus; it is
a mutated form of the Brucella
bacterium, combined with a visna virus, from which the mycoplasma is
extracted.
The pathogenic Mycoplasma used to be very innocuous, but biological
warfare research conducted
between 1942 and the present time has resulted in the creation of more
deadly and infectious forms of
Mycoplasma. Researchers extracted this mycoplasma from the Brucella
bacterium and actually reduced
the disease to a crystalline form. They "weaponised" it and tested it on
an unsuspecting public in North
America.
Dr Maurice Hilleman, chief virologist for the pharmaceutical company
Merck Sharp & Dohme, stated that
this disease agent is now carried by everybody in North America and
possibly most people throughout the
world.
Despite reporting flaws, there has clearly been an increased incidence
of all the neuro/systemic
degenerative diseases since World War II and especially since the 1970s
with the arrival of previously
unheard-of diseases like chronic fatigue syndrome and AIDS.
According to Dr Shyh-Ching Lo, senior researcher at The Armed Forces
Institute of Pathology and one of
America's top mycoplasma researchers, this disease agent causes many
illnesses including AIDS, cancer,
chronic fatigue syndrome, Crohn's colitis, Type I diabetes, multiple
sclerosis, Parkinson's disease,
Wegener's disease and collagen-vascular diseases such as rheumatoid
arthritis and Alzheimer's.
Dr Charles Engel, who is with the US National Institutes of Health,
Bethesda, Maryland, stated the
following at an NIH meeting on February 7, 2000: "I am now of the view that the probable cause of chronic fatigue syndrome and fibromyalgia is the mycoplasma..."
I have all the official documents to prove that mycoplasma is the
disease agent in chronic fatigue
syndrome/fibromyalgia as well as in AIDS, multiple sclerosis and many
other illnesses. Of these, 80% are
US or Canadian official government documents, and 20% are articles from
peer-reviewed journals such
as the Journal of the American Medical Association, New England Journal
of Medicine and the
Canadian Medical Association Journal. The journal articles and
government documents complement
each other.
How the Mycoplasma Works
The mycoplasma acts by entering into the individual cells of the body,
depending upon your genetic
predisposition.
You may develop neurological diseases if the pathogen destroys certain
cells in your brain, or you may
develop Crohn's colitis if the pathogen invades and destroys cells in
the lower bowel.
Once the mycoplasma gets into the cell, it can lie there doing nothing
sometimes for 10, 20 or 30 years,
but if a trauma occurs like an accident or a vaccination that doesn't
take, the mycoplasma can become
triggered.
Because it is only the DNA particle of the bacterium, it doesn't have
any organelles to process its own
nutrients, so it grows by uptaking pre-formed sterols from its host cell
and it literally kills the cell; the cell
ruptures and what is left gets dumped into the bloodstream.
II – CREATION OF THE MYCOPLASMA
A Laboratory-Made Disease Agent
Many doctors don't know about this mycoplasma disease agent because it
was developed by the US
military in biological warfare experimentation and it was not made
public. This pathogen was patented by
the United States military and Dr Shyh-Ching Lo. I have a copy of the
documented patent from the US
Patent Office.1
All the countries at war were experimenting with biological weapons. In
1942, the governments of the
United States, Canada and Britain entered into a secret agreement to
create two types of biological
weapons (one that would kill, and one that was disabling) for use in the
war against Germany and Japan,
who were also developing biological weapons. While they researched a
number of disease pathogens, they
primarily focused on the Brucella bacterium and began to weaponise it.
From its inception, the biowarfare program was characterised by
continuing in-depth review and
participation by the most eminent scientists, medical consultants,
industrial experts and government
officials, and it was classified Top Secret.
The US Public Health Service also closely followed the progress of
biological warfare research and
development from the very start of the program, and the Centers for
Disease Control (CDC) and the
National Institutes of Health (NIH) in the United States were working
with the military in weaponising
these diseases. These are diseases that have existed for thousands of
years, but they have been
weaponised--which means they've been made more contagious and more
effective. And they are
spreading.
