[CTRL] FW: Anthrax vaccinations, Military resistors, Mycoplasma Fermentans-2

[Dave]

 -Caveat Lector-

Dave Hartley
http://www.Asheville-Computer.com
http://www.ioa.com/~davehart


-----Original Message-----
From: Prof. Garth Nicolson [mailto:[EMAIL PROTECTED]]
Sent: Saturday, October 30, 1999 5:51 PM
To: Dave
Subject: Re: Anthrax vaccinations, Military resistors, Mycoplasma
Fermentans-2



Prof. Garth Nicolson
The Institute for Molecular Medicine
15162 Triton Lane
Huntington Beach, CA 92649
714-903-2900

http://www.immed.org
Please note that our address is no longer in Irvine, CA.
You can also call our telephone number and use the menu to request materials
and publications be Faxed back immediately.


BACTERIA TIED TO CHRONIC ILLNESSES

BY DAN VERGANO


EMBARGOED FOR RELEASE MONDAY AT 12:01 AM EST, AUG. 30, 1999



Slow growing infections may cause or promote a host of chronic illnesses,
including Chronic Fatigue Syndrome, Fibromyalgia Syndrome and Gulf War
Syndrome, according to one team of researchers.

 "We've found a large subset of various chronic illnesses are associated
with infections," said Prof. Garth L. Nicolson of the Institute for
Molecular Medicine in Huntington Beach, Calif.  Specifically, infections
caused by primitive bacteria known as mycoplasms, he added. Symptoms such as
fatigue, headaches, soreness, joint pain and others overlap across many
chronic illnesses, he noted. And patients with these ailments have few
treatment options because of limited understanding about the cause of their
signs and symptoms.

 In a study published in the Monday edition of the journal Medical Sentinel,
the official, peer-reviewed journal of the Association of American
Physicians and Surgeons, Nicolson and his colleagues lay out the case for
mycoplasms as one of the
culprits behind Chronic Fatigue Syndrome, Fibromyalgia Syndrome, Gulf War
Syndrome and Rheumatoid Arthritis. In one study on 203 Chronic Fatigue
Syndrome patients, around 70 percent had mycoplasma  DNA in their
bloodstream, indicarting the presence of mycoplasmas.   In contrast, only
nine percent of 70 healthy individuals he compared them to carried such
signs.

 Another trial compared 200 Gulf War Syndrome patients to 62 healthy
military subjects.  People with the illness were more than seven times more
likely
to have mycoplasmal  infections, said Nicolson.

 Mycoplasmas lack many of the features of more aggressive infectious
bacteria, such as cell walls, that enable antibiotics like penicillins  to
target invading germs.   Because of their simple structure, mycoplasmas
reproduce slowly, using the machinery of invaded cells to produce their
energy and many of their synthetic moleucles.   Nicolson theorized that
individuals with immune systems compromised by a viruses, radiation or
pollutants are at risk from mycoplasmal infections.

 "The breakthrough is using new genetic tools to find and measure the
bacteria. We couldn't do that before," said Nicolson, who has adapted the
DNA analysis used by crime investigators to detect germ genes in each
patient's bloodstream.  Once mycoplasmas are identified, Nicolson provides
antibiotic treatment suggestions to physicians who then treat their
patients.

 "We really need to know more about these organisms before we can say with
certainty what illnesses they cause," said Joseph Tully, who recently
retired as chief of the mycoplasma lab at the National Institute of Allergy
and Infectious Diseases (NIAID) division in Fredrick, MD. He added that
physicians who treat chronic illnesses have estimated that more than a
quarter of their patients benefit from long-term antibiotic treatment, which
he said inhibits mycoplasmas  long enough for the body's natural immune
system to wipe out the invaders. "I think that treatment is fine as long as
doctors tell their patient it's experimental," he added.

 Two federal efforts based on Nicolson�s results are now underway seek to
determine whether antibiotics can cure chronic illness.   One conducted at
Walter Reed Army Medical Center looks at the blood of Gulf War veterans for
signs of mycoplasms.   The other, conducted at Veterans Affairs Medical
Centers nationwide, involves giving some mycoplasma-positive  Gulf War
Syndrome patients antibiotics and others dummy pills under rigorous
experimental conditions designed to ferret out the true effectiveness of the
therapy.

