Looking Back on
the Oxidative Stress Theory of Aids
Eleni
Papadopulos-Eleopulos
Department
of Medical Physics, Royal Perth Hospital, Perth, Western
Australia
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The whole purpose of a scientific theory is to explain the mechanism
behind observations and make predictions. If a theory cannot explain the
observations for which it was put forward, or if its predictions are not
fulfiled, then it should be abandoned. In this regard, despite the lapse
of 18 years, there is still no proof as to the cause(s) of AIDS. Of
course, there are theories but the biggest obstacle in overcoming the
problem of AIDS, and proving its cause, is that one of these theories, the
HIV theory, has been uncritically accepted since 1984. However, of all the
theories, the HIV is the least likely.
The observations the HIV theory was proposed to explain were threefold.
The high frequency of a malignancy, Kaposi's sarcoma (KS), a few
opportunistic infections (OI), principally pneumocystis carinii pneumonia,
and a decrease in a specific cell type, T4 lymphocytes, in gay men, IV
drug users and haemophiliacs. It was accepted that no single infectious
agent could possibly be the direct cause of the multiple diseases seen in
AIDS patients. So, it was proposed that the "hallmark" of HIV infection
was the destruction of T4 cells by HIV which inevitably led to the
appearance of KS and the OI. The proposition that decrease in T4 cells was
the hallmark of HIV/AIDS is difficult to comprehend. At the time when the
HIV theory of AIDS was put forward:
(a) there was no evidence that retroviruses kill cells, to the
contrary;
(b) many factors to which patients belonging to the AIDS risk groups
are exposed are immunosuppressive. This fact was known to some of the best
known HIV experts. In 1985 Montagnier wrote: "This syndrome [the AIDS
diseases] occurs in a minority of infected persons, who generally have in
common a past of antigenic stimulation and of immune depression before LAV
[HIV] infection",1. In the same year Weiss, Ludlam and their associates
wrote (concerning patients with haemophilia): "Our finding...supports our
previous conclusion that the abnormal T-lymphocyte subsets are a result of
the intravenous infusion of Factor VIII concentrates per se, not HTLV-III
infection",2. One year later researchers from CDC: "...factor concentrate
[Factor VIII] itself may be immunosuppressive even when produced from a
population of donors not at risk for AIDS" ,3 ;
(c) evidence also existed that many factors including infections, and
trivial ones, such as exposure to the sun or radiation in solaria lead to
decreased T4 cells. Although some of the T4 decreases were long lasting,
the patients did not develop KS and OI;4 a significant proportion of the
"AIDS" patients, including patients with KS and OI infections, had normal
numbers of T4 cells.4 In other words, T4 decrease (immune deficiency) is
neither necessary nor sufficient for the development of KS and OI. Thus
the proposition that KS and the OI are the result of T4 decrease and that
the T4 decrease detected in the patients belonging to the AIDS risk groups
was caused by HIV infection was totally inconsistent with the data
available even before the hypothesis was put forward. For some time now,
all HIV/AIDS experts, including Robert Gallo, accept that HIV has no
direct or indirect role in KS.5-7
FAILED PREDICTIONS
The HIV theory predicted that HIV was sexually transmitted and
therefore AIDS would spread throughout the heterosexual population.
Obviously this has not happened. The prediction by proponents of the HIV
theory that a vaccine would be developed by 1986 also has not been
fulfilled. In 1984 Montagnier said that the only way to prove HIV is the
cause of AIDS is to have an animal model.8 Although no effort has been
spared, no model of a retrovirus causing AIDS has been forthcoming.
Indeed, the only animal model that bears any resemblance to human AIDS
fully supports a non-infectious modus operandi.9
WHAT LED A PHYSICIST TO STUDY AIDS
At the outbreak of AIDS, Gallo had already spent a decade in attempts
to prove that the cause of some cancers was a retrovirus. This led him to
put forward the retroviral theory of AIDS. From an equally biased position
I put my non-infectious theory. Although trained as a nuclear physicist,
with the exception of a few years, I have worked in the medical field in
the Department of Medical Physics of the Royal Perth Hospital, the largest
teaching hospital in Western Australia. Among its many activities it was
involved in treating cancer by radiation and pioneered hyperthermia for
the same purpose.