The Special Virus Cancer Program, created by the CIA and NIH to develop
a deadly pathogen for which
humanity had no natural immunity (AIDS), was disguised as a war on
cancer but was actually part of
MKNAOMI.2 Many members of the Senate and House of Representatives do not
know what has been
going on. For example, the US Senate Committee on Government Reform had
searched the archives in
Washington and other places for the document titled "The Special Virus
Cancer Program: Progress Report
No. 8", and couldn't find it. Somehow they heard I had it, called me and
asked me to mail it to them.
Imagine: a retired schoolteacher being called by the United States
Senate and asked for one of their secret
documents! The US Senate, through the Government Reform Committee, is
trying to stop this type of
government research.
Crystalline Brucella
The title page of a genuine US Senate Study, declassified on February
24, 1977, shows that George
Merck, of the pharmaceutical company, Merck Sharp & Dohme (which now
makes cures for diseases
that at one time it created), reported in 1946 to the US Secretary of
War that his researchers had managed
"for the first time" to "isolate the disease agent in crystalline
form".3
They had produced a crystalline bacterial toxin extracted from the
Brucella bacterium. The bacterial toxin
could be removed in crystalline form and stored, transported and
deployed without deteriorating. It could
be delivered by other vectors such as insects, aerosol or the food chain
(in nature it is delivered within the
bacterium). But the factor that is working in the Brucella is the
mycoplasma.
Brucella is a disease agent that doesn't kill people; it disables them.
But, according to Dr Donald
MacArthur of the Pentagon, appearing before a congressional committee in
1969,4 researchers found that
if they had mycoplasma at a certain strength--actually, 10 to the 10th
power (1010)--it would develop into
AIDS, and the person would die from it within a reasonable period of
time because it could bypass the
natural human defences. If the strength was 108, the person would
manifest with chronic fatigue
syndrome or fibromyalgia. If it was 107, they would present as wasting;
they wouldn't die and they
wouldn't be disabled, but they would not be very interested in life;
they would waste away.
Most of us have never heard of the disease brucellosis because it
largely disappeared when they began
pasteurising milk, which was the carrier. One salt shaker of the pure
disease agent in a crystalline form
could sicken the entire population of Canada. It is absolutely deadly,
not so much in terms of killing the
body but disabling it.
Because the crystalline disease agent goes into solution in the blood,
ordinary blood and tissue tests will
not reveal its presence. The mycoplasma will only crystallise at 8.1 pH,
and the blood has a pH of 7.4
pH. So the doctor thinks your complaint is "all in your head".
Crystalline Brucella and Multiple Sclerosis
In 1998 in Rochester, New York, I met a former military man, PFC Donald
Bentley, who gave me a
document and told me: "I was in the US Army, and I was trained in
bacteriological warfare. We were
handling a bomb filled with brucellosis, only it wasn't brucellosis; it
was a Brucella toxin in crystalline
form. We were spraying it on the Chinese and North Koreans."
He showed me his certificate listing his training in chemical,
biological and radiological warfare. Then he
showed me 16 pages of documents given to him by the US military when he
was discharged from the
service. They linked brucellosis with multiple sclerosis, and stated in
one section: "Veterans with multiple
sclerosis, a kind of creeping paralysis developing to a degree of 10% or
more disability within two years
after separation from active service, may be presumed to be
service-connected for disability
compensation. Compensation is payable to eligible veterans whose
disabilities are due to service." In other
words: "If you become ill with multiple sclerosis, it is because you
were handling this Brucella, and we
will give you a pension. Don't go raising any fuss about it." In these
documents, the government of the
United States revealed evidence of the cause of multiple sclerosis, but
they didn't make it known to the
public--or to your doctor.