Medical Sentinel (1999;4:172-176)


 ******************************************************************
 Dan Vergano   | 703/527-6065(o)
 DC Correspondent  | 703/527-6075(f)
 Medical Tribune    [EMAIL PROTECTED]
 520 N. Garfield St. #2  |
 Arlington, VA 22201  |
 ******************************************************************


[Note: the final version of this press release may vary slightly after
editing.  G.L.N.]
 The full article is at:

http://www.haciendapub.com/article24.html


____________________________________________________________________________
______

Medical Sentinel 1999; 4: 172-176. Medical Sentinel is the official,
peer-reviewed journal of the Association of American Physicians and Surgeons
(AAPS).


MYCOPLASMAL INFECTIONS IN CHRONIC ILLNESSES: FIBROMYALGIA AND CHRONIC
FATIGUE SYNDROMES, GULF WAR ILLNESS, HIV-AIDS AND RHEUMATOID ARTHRITIS



Prof. Garth L. Nicolson, Marwan Y. Nasralla, Joerg Haier, Robert Irwin,
Nancy L. Nicolson and Richard Ngwenya


The Institute for Molecular Medicine, 15162 Triton Lane, Huntington Beach,
CA 92649 and
 James Mobb Immune Enhancement, Harare, Zimbabwe


ABSTRACT Invasive bacterial infections are associated with several acute and
chronic illnesses, including:  Aerodigestive Diseases such as Asthma,
Pneumonia, Inflammatory Bowel Disease; Rheumatoid Diseases, such as
Rheumatoid Arthritis (RA); Immunosuppression Diseases such as HIV-AIDS;
Genitourinary Infections and Chronic Fatigue Illnesses such as Chronic
Fatigue Syndrome (CFS), Fibromyalgia Syndrome (FMS) and Gulf War Illnesses
(GWI). It is now apparent that such infections could be causative, cofactors
or opportunistic agents in a variety of illnesses. Using Forensic Polymerase
Chain Reaction we have looked for the presence of one class of invasive
infection (mycoplasmal infections) inside blood leukocyte samples from
patients with CFS (Myalgic Encephalomyelitis ), FMS, RA and GWI.  There was
a significant difference between symptomatic CFS, FMS, GWI and RA patients
with positive mycoplasmal infections of any species (45-63%) and healthy
positive controls (6-9%) (P<0.001).  This difference was even greater when
specific species (M. fermentans, M. hominis, M. penetrans, M. pneumoniae)
were detected.  Except  for GWI, most patients had multiple mycoplasmal
infections (more than one species of mycoplasma).  Patients with different
diagnoses but overlapping signs and symptoms often have mycoplasmal
infections, and such mycoplasma-positive patients generally respond to
multiple cycles of particular antibiotics (doxycycline, minocycline,
ciprofloxacin, azithromycin and clarithromycin).  Multiple cycles of these
antibiotics plus nutritional support appear to be necessary for successful
treatment.  In addition, immune enhancement and other supplements appear to
help these patients regain their health.  Other chronic infections may also
be involved to various degrees with or without mycoplasmal infections  in
causing patient morbidity in chronic illnesses.