It was known that both radiation and radio-sensitisers were oxidising
agents, and apart from hyperbaric oxygen the chemical radiosensitiser
included compounds containing the -NO2 group, that is, nitro-compounds. To
understand the interaction between the agents used to treat cancer and
cancer tissue, I first needed to determine what makes a cell cancerous. I
decided the best way to approach this was to attempt to fully understand
the normal cell. This included the understanding of the mechanism by which
sperm induced the division of the ova. In doing so I developed my own
theory of biological functioning. A short version was first presented at a
meeting in Colorado in 1979 and was published in Speculation in Science
and Technology in 1980. A more detailed version was published in 1982 in
the Journal of Theoretical Biology, after it was first rejected by Nature,
under the title "A Mitotic Theory". Although the title suggests that it
deals only with cellular division and cancer, the theory, as one of the
reviewers pointed out, also proposed a "relationship between modifications
in the redox state of the actin-myosin system and other key biological
processes (e.g. transport, muscle function, metabolism...). Most
importantly in this article, there is a clear integration of older and
present data as well as "classical" and "contemporary" concepts.
The theory claimed that the cellular redox level and its oscillations,
that is, the cyclic variation between oxidation and reduction, plays a
pivotal role in both normal and abnormal cellular function and structure.
Diseases such as cancer, cardiovascular, clotting abnormalities and
ageing, for example are the result of perturbation of the cellular redox
level and its oscillations.
Thus, by the time AIDS was diagnosed I was aware of the biological and
pathological effects induced by many agents (semen, nitrites, recreational
drugs, Factor VIII, infectious agents and the drugs used to eradicate
them) to which the patients belonging to the AIDS risk groups were
exposed.
More importantly all these agents showed a common property: they were
oxidising agents. This led me to put forward the non-infectious theory of
AIDS which claimed that the primary risk factors for AIDS were the
oxidising agents to which the individuals were exposed. While the
manuscript discussing this theory (in which neither HTLV-I nor
Montagnier's retrovirus were mentioned) was in the hands of a few
colleagues for evaluation, Gallo claimed to have proven that HTLV-III was
the cause of AIDS. I was advised to re-write the manuscript to take
account of these claims. The revised manuscript, which was twice rejected
by Nature and initially by Medical Hypotheses, was later accepted by the
latter journal.
PREDICTION OF THE OXIDATIVE STRESS THEORY OF
AIDS
The predictions of my theory included:
(1) AIDS would remain restricted to the risk groups. This has been the
case.
(2) The only sexual act leading to AIDS or a positive antibody test is
a very high frequency of receptive anal intercourse in either sex. One of
the first to publish supporting evidence of this was Gallo and his
associates. In a study published in 1984 he wrote: "of eight different sex
acts, seropositivity correlated only with receptive anal intercourse...and
was inversely correlated with insertive anal intercourse.10 In 1986 Gallo
wrote: "Data from this and previous studies have shown that receptive
rectal intercourse, for example, is an important risk factor for HTLV-III
[HIV] infection. Yet, at the time of entry into this project, nearly half
of the participants still practised this technique. We found no evidence
that other forms of sexual activity contributed to the risk".11 Thus Gallo
was one of the first to publish evidence which contradicted his own
assertion that HIV/AIDS is bi-directionally sexually transmitted.
In 1985 Montagnier and his colleagues reported that the wife of a
haemophilia man who, in addition to other sexual acts, practised anal
intercourse was found to have a positive antibody test and low numbers of
T4 cells. "During 10 months of follow-up his wife remained clinically
well, discontinued exposure to semen, and then lost the LAV antibody, and
regained a normal number of T-helper cells" (T4 cells).12
The best and largest study, the Multicenter AIDS Cohort Study of 4995
gay men, which commenced in 1984 and is still ongoing, also confirmed this
in 1987. "Receptive anal intercourse accounted for nearly all new HIV
infections among the homosexual men enrolled in this study, and the
hazards of this practice need to be emphasised in community educational
projects".13
In a review of most, if not all, epidemiological studies conducted in
gay men published in 1994, the authors concluded: "it can be said that the
cited reports yield convincing evidence that:
(1) unprotected ano-genital receptive intercourse poses the highest
risk for the sexual acquisition of HIV-1 infection;
(3) ano-genital insertive intercourse poses the highest risk for the
sexual transmission of HIV-1 infection;
(4) there is mounting epidemiologic evidence for a small risk attached
to oro-genital receptive sex, biologic plausibility, credible case reports
and some studies show a modest risk, detectable only with powerful
designs; (5) sexual practices involving the rectum and the presence of
(ulcerative) STD facilitate the acquisition of HIV-1;
(5) no or no consistent risk for the acquisition of HIV-1 infection has
been reported regarding other sexual practices such as ano-genital
insertive intercourse and oro-anal sex... (8) the association of substance
use with HIV infection is probably the result of interaction, because
substance use increases the likelihood of practising ano-genital receptive
intercourse".14
Unquestionably, to date, the best designed and executed study in
heterosexuals was conducted by Nancy Padian and her associates. In a paper
entitled "Male-to-Female Transmission of Human Immunodeficiency Virus"
published in 1987 wrote:
"The total number of exposures to the index case (sexual contacts with
ejaculation) and the specific practice of anal intercourse, also with the
infected partner, were associated with transmission".15
The results from their long prospective study of couples, of whom only
one partner of either sex was antibody positive, were published in 1997 in
a paper entitled Heterosexual Transmission of Human Immunodeficiency Virus
(HIV) in Northern California; Results from a Ten-Year Study.