In a 1949 report, Drs Kyger and Haden suggested "the possibility that
multiple sclerosis might be a central
nervous system manifestation of chronic brucellosis". Testing
approximately 113 MS patients, they found
that almost 95% also tested positive for Brucella.5 We have a document
from a medical journal, which
concludes that one out of 500 people who had brucellosis would develop
what they call neurobrucellosis;
in other words, brucellosis in the brain, where the Brucella settles in
the lateral ventricles--where the
disease multiple sclerosis is basically located.6
Contamination of Camp Detrick Lab Workers
A 1948 New England Journal of Medicine report titled "Acute Brucellosis
Among Laboratory Workers"
shows us how actively dangerous this agent is.7 The laboratory workers
were from Camp Detrick,
Frederick, Maryland, where they were developing biological weapons. Even
though these workers had
been vaccinated, wore rubberised suits and masks and worked through
holes in the compartment, many
of them came down with this awful disease because it is so absolutely
and terrifyingly infectious.
The article was written by Lt Calderone Howell, Marine Corps, Captain
Edward Miller, Marine Corps, Lt
Emily Kelly, United States Naval Reserve, and Captain Henry Bookman.
They were all military personnel
engaged in making the disease agent Brucella into a more effective
biological weapon.
III – COVERT TESTING OF MYCOPLASMA
Testing the Dispersal Methods
Documented evidence proves that the biological weapons they were
developing were tested on the public
in various communities without their knowledge or consent.
The government knew that crystalline Brucella would cause disease in
humans. Now they needed to
determine how it would spread and the best way to disperse it. They
tested dispersal methods for
Brucella suis and Brucella melitensis at Dugway Proving Ground, Utah, in
June and September 1952.
Probably, 100% of us now are infected with Brucella suis and Brucella
melitensis.8
Another government document recommended the genesis of open-air
vulnerability tests and covert
research and development programs to be conducted by the Army and
supported by the Central
Intelligence Agency.
At that time, the Government of Canada was asked by the US Government to
cooperate in testing
weaponised Brucella, and Canada cooperated fully with the United States.
The US Government wanted
to determine whether mosquitoes would carry the disease and also if the
air would carry it. A government
report stated that "open-air testing of infectious biological agents is
considered essential to an ultimate
understanding of biological warfare potentialities because of the many
unknown factors affecting the
degradation of micro-organisms in the atmosphere".9
Testing via Mosquito Vector in Punta Gorda, Florida
A report from The New England Journal of Medicine reveals that one of
the first outbreaks of chronic
fatigue syndrome was in Punta Gorda, Florida, back in 1957.10 It was a
strange coincidence that a week
before these people came down with chronic fatigue syndrome, there was a
huge influx of mosquitoes.
The National Institutes of Health claimed that the mosquitoes came from
a forest fire 30 miles away. The
truth is that those mosquitoes were infected in Canada by Dr Guilford B.
Reed at Queen's University.
They were bred in Belleville, Ontario, and taken down to Punta Gorda and
released there.
Within a week, the first five cases ever of chronic fatigue syndrome
were reported to the local clinic in
Punta Gorda. The cases kept coming until finally 450 people were ill
with the disease.
Testing via Mosquito Vector in Ontario
The Government of Canada had established the Dominion Parasite
Laboratory in Belleville, Ontario,
where it raised 100 million mosquitoes a month. These were shipped to
Queen's University and certain
other facilities to be infected with this crystalline disease agent. The
mosquitoes were then let loose in
certain communities in the middle of the night, so that the researchers
could determine how many people
would become ill with chronic fatigue syndrome or fibromyalgia, which
was the first disease to show.
One of the communities they tested it on was the St Lawrence Seaway
valley, all the way from Kingston
to Cornwall, in 1984. They let out hundreds of millions of infected
mosquitoes. Over 700 people in the
next four or five weeks developed myalgic encephalomyelitis, or chronic
fatigue syndrome.
IV – COVERT TESTING OF OTHER DISEASE AGENTS
Mad Cow Disease/Kuru/CJD in the Fore Tribe
Before and during World War II, at the infamous Camp 731 in Manchuria,
the Japanese military
contaminated prisoners of war with certain disease agents.