Introduction--Chronic Illnesses

 There is growing awareness that many chronic illnesses may have an
infectious nature that is either responsible (causative) for the illness, a
cofactor for the illness or appears as an opportunistic infection(s) that is
responsible for aggravating patient morbidity [1].  There are several
reasons for this notion, including the nonrandom or clustered appearance of
an illness, often in immediate family members, the course of the illness and
its response to therapies based on infectious agents.  Since chronic
illnesses are often complex, involving multiple, nonspecific, overlapping
signs and symptoms, they are difficult to diagnose and even more difficult
to treat.  Most chronic illnesses do not have effective therapies, and
patients rarely recover from their conditions [2], causing in some areas of
the world catastrophic economic problems.
 Some chronic illnesses, such as Rheumatoid Arthritis (RA), are well
established in their clinical diagnosis [3], whereas others, such as Chronic
Fatigue Syndrome (CFS, sometimes called Myalgic Encephalomyelitis),
Fibromyalgia Syndrome (FMS) and Gulf War Syndrome or Gulf War Illnesses
(GWI), have rather nonspecific but similar complex, multi-organ signs and
symptoms that overlap or are almost identical [1].  In the case of CFS, FMS
and GWI these include:  chronic fatigue, headaches, muscle pain and
soreness, nausea, gastrointestinal problems, joint pain and soreness, lymph
node pain, cognitive problems, depression, breathing problems and other
signs and symptoms [4].   The major difference between these illnesses
appears to be in the severity of specific signs and symptoms.  For example,
FMS patients have as their major complaint muscle and overall pain, soreness
and weakness, whereas CFS patients most often complain of chronic fatigue
and joint pain, stiffness and soreness, but otherwise their complaints
usually overlap [5].  Often these patients have increased sensitivities to
various environmental irritants and enhanced allergic responses.  Although
chronic fatigue illnesses have been known for several years, most patients
with CFS, FMS, GWI and in some cases RA have had few treatment options.
This may have been due to the imprecise nature of their diagnoses, which are
based primarily on clinical observations rather than laboratory tests, and a
lack of understanding about the underlying causes of these illnesses or the
factors responsible for patient morbidity [1].  These illnesses could have
different initial causes or triggers but similar cofactors or similar
opportunistic infections that cause significant morbidity.

Chronic Illnesses--Overlapping Signs and Symptoms

 The multiple signs and symptoms of FMS, CFS and GWI are complex,
nonspecific and completely overlapping (Figure 1), suggesting that these
illnesses are related and not completely separate syndromes [1, 6].   In
this figure only differences in the signs and symptoms after the onset of
illness are shown, and the data for FMS and CFS have been combined, because
previous studies indicated that with the exception of muscle pain and
tenderness, there was essentially no difference in patient signs [4].
Illness Survey Forms were analyzed to determine the most common signs and
symptoms at the time when blood was drawn from patients.  The intensity of
patient signs and symptoms prior to and after onset of illness was recorded
on a 10-point rank scale (0-10, extreme).  The data were arranged by 38
different signs and symptoms and were considered positive if the value after
onset of illness was two or more points higher than prior to the onset of
illness. The data in Figure 1 indicate that patients diagnosed with CFS or
FMS had complex signs and symptoms that were similar to those reported for
GWI.  In addition, the presence of rheumatoid signs and symptoms in each of
these disorders indicates that there are also similarities to RA [7].
Moreover, it is not unusual to find immediate family members who display
similar signs and symptoms.  For example, there is evidence that GWI has
slowly spread to immediate family members [8],  and it is likely that it has
also spread to some degree in the workplace [1].  A preliminary survey of
approximately 1,200 GWI families indicated that approximately 77% of spouses
and a majority of children born after the war had signs and symptoms similar
or identical to veterans with GWI [8].
 In the absence of laboratory tests to the contrary, chronic illnesses are
often misdiagnosed as somatoform disorders caused by stress and other
nonorganic factors [9].  Patients with CFS, FMS and GWI usually have
cognitive problems, such as short term memory loss, difficulty concentrating
and other problems, and physicians who find psychological or psychiatric
problems in these patients often decide that these conditions are caused by
somatoform disorders, not organic problems [1].  Stress is often mentioned
as an important factor or the important factor in these disorders.  Indeed,
GWI patients are often diagnosed with Post Traumatic Stress Disorder (PTSD)
in veterans� and military hospitals [10].  The evidence that has been
offered as proof that stress or PTSD is the source of GWI sickness is the
assumption that veterans must have suffered from stress by virtue of the
stressful environment in which they found themselves during the Gulf War
[10], but the veterans themselves do not feel that stress-related diagnoses
are an accurate portrayal of their illnesses.  Most testimony to date
refutes the notion that stress is the major factor in GWI [11], suggesting
that stress, albeit important, is not the cause of GWI [12].  But most
physicians would agree that stress can exacerbate chronic illnesses and
suppress immune systems, suggesting that stress plays a secondary not
primary role in chronic illnesses, such as GWI, CFS and FMS [1].  However,
in the absence of physical or laboratory tests that can identify possible
origins of FMS, CFS or GWI, many physicians accept that stress is the cause
of these chronic illnesses.  It has been only recently that other causes
were seriously considered, including chronic infections [13].