"Prospective results. We followed 175 HIV-discordant couples over time,
for a total of approximately 282 couple-years of follow-up...At last
follow-up, couples were much more likely to be abstinent or to use condoms
consistently, and were much less likely to practice anal intercourse (p
< 0.0005 for all). Nevertheless, only 75% reported consistent condom
use in the 6 months prior to their final follow-up visit...no
seroconversions occurred among exposed partners".16
Thus, a positive antibody test and AIDS, like pregnancy, can be
sexually acquired but not sexually transmitted. The difference is, that
while pregnancy can be acquired by a single sexual intercourse, for AIDS
to appear a very high frequency of receptive intercourse over a long
period is absolutely necessary. AIDS is more like cervical cancer. The
effect is not the result of the act itself, but its high frequency. But,
as with pregnancy and cervical cancer, other factors may mitigate against
the development of AIDS.
(3) Both antibody positive and antibody negative drug users will
develop AIDS and that not only individuals who use dirty needles but also
those who use clean needles or even non-parenteral drugs will develop
positive antibody tests.
According to an interview published in the June 1986 issue of AIDS
ALERT with Susan Neshin, Medical Director of Asbury Park (NJ) Drug
Treatment Center, for clinicians to differentiate between AIDS and the
health problems typically experienced by intravenous drug users, "First
clinicians should interview NDUs to determine if their symptoms are
related to drug abuse or AIDS. You have to talk to them and get them to
tell you if their symptoms are drug-related. They can have weight loss,
diarrhoea, and night sweating, but they could be having that on an on-
going basis from bad dope, withdrawal, or just poor health in general.
It's very common for drug addicts to have inguinal lymphadenopathy, and
maybe a few cervical or axillary nodes that are kind of shoddy. If you see
oral candidiasis in an NDU, that's a real tip off". A few months later
researchers from the USA wrote, "a real T- helper lymphopenia [that is, T4
cell decrease] is only consistent with and not diagnostic of AIDS; other
diseases and some treatment regimens also can express a T-helper
lymphopenia, such as hospitalised IV drug abusers".17
One year later, in an article published in the British Medical Journal,
one reads, "Intravenous drug abusers appear to be at special risk of
acquiring tuberculosis, and a high rate of infection in this group was
reported well before AIDS began".18
In a 1994 paper published in the Scientific American, two researchers
who studied drug abuse wrote, "Many manifestations of AIDS in drug users
who inject are quite different from those in homosexual and bisexual men
who do not use drugs in this manner; in drug users who inject and in their
sexual partners HIV infection is associated with substantially increased
morbidity and mortality from bacterial infections. In the US much of the
resurgence of tuberculosis is occurring among HIV-infected users who live
in crowded conditions without access to good medical care. The CDC
definition of AIDS has been periodically updated to incorporate these
findings".19
In 1994, researchers from Switzerland reported their findings from a
prospective study designed "to examine differences in the incidence and
spectrum of diseases comprising 314 HIV-seronegative NDU, 217
HIV-seropositive NDU, and 10 NDU with admissions registered in either
group (from a total of 1011 admissions)". Narcotic drug users (NDU) were
enrolled in the study if "they were hospitalised for a minimum of 24 hrs,
and also presented with at least one of the following characteristics:
history of either parenteral drug use or a corresponding oral substitutive
medication (mainly methadone); or actual intoxication and miosis [pinpoint
pupils] responding to naloxone; or opiate or cocaine metabolites in a
urine sample. Individuals with exclusive oral drug use other than opiates
were not included". "HIV- seropositive NDU were more frequently admitted
for infectious complications or various non-infectious medical
complications (including as most frequent cases, 38 admissions for
ill-defined episodes, 11 for repeated seizures, nine for acute