They also established a research camp in New Guinea in 1942. There they
experimented upon the Fore
Indian tribe and inoculated them with a minced-up version of the brains
of diseased sheep containing the
visna virus which causes "mad cow disease" or Creutzfeldt&endash;Jakob
disease.
About five or six years later, after the Japanese had been driven out,
the poor people of the Fore tribe
developed what they called kuru, which was their word for "wasting", and
they began to shake, lose their
appetites and die. The autopsies revealed that their brains had
literally turned to mush. They had
contracted "mad cow disease" from the Japanese experiments.
When World War II ended, Dr Ishii Shiro--the medical doctor who was
commissioned as a General in the
Japanese Army so he could take command of Japan's biological warfare
development, testing and
deployment--was captured. He was given the choice of a job with the
United States Army or execution as
a war criminal. Not surprisingly, Dr Ishii Shiro chose to work with the
US military to demonstrate how
the Japanese had created mad cow disease in the Fore Indian tribe.
In 1957, when the disease was beginning to blossom in full among the
Fore people, Dr Carleton Gajdusek
of the US National Institutes of Health headed to New Guinea to
determine how the minced-up brains of
the visna-infected sheep affected them. He spent a couple of years
there, studying the Fore people, and
wrote an extensive report. He won the Nobel Prize for "discovering" kuru
disease in the Fore tribe.
Testing Carcinogens over Winnipeg, Manitoba
In 1953, the US Government asked the Canadian Government if it could
test a chemical over the city of
Winnipeg. It was a big city with 500,000 people, miles from anywhere.
The American military sprayed
this carcinogenic chemical in a 1,000%-attenuated form, which they said
would be so watered down that
nobody would get very sick; however, if people came to clinics with a
sniffle, a sore throat or ringing in
their ears, the researchers would be able to determine what percentage
would have developed cancer if
the chemical had been used at full strength.
We located evidence that the Americans had indeed tested this
carcinogenic chemical--zinc cadmium
sulphide--over Winnipeg in 1953. We wrote to the Government of Canada,
explaining that we had solid
evidence of the spraying and asking that we be informed as to how high
up in the government the request
for permission to spray had gone. We did not receive a reply.
Shortly after, the Pentagon held a press conference on May 14, 1997,
where they admitted what they had
done. Robert Russo, writing for the Toronto Star11 from Washington, DC,
reported the Pentagon's
admission that in 1953 it had obtained permission from the Canadian
Government to fly over the city of
Winnipeg and spray out this chemical--which sifted down on kids going to
school, housewives hanging out
their laundry and people going to work. US Army planes and trucks
released the chemical 36 times
between July and August 1953. The Pentagon got its statistics, which
indicated that if the chemical
released had been full strength, approximately a third of the population
of Winnipeg would have
developed cancers over the next five years.
One professor, Dr Hugh Fudenberg, MD, twice nominated for the Nobel
Prize, wrote a magazine article
stating that the Pentagon came clean on this because two researchers in
Sudbury, Ontario--Don Scott and
his son, Bill Scott--had been revealing this to the public. However, the
legwork was done by other
researchers!
The US Army actually conducted a series of simulated germ warfare tests
over Winnipeg. The Pentagon
lied about the tests to the mayor, saying that they were testing a
chemical fog over the city, which would
protect Winnipeg in the event of a nuclear attack.
A report commissioned by US Congress, chaired by Dr Rogene Henderson,
lists 32 American towns and
cities used as test sites as well.
V – BRUCELLA MYCOPLASMA AND DISEASE
AIDS
The AIDS pathogen was created out of a Brucella bacterium mutated with a
visna virus; then the toxin
was removed as a DNA particle called a mycoplasma. They used the same
mycoplasma to develop
disabling diseases like MS, Crohn's colitis, Lyme disease, etc.
In the previously mentioned US congressional document of a meeting held
on June 9, 1969,12 the
Pentagon delivered a report to Congress about biological weapons. The
Pentagon stated: "We are
continuing to develop disabling weapons." Dr MacArthur, who was in
charge of the research, said: "We
are developing a new lethal weapon, a synthetic biological agent that
does not naturally exist, and for
which no natural immunity could have been acquired."