Mycoplasmal Infections in CFS, FMS and GWI

 We have been particularly interested in the roles of certain chronic
infectious agents in CFS, FMS and GWI, because these microorganisms can
cause most or essentially all of the signs and symptoms found in these
patients [1, 14].  One of the types of infections that elicited our
attention are microorganisms of the class Molecutes, small bacterial
mycoplasmas, lacking cell walls, that are capable of invading several types
of human cells and are associated with a wide variety of human diseases
[14].
 We have examined the presence of mycoplasmal blood infections in GWI, CFS
and FMS patients.  The clinical diagnosis of these disorders was obtained
from referring physicians according to the patients� major signs and
symptoms.  Since the signs and symptoms of CFS and FMS patients  completely
overlapped, these patients were therefore considered together (CFS/FMS) [1].
Blood was collected, shipped over night at 4�C and processed immediately for
PCR after purification of DNA using a Chelex procedure [1, 7].  Patients�
blood was analyzed for the presence of mycoplasmal infections in blood
leukocytes.  Positive PCR results were confirmed if the PCR product was 717
base pairs in size using the genus-specific primers (or 850 base pairs for
M. fermentans specific primers, etc.) along with a positive control of the
same size in the same gel, and if a visible band obtained after
hybridization with the internal probe [15].  The sensitivity and specificity
of the PCR methods were determined by examining serial dilutions of purified
DNA of M. fermentans, M. pneumoniae, M. penetrans, M. hominis and M.
genetalium.  Amounts as low as 10 fg of purified DNA were detectable for all
species using the genus primers.  The amplification with genus primers
produced the expected fragment size in all tested species, which was
confirmed by hybridization with an inner probe [16].
 Mycoplasma tests were performed on all patients as described previously [1,
7, 17] either from Chelex-purified DNA or DNA prepared from whole blood
using a commercial kit.  The targeted Mycoplasma spp. sequence was amplified
from DNA extracted from the peripheral blood of 144/203 CFS or FMS patients
(71%).  In 70 healthy subjects positive results for Mycoplasma spp. were
obtained in 6 samples (~9%).  Two of these were positive for M. fermentans.
The difference between patient and control groups was significant (p<0.001)
[16]. The ratio between positive and negative patients was comparable in
female and male patients.  Similarly, using Nucleoprotein Gene Tracking to
analyze the blood leukocytes from GWI patients we found that 91/200 (45%)
were positive for mycoplasmal infections [18, 19].   In contrast, in
nondeployed, healthy adults the incidence of mycoplasmal infections was 4/62
(~6%) [18, 19].
 Patients with FMS or CFS often have multiple mycoplasmal infections and
probably other chronic infections as well.  When we examined CFS/FMS
patients for M. fermentans, M. pneumoniae, M. penetrans, M. hominis
infections, multiple infections were found in over one-half of ~100 patients
(Figure 2).  CFS/FMS patients had double (over 30%) or triple (over 20%)
mycoplasmal infections, but only when one of the species was M. fermentans
or M. pneumoniae [17].  Higher score values for increases in the severity of
signs and symptoms were also found in patients with multiple infections.
CFS/FMS patients infected with different mycoplasma species generally had a
longer history of illness, suggesting that patients may have contracted
additional infections with time [17].
 In the course of our studies we found that DNA preparation and blood
storage was extremely important in preserving the test samples.  Storage of
blood frozen or at 0-4�C resulted in reproducible assay results, whereas
storage at room temperature resulted in loss of PCR signal over time.
Within 1-2 days at room temperature, most of the positive samples reverted
to negative results [1].  Also, blood drawn in tubes (blue-top) containing
citrate and kept at  0-4�C before the assay yielded better results than
other anticoagulants, unless the samples were frozen in EDTA (purple-top)
tubes.