pancreatitis, and six for adverse medical drug reaction). Moreover, they
also tended to have a higher admission incidence density for intoxication,
whereas there was no difference in admissions for suicide tentative or
withdrawal reaction". However, individuals from both groups, seropositive
and seronegative were admitted for "infectious complications", including
non-opportunistic pneumonia, purulent bronchitis, tuberculosis, soft
tissue infection, osteoarticular infection, endocarditis, primary
bacteremia and disseminated candidiasis. More importantly, of a total of
541 admissions of seropositive individuals, 187 (35%) were individuals who
had an ORAL mode of drug "application" and 9 (0.5%) inhalation.20
That both intravenous and oral drug users develop positive "HIV"
antibody tests was shown as far back as 1988 when Sterk reported that a
higher percentage of prostitutes who use oral drugs (84%), than IV (46%),
test positive.21
In another study published in 1993, researchers from New York City
tested 1246 seronegative drug users. "Nine had at least one CD4 cell count
of <300 cells/ml or a CD4<20%" and 21 subjects "had one CD4 cell
count between 300 and 500 cells/ul". They also reported that "CD4 cell
counts of <500 cells/ul were, however, associated with subsequent HIV
seroconversion...The relative risk for seroconversion among subjects with
one or more CD4 count <500 cells/ul, compared with HIV-negative
subjects with all counts >500 cells/ul was 4.53"...consistent with an
Italian study showing IDU's with CD4 counts <1,000/ul were more likely
to seroconvert"22. (The authors of the latter reported a "low number of T4
cells was the highest risk factor for HIV infection" (relative
risk=8.5)23. In other words, in drug users, a decrease in T4 cells instead
of following seroconversion is a predictor for seroconversion, a finding
completely at odds with the HIV theory of AIDS.
(4) In Africa there was neither a new disease AIDS nor a new virus HIV.
When Reappraisal of AIDS: Is the oxidation caused by the risk factors the
primary cause? as finally published was written in 1984/85, Africa was not
considered an important issue. Thus, Africa is only briefly mentioned.
Following the 1986 Paris AIDS conference, AIDS in Africa became the
defining example of heterosexual transmission. This is the reason that my
paper was initially rejected by Medical Hypotheses. The March 1987 letter
of resubmission was accompanied by a 12 page document entitled "AIDS in
Africa and its heterosexual transmission". This included the following
summary:
"SUMMARY
a. The operational definition of AIDS in Africa is different from
the rest of the World. In Africa there is neither direct or indirect data
which proves beyond any scientific doubt the existence of a new disease,
AIDS, which affects both men and women equally and of its postulated
causative virus, HTLV-III/LAV assumed to be sexually transmitted.
b. In Africa immune deficiency, opportunistic infections and KS exist
and have existed for a long time in both men and women. However the
pathogens could be other than HTLV-III/LAV, for e.g. poverty, infections
other than HTLV-III/LAV and the drugs used for their treatment, copper,
recreational drugs (if not opiates other traditional drugs), anally or
orally deposited sperm itself via homosexual, bisexual or heterosexual
practices.
The data from Africa used to prove heterosexual transmission will not
stand up to even superficial scientific analysis". The detail of the text
included:
"IMMUNOLOGY In 1, Piot et al., [Lancet 1984,2:65] found that 7 out of
12 controls had low T4 /T8 ratio, 5 of which were due to a decreased T4.
They state "Tuberculosis, protein caloric malnutrition and various
parasitic diseases can all be associated with depression of cellular
immunity".
"...Among healthy Africans resident in a non-AIDS area, the number of
helper and suppressor lymphocytes were the same in HTLV-III/LAV
seropositive and seronegative subjects..." (Bigger, Lancet 1986, 1,
79).
"Parasitic diseases and malnutrition are two possible causes of
immunodepression in Africa. A wide range of prevalent protozoal and
helminthic infestations have been reported to induce immunodeficiency"
(Clumeck, JAMA, 1985, 254, 2599).
"Mild sunstroke induces immunosuppression including T4/T8 inversion"
(Walker, Lancet, 1983, 2, 344).