Think about it. If you have a deficiency of acquired immunity, you have
an acquired immunity
deficiency. Plain as that. AIDS.
In laboratories throughout the United States and in a certain number in
Canada including at the University
of Alberta, the US Government provided the leadership for the
development of AIDS for the purpose of
population control. After the scientists had perfected it, the
government sent medical teams from the
Centers for Disease Control--under the direction of Dr Donald A.
Henderson, their investigator into the
1957 chronic fatigue epidemic in Punta Gorda--during 1969 to 1971 to
Africa and some countries such as
India, Nepal and Pakistan where they thought the population was becoming
too large.13 They gave them
all a free vaccination against smallpox; but five years after receiving
this vaccination, 60% of those
inoculated were suffering from AIDS. They tried to blame it on a monkey,
which is nonsense.
A professor at the University of Arkansas made the claim that while
studying the tissues of a dead
chimpanzee she found traces of HIV. The chimpanzee that she had tested
was born in the United States
23 years earlier. It had lived its entire life in a US military
laboratory where it was used as an experimental
animal in the development of these diseases. When it died, its body was
shipped to a storage place where
it was deep-frozen and stored in case they wanted to analyse it later.
Then they decided that they didn't
have enough space for it, so they said, "Anybody want this dead
chimpanzee?" and this researcher from
Arkansas said: "Yes. Send it down to the University of Arkansas. We are
happy to get anything that we
can get." They shipped it down and she found HIV in it. That virus was
acquired by that chimpanzee in
the laboratories where it was tested.14
Chronic Fatigue Syndrome/ Myalgic Encephalomyelitis
Chronic fatigue syndrome is more accurately called myalgic
encephalomyelitis. The chronic fatigue
syndrome nomenclature was given by the US National Institutes of Health
because it wanted to
downgrade and belittle the disease.
An MRI scan of the brain of a teenage girl with chronic fatigue syndrome
displayed a great many scars or
punctate lesions in the left frontal lobe area where portions of the
brain had literally dissolved and been
replaced by scar tissue. This caused cognitive impairment, memory
impairment, etc. And what was the
cause of the scarring? The mycoplasma. So there is very concrete
physical evidence of these tragic
diseases, even though doctors continue to say they don't know where it
comes from or what they can do
about it.
Many people with chronic fatigue syndrome, myalgic encephalo-myelitis
and fibromyalgia who apply to
the Canada Pensions Plan Review Tribunal will be turned down because
they cannot prove that they are
ill. During 1999 I conducted several appeals to Canada Pensions and the
Workers Compensation Board
(WCB, now the Workplace Safety and Insurance Board) on behalf of people
who have been turned
down. I provided documented evidence of these illnesses, and these
people were all granted their pensions
on the basis of the evidence that I provided.
In March 1999, for example, I appealed to the WCB on behalf of a lady
with fibromyalgia who had been
denied her pension back in 1993. The vice-chairman of the board came to
Sudbury to hear the appeal,
and I showed him a number of documents which proved that this lady was
physically ill with
fibromyalgia. It was a disease that caused physical damage, and the
disease agent was a mycoplasma. The
guy listened for three hours, and then he said to me: "Mr Scott, how is
it I have never heard of any of this
before? I said: "We brought a top authority in this area into Sudbury to
speak on this subject and not a
single solitary doctor came to that presentation."
VI – TESTING FOR MYCOPLASMA IN YOUR BODY
Polymerase Chain Reaction Test
Information is not generally available about this agent because, first
of all, the mycoplasma is such a
minutely small disease agent. A hundred years ago, certain medical
theoreticians conceived that there
must be a form of disease agent smaller than bacteria and viruses. This
pathogenic organism, the
mycoplasma, is so minute that normal blood and tissue tests will not
reveal its presence as the source of
the disease.