Mycoplasmal Infections in Rheumatoid Diseases

 The underlying causes of rheumatoid diseases are not known, but RA and
other autoimmune diseases could be triggered or exacerbated  by infectious
agents.  It has been known for some time that infectious diseases in some
animal species result in remarkable clinical and pathological similarities
to RA and other rheumatoid diseases.  Aerobic and anaerobic intestinal
bacteria, viruses and mycoplasmas have been proposed as important agents in
RA [20].  Recently there has been increasing evidence that mycoplasmas may
play a role in the initiation or progression of RA [21].  Mycoplasmas have
been proposed to interact nonspecifically with B-lymphocytes, resulting in
modulation of immunity, autoimmune reactions and promotion of rheumatoid
diseases [22].  M. pneumoniae, M. salivarium and U. urealyticum have also
been found in the joint tissues of patients with rheumatological diseases,
suggesting their pathogenic involvement [23].
 When we examined RA patients� blood leukocytes for the presence of
mycoplasmas, we found that approximately one-half were infected with various
species of mycoplasmas [7].  The most common species found was M.
fermentans, followed by M. pneumoniae and M. hominis and finally M.
penetrans.  Similar to what we found in CFS/FMS patients, there was a high
percentage of multiple mycoplasmal infections in RA patients when one of the
species was M. fermentans [7].
 Although the precise role of mycoplasmas in RA and other rheumatoid
inflammatory diseases remains unknown, mycoplasmas could be important
cofactors in the development of inflammatory responses and progression of
the disease.  As an example of the possible role of mycoplasmas in
rheumatological diseases, M. arthritidis infections in animals can trigger
and exacerbate autoimmune arthritis [24].  This mycoplasma can also suppress
T-cells and release substances that act on polymorphonuclear granulocytes,
such as oxygen radicals, chemotactic factors  and other substances [25].
Mycoplasmal infections can increase proinflammatory cytokines, such as
Interleukin-1, -2 and -6 [26], suggesting that they are involved in the
development and possibly progression of rheumatological diseases.
 In addition to mycoplasmal infections, other microorganisms have been under
investigation as cofactors or causative agents in rheumatological diseases.
The discovery of EB virus [27] and cytomegalovirus [28]  in the cells of the
synovial lining in RA patients suggested their involvement in RA, possibly
as a cofactor.  There are a number of bacteria and viruses that are
candidates in the induction of RA or its progression [29].  In support of
bacterial involvement in RA, it has been known for some time that
antibiotics like minocycline can alleviate the clinical signs and symptoms
of RA [30].  Although this has been proposed to be due to their
anti-inflammatory activities, these drugs are likely to be acting to
suppress infections of sensitive microorganisms like mycoplasmas.