"Normal volunteers (hospital and university staff) underwent a 12
half-hour exposure to a commercially available solarium on consecutive
days excluding Saturday and Sunday, to acquire a suntan. Tests of immune
function were carried out before, on completion and 2 weeks after
exposure. A number of abnormalities were found in the exposed subjects
including significant decrease in T 4 and T4/T8 which persisted 2 weeks
after exposure". (Hersey, Lancet, 1983, 1, 545).
SEROLOGY
Very high levels of HTLV-III/LAV seropositivity has been reported
from Africa.
"...25% of a sample of hospital workers in Zaire were seropositive in
1984" (Frazer, Med. J. Aust. 1986, 145, 525).
"65% of Ugandan children were found to have been positive in 1972"
(Gallo et al., Ann. Int. Med. 1985, 103, 679).
"15.5% of blood donors were found to be positive at Kigali in Rwanda in
1984" (Clumeck, JAMA, 1985, 254, 2599).
"41 out of 410 (10%) of healthy medical personnel from Mulago Hospital
Kampala were positive for HTLV-III/LAV. 5 out of 30 (17%) of controls
outside the hospital were positive. 4 out of 10 (40%) of control patients
deemed sexually immature were also found positive" (Serwadda, Lancet,
1985, 2, 849).
"Of a total of 274 patients at the Makala Tuberculosis Sanatorium in
Kinshasa, half of the suspected pulmonary cases (total 56); one third of
the confirmed pulmonary cases (160) and two thirds of the remaining 15 who
were confirmed to have extrapulmonary disease tested positive both in the
ELISA and Western blot." (Mann, Paris Conference).
"Forty out of 368 (11%) children admitted to Mama Yemo Hospital in
Kinshasa, Zaire were positive by ELISA and 39 out of the 40, also by
Western Blot. Clinically seropositivity was associated with the diagnosis
of malnutrition and pneumonia" (Davachi, Paris Conference).
"21% of the staff at the Zambian Consolidated Copper Mines, and 14% of
males and 44% of females at the mine hospital were found positive. Other
people tested who had no connection with the mines were negative."
(Buchanan, Lancet, 1986, 1, 155)
The diversity of these reports leads to the conclusion that, either
copper mining, tuberculosis, malnutrition and pneumonia have as their
aetiological factor HTLV-III/LAV or the tests are non-specific. If the
tests are specific, because 10-30%. of infected cases develop AIDS within
3 years (Bigger, Lancet, 1986, 1, 79) then 1.5-4.6% of the Rwanda
population (certainly of its blood donors) and 3.5-7.5% of the Zaireans
(certainly of the medical staff at the hospital where the tests were done
in 1984) should be either dead or dying by the middle of this year, not to
mention prostitutes, Ugandan children, TB patients and workers in regions
with copper mining. Obviously this is not the case. Even Quinn Mann,
Curren and Piot admit that in developing countries, "...serodiagnosis is
complicated by the need for confirmatory testing because of the presence
of possible cross-reacting antibodies" (IV). [Quinn et al., Science 1986,
234:955]
The final section examined the evidence for heterosexual transmission
of AIDS in Africa and concluded that "we are left with a sexually
transmitted disease which: (a) Has continental preferences (b) Has racial
preferences (c) Has sexual preferences. The same bisexual men can get
infected by an African woman but not by a confirmed homosexual AIDS
patient with whom he practices repeatedly exclusive active
intercourse".
That even today in Africa there is no such thing as a new disease AIDS,
and that a positive antibody test does not prove HIV infection, it
suffices to mention that: according to an editorial in the July 11th 1998
Lancet, the developing world "bears more than 90% of the global burden of
HIV infection" and "Tuberculosis (TB) is the leading cause of death
worldwide among people with HIV"; no less an authority in AIDS in Africa
than de Cock admits that TB has been present in Africa in endemic
proportions long before the AIDS era24; no less an authority on HIV/AIDS
than Essex has proved that in Africa a positive antibody test does not
prove HIV infection.25
(5)The theory also predicted that decrease in T4 cells is not the
hallmark of either HIV infection or the clinical syndrome, that is, the
decrease in T4 cells is not HIV specific and is neither necessary nor
sufficient for the syndrome to appear, that is, the clinical syndrome is
not the result of immune deficiency. In fact it was postulated that the
decrease in T4 cells may not be due to their destruction by HIV or any
other agent but could result from (i) the extreme sensitivity of T cells
to oxidative stress; (ii) T4 cells possessing a lower negative charge than
T8 cells could be the first to be destroyed by persistent oxidative
stress; (iii) to be sequestrated in diseased