Your doctor may diagnose you with Alzheimer's disease, and he will say:
"Golly, we don't know where
Alzheimer's comes from. All we know is that your brain begins to
deteriorate, cells rupture, the myelin
sheath around the nerves dissolves, and so on." Or if you have chronic
fatigue syndrome, the doctor will
not be able to find any cause for your illness with ordinary blood and
tissue tests.
This mycoplasma couldn't be detected until about 30 years ago when the
polymerase chain reaction
(PCR) test was developed, in which a sample of your blood is examined
and damaged particles are
removed and subjected to a polymerase chain reaction. This causes the
DNA in the particles to break
down. The particles are then placed in a nutrient, which causes the DNA
to grow back into its original
form. If enough of the substance is produced, the form can be
recognised, so it can be determined
whether Brucella or another kind of agent is behind that particular
mycoplasma.
Blood Test
If you or anybody in your family has myalgic encephalomyelitis,
fibromyalgia, multiple sclerosis or
Alzheimer's, you can send a blood sample to Dr Les Simpson in New
Zealand for testing.
If you are ill with these diseases, your red blood cells will not be
normal doughnut-shaped blood cells
capable of being compressed and squeezed through the capillaries, but
will swell up like cherry-filled
doughnuts which cannot be compressed. The blood cells become enlarged
and distended because the only
way the mycoplasma can exist is by uptaking pre-formed sterols from the
host cell. One of the best
sources of pre-formed sterols is cholesterol, and cholesterol is what
gives your blood cells flexibility. If the
cholesterol is taken out by the mycoplasma, the red blood cell swells up
and doesn't go through, and the
person begins to feel all the aches and pains and all the damage it
causes to the brain, the heart, the
stomach, the feet and the whole body because blood and oxygen are cut
off.
And that is why people with fibromyalgia and chronic fatigue syndrome
have such a terrible time. When
the blood is cut off from the brain, punctate lesions appear because
those parts of the brain die. The
mycoplasma will get into portions of the heart muscle, especially the
left ventricle, and those cells will die.
Certain people have cells in the lateral ventricles of the brain that
have a genetic predisposition to admit
the mycoplasma, and this causes the lateral ventricles to deteriorate
and die. This leads to multiple
sclerosis, which will progress until these people are totally disabled;
frequently, they die prematurely. The
mycoplasma will get into the lower bowel, parts of which will die, thus
causing colitis. All of these
diseases are caused by the degenerating properties of the mycoplasma.
In early 2000, a gentleman in Sudbury phoned me and told me he had
fibromyalgia. He applied for a
pension and was turned down because his doctor said it was all in his
head and there was no external
evidence. I gave him the proper form and a vial, and he sent his blood
to Dr Simpson to be tested. He did
this with his family doctor's approval, and the results from Dr Simpson
showed that only 4% of his red
blood cells were functioning normally and carrying the appropriate
amount of oxygen to his poor body,
whereas 83% were distended, enlarged and hardened, and wouldn't go
through the capillaries without an
awful lot of pressure and trouble. This is the physical evidence of the
damage that is done.
ECG Test
You can also ask your doctor to give you a 24-hour Holter ECG. You know,
of course, that an
electrocardiogram is a measure of your heartbeat and shows what is going
on in the right ventricle, the left
ventricle and so on. Tests show that 100% of patients with chronic
fatigue syndrome and fibromyalgia
have an irregular heartbeat. At various periods during the 24 hours, the
heart, instead of working happily
away going "bump-BUMP, bump-BUMP", every now and again goes
"buhbuhbuhbuhbuhbuhbuhbuhbuh". The T-wave (the waves are called P, Q, R,
S and T) is normally a
peak, and then the wave levels off and starts with the P-wave again. In
chronic fatigue and fibromyalgia
patients, the T-wave flattens off, or actually inverts. That means the
blood in the left ventricle is not being
squeezed up through the aorta and around through the body.
My client from Sudbury had this test done and, lo and behold, the
results stated: "The shape of T and
S-T suggests left ventricle strain pattern, although voltage and so on
is normal." The doctor had no clue as
to why the T-wave was not working properly. I analysed the report of
this patient who had been turned
down by Canada Pensions and sent it back to them. They wrote back,
saying: "It looks like we may have
made a mistake. We are going to give you a hearing and you can explain
this to us in more detail."