Mycoplasmal Infections in Immunosuppresive and Autoimmune Diseases

 Mycoplasmas have been implicated in the progression of HIV-AIDS.  It has
been known for some time that some species of mycoplasmas are associated
with certain terminal human diseases, such as an acute fatal illness found
with certain Mycoplasma fermentans  infections in non-AIDS patients [31].
Recently, mycoplasmal infections have attracted attention as a major source
of morbidity in AIDS patients.  For example, M. fermentans  can cause renal
and CNS complications in patients with AIDS [32],  and M. penetrans has also
been found in the respiratory epithelial cells of AIDS patients [33].  Other
species of mycoplasmas have also been found in AIDS patients where they have
been associated with disease progression, such as M. prium and M. hominis
[31].  Montagnier and Blanchard [34] have proposed that mycoplasmas are
cofactors in HIV-AIDS, accelerating progression and accounting, at least in
part, for increased susceptibility of AIDS patients to additional
infections.  In addition to immune suppression, some of this increased
susceptibility may be the result of mycoplasma-induced host cell membrane
damage from toxic oxygenated products released from intracellular
mycoplasmas [35].  Also, mycoplasmas may regulate HIV-LTR-dependent gene
expression [36], suggesting that mycoplasmas may play an important
regulatory role in HIV pathogenicity.
 There is some preliminary evidence that mycoplasmal infections could be
associated with autoimmune diseases.  In some mycoplasma-positive GWI cases
the signs and symptoms of Multiple Sclerosis (MS), Amyotrophic Lateral
Sclerosis (ALS or Lew Gehrig�s Disease), Lupus, Graves� Disease and other
complex autoimmune diseases have been seen.  Such usually rare autoimmune
responses are consistent with certain chronic infections, such as
mycoplasmal infections, that penetrate into nerve cells, synovial cells and
other cell types.  These autoimmune signs and symptoms could be caused when
intracellular pathogens, such as mycoplasmas, escape from cellular
compartments and incorporate into their own structures pieces of host cell
membranes that contain important host membrane antigens that can trigger
autoimmune responses.  Alternatively, mycoplasma surface �superantigens� may
directly stimulate autoimmune responses [37].

Mycoplasmal Infections in Other Clinical Conditions

 Asthma, airway inflammation, chronic pneumonia and other respiratory
diseases are known to be associated with mycoplasmal infections.  For
example, M. pneumoniae is a common cause of upper respiratory infections,38
and severe Asthma is commonly associated with mycoplasmal infections [39].
Recent evidence has shown that certain mycoplasmas, such as M. fermentans
(incognitus strain), are unusually invasive and often found within
respiratory epithelial cells [33].
 Heart infections (myocarditis, endocarditis, pericarditis and others) are
often due to chronic infections, such as Mycoplasma [40, 41], Chlamydia [42]
and possibly other infectious agents.
 Other species of mycoplasmas are also associated with various illnesses: M.
hominis infections were first found in patients with hypogammaglobulinemia,
and M. genitalium  was first isolated from the urogenital tracts of patients
with nongonococcal urethritis [43, 44].  Although mycoplasmas can exist in
the oral cavity and gut as normal flora, when they penetrate into the blood
and tissues, they can cause a variety of acute or chronic illnesses.  These
cell-penetrating  species, such as M. penetrans, M. fermentans and M. pirum
among others, can cause complex systemic signs and symptoms. Mycoplasmas are
also very effective at evading the immune system, and synergism with other
infectious agents can occur [14].  Similar types of chronic infections
caused by Chlamydia, Brucella, Coxiella or Boriella may also be involved
either as single agents or as complex, multiple infections (see Figure 2) in
many of the diseases discussed above.