So it is not all in your imagination. There is actual physical damage to
the heart. The left ventricle muscles
do show scarring. That is why many people are diagnosed with a heart
condition when they first develop
fibromyalgia, but it's only one of several problems because the
mycoplasma can do all kinds of damage.
Blood Volume Test
You can also ask your doctor for a blood volume test. Every human being
requires a certain amount of
blood per pound of body weight, and it has been observed that people
with fibromyalgia, chronic fatigue
syndrome, multiple sclerosis and other illnesses do not have the normal
blood volume their body needs to
function properly. Doctors aren't normally aware of this.
This test measures the amount of blood in the human body by taking out 5
cc, putting a tracer in it and
then putting it back into the body. One hour later, take out 5 cc again
and look for the tracer. The thicker
the blood and the lower the blood volume, the more tracer you will find.
The analysis of one of my clients stated: "This patient was referred for
red cell mass study. The red cell
volume is 16.9 ml per kg of body weight. The normal range is 25 to 35 ml
per kg. This guy has 36% less
blood in his body than the body needs to function." And the doctor
hadn't even known the test existed.
If you lost 36% of your blood in an accident, do you think your doctor
would tell you that you are alright
and should just take up line dancing and get over it? They would rush
you to the nearest hospital and start
transfusing you with blood. These tragic people with these awful
diseases are functioning with anywhere
from 7% to 50% less blood than their body needs to function.
VII – UNDOING THE DAMAGE
The body undoes the damage itself. The scarring in the brain of people
with chronic fatigue and
fibromyalgia will be repaired. There is cellular repair going on all the
time. But the mycoplasma has
moved on to the next cell.
In the early stages of a disease, doxycycline may reverse that disease
process. It is one of the tetracycline
antibiotics, but it is not bactericidal; it is bacteriostatic--it stops
the growth of the mycoplasma. And if the
mycoplasma growth can be stopped for long enough, then the immune system
takes over.
Doxycycline treatment is discussed in a paper by mycoplasma expert
Professor Garth Nicholson, PhD, of
the Institute for Molecular Medicine.15 Dr Nicholson is involved in a
US$8-million mycoplasma research
program funded by the US military and headed by Dr Charles Engel of the
NIH. The program is studying
Gulf War veterans, 450 of them, because there is evidence to suggest
that Gulf War syndrome is another
illness (or set of illnesses) caused by mycoplasma.
Endnotes:
1. "Pathogenic Mycoplasma", US Patent No. 5,242,820, issued September 7,
1993. Dr Lo is listed as the
"Inventor" and the American Registry of Pathology, Washington, DC, is
listed as the "Assignee".
2. "Special Virus Cancer Program: Progress Report No. 8", prepared by
the National Cancer Institute,
Viral Oncology, Etiology Area, July 1971, submitted to NIH Annual Report
in May 1971 and updated
July 1971.
3. US Senate, Ninety-fifth Congress, Hearings before the Subcommittee on
Health and Scientific
Research of the Committee on Human Resources, Biological Testing
Involving Human Subjects by the
Department of Defense, 1977; released as US Army Activities in the US
Biological Warfare Programs,
Volumes One and Two, 24 February 1977.
4. Dr Donald MacArthur, Pentagon, Department of Defense Appropriations
for 1970, Hearings before
Subcommittee of the Committee on Appropriations, House of
Representatives, Ninety-First Congress,
First Session, Monday June 9, 1969, pp 105&endash;144, esp. pp. 114,
129.
5. Kyger, E. R. and Russell L. Haden, "Brucellosis and Multiple
Sclerosis", The American Journal of
Medical Sciences 1949:689-693.
6. Colmonero et al., "Complications Associated with Brucella melitensis
Infection: A Study of 530 Cases",
Medicine 1996;75(4).
7. Howell, Miller, Kelly and Bookman, "Acute Brucellosis Among
Laboratory Workers", New England
Journal of Medicine 1948;236:741.
8. "Special Virus Cancer Program: Progress Report No. 8", ibid., table
4, p. 135.
9. US Senate, Hearings before the Subcommittee on Health and Scientific
Research of the Committee on
Human Resources, March 8 and May 23, 1977, ibid.
10. New England Journal of Medicine, August 22, 1957, p. 362.
11. Toronto Star, May 15, 1997.
12. Dr Donald MacArthur, Pentagon, Department of Defense Appropriations
for 1970, Hearings,
Monday June 9, 1969, ibid., p. 129.
13. Henderson, Donald A., "Smallpox: Epitaph for a Killer", National
Geographic, December 1978, p.
804.
14. Blum, Deborah, The Monkey Wars, Oxford University Press, New York,
1994.
15. Nicholson, G. L., "Doxycycline treatment and Desert Storm", JAMA
1995;273:618-619.
Recommended Reading:
¥ Horowitz, Leonard, Emerging Viruses: Aids and Ebola, Tetrahedron
Publishing, USA, 1996.
¥ Johnson, Hillary, Osler's Web, Crown Publishers, New York, 1996.
¥ Scott, Donald W. and William L. C. Scott, The Brucellosis Triangle,
The Chelmsford Publishers (Box
133, Stat. B., Sudbury, Ontario P3E 4N5), Canada, 1998 (US$21.95 + $3
s&h in US).
¥ Scott, Donald W. and William L. C. Scott, The Extremely Unfortunate
Skull Valley Incident, The
Chelmsford Publishers, Canada, 1996 (revised, extended edition available
from mid-September 2001;
US$16.00 pre-pub. price + US$3 s&h in US).
¥ The Journal of Degenerative Diseases (Donald W. Scott, Editor), The
Common Cause Medical
Research Foundation (Box 133, Stat B., Sudbury, Ontario, P3E 4N5),
Canada (quarterly journal; annual
subscription: US$25.00 in USA, $30 foreign).
Additional Contacts:
¥ Ms Jennie Burke, Australian Biologics, Level 6, 383 Pitt Street,
Sydney NSW 2000, Australia tel +61
(0)2 9283 0807, fax +61 (0)2 9283 0910. Australian Biologics does tests
for mycoplasma.
¥ Consumer Health Organization of Canada, 1220 Sheppard Avenue East
#412, Toronto, Ontario,
Canada M2K 2S5, tel +1 (416) 490 0986, website www.consumerhealth.org/.
¥ Professor Garth Nicholson, PhD, Institute for Molecular Medicine,
15162 Triton Lane, Huntington
Beach, CA, 92649-1401, USA, tel +1 (714) 903 2900.
¥ Dr Les Simpson, Red Blood Cell Research Ltd, 31 Bath Street, Dunedin,
9001, New Zealand, tel +64
(0)3 471 8540, email rbc.research.limited@xtra.co.nz. (Note: Dr Simpson
directs his study to red cell
shape analysis, not the mycoplasma hypothesis.)
¥ The Mycoplasma Registry for Gulf War Illness, S. & L. Dudley, 303 47th
St, J-10 San Diego, CA
92102-5961, tel/fax +1 (619) 266 1116, fax (619) 266 1116, email
mycoreg@juno.com.
About the Author:
Donald Scott, MA, MSc, is a retired high school teacher and university
professor. He is also a veteran of
WWII and was awarded the North Atlantic Star, the Burma Star with Clasp,
the 1939–1945
Volunteer Service Medal and the Victory Medal. He is currently President
of The Common Cause
Medical Research Foundation, a not-for-profit organisation devoted to
research into neurosystemic
degenerative diseases. He is also Adjunct Professor with the Institute
for Molecular Medicine and he
produces and edits the Journal of Degenerative Diseases. He has
extensively researched neurosystemic
degenerative diseases over the past five years and has authored many
documents on the relationship
between degenerative diseases and a pathogenic mycoplasma called
Mycoplasma fermentans. His
research is based upon solid government evidence.