Mycoplasmal Infections--Treatment Suggestions

 Once mycoplasmal infections have been identified in the white blood cell
fractions of subsets of CFS, FMS, GWI, RA and other patients, they can be
successfully treated.  Appropriate treatment with antibiotics should result
in patient improvement and even recovery [6, 18, 19].  The recommended
treatments for mycoplasmal blood infections require long-term antibiotic
therapy, usually multiple 6-week cycles of doxycycline (200-300 mg/day)
[45], ciprofloxacin (1,500 mg/day), azithromycin (500 mg/day) or
clarithromycin (750-1,000 mg/day) [46].  Multiple cycles are required,
because few patients recover after only a few cycles, possibly because of
the intracellular locations of mycoplasmas like M. fermentans and M.
penetrans, the slow-growing nature of these microorganisms and their
relative drug sensitivities.  For example, of 87 GWI patients that tested
positive for mycoplasmal infections, all patients relapsed after the first
6-week cycle of antibiotic therapy, but after up to 6 cycles of therapy
69/87 patients recovered and returned to active duty [18, 19].  The clinical
responses that were seen were not due to placebo effects, because
administration of some antibiotics, such as penicillins, resulted in
patients becoming more not less symptomatic, and they were not due to
immunosuppressive effects that can occur with some of the recommended
antibiotics.  Interestingly, CFS, FMS and GWI patients that slowly recover
after several cycles of antibiotics are generally less environmentally
sensitive, suggesting that their immune systems may be returning to
pre-illness states.  If such patients had illnesses that were caused by
psychological or psychiatric problems or solely by chemical exposures, they
should not respond to the recommended antibiotics and slowly recover.  In
addition, if such treatments were just reducing autoimmune responses, then
patients should relapse after the treatments are discontinued [1].
 Patients with CFS, FMS, RA or GWI usually have nutritional and vitamin
deficiencies that must be corrected [46].  These patients are often depleted
in vitamins B, C and E and certain minerals.  Unfortunately, patients with
these chronic illnesses often have poor absorption.  Therefore, high doses
of some vitamins must be used, and others, such as vitamin B complex, must
be given sublingual. Antibiotics that deplete normal gut bacteria can result
in over-growth of less desirable flora, so Lactobacillus acidophillus
supplementation is recommended.  In addition, a number of natural remedies
that boost the immune system are available and are potentially useful,
especially during antibiotic therapy or after therapy has been completed
[46].  One of us (R.N.) has been involved in the development of ancient
African and Chinese natural immune enhancers and cleansers help to restore
natural immunity and absorption.  Although these products are known to help
AIDS patients, their clinical effectiveness in GWI/CFS/FMS/RA patients has
not been carefully evaluated.  They appear to be useful during therapy to
boost the immune system or after antibiotic therapy in a maintenance program
to prevent relapses [43].

Conclusions

 We have proposed that chronic infections are an appropriate explanation for
the morbidity seen in a rather large subset of CFS, FMS, GWI and RA
patients, and in a variety of other illnesses.  Not every patient will have
this as a diagnostic explanation or have the same types of chronic
infections [1, 7, 17].  Some patients may have chemical or radiological
exposures or other environmental problems as an underlying reason for their
chronic signs and symptoms.  In these patients, chronic infections may be
opportunistic.  In others, somatoform disorders or illnesses caused by
psychological or psychiatric problems may indeed be important.  However, in
these patients antibiotics or immune enhancers should have no lasting effect
whatsoever, and they should not recover on such therapies.  The
identification of specific infectious agents in the blood of chronically ill
patients may allow many patients with CFS, FMS, GWI or RA and other chronic
diseases to obtain more specific diagnoses and effective treatments for
their illnesses.  Finally, patients with cardiopathies, AIDS, respiratory
illnesses and urogenital infections are often infected with Mycoplasma,
Chlamydia, Brucella or other chronic, invasive bacterial and parasitic
infections, and these patients could benefit from appropriate antibiotic and
neutraceutical therapies that alleviate morbidity.

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Prof. Garth L. Nicolson, Drs. Marwan Nasralla, Joerg Haier, Robert Irwin and
Nancy L. Nicolson are affilated with The Institute for Molecular Medicine,
15162 Triton Lane, Huntington Beach, CA 92649-1401, Tel: +1-714-903-2900,
Fax: +1-714-379-2082, website: www.immed.org, email: [EMAIL PROTECTED];
Dr. Richard Ngwenya is affiliated with the James Mobb Immune Enhancement
Clinics, 132 Josiah Chinamano Ave., Harare, Zimbabwe, Fax: +263-4-739-832.
Figure Legends

Figure 1. Incidence of increase in severity of signs and symptoms in 203
patients with CFS/FMS compared to GWI after the onset of illness.  Severity
of signs and symptoms was assessed using a Patient Illness Survey Form that
included 114 signs and symptoms.  The intensity of signs and symptoms were
scored by patients on a 10-point scale (0, none; 10, extreme) prior to and
after onset of illness.  Scores were determined in each category (3-9
questions) as the sum of differences between values prior to and after onset
of illness divided by the number of questions in the category.  Changes in
socre values of 2 or more points were considered relevant.

Figure 2. Incidence of multiple mycoplasmal infections in 93 CFS/FMS
patients.  Patients were examined for M. fermentans, M. pneumoniae, M.
penetrans or M. hominis blood infections by Forensic PCR.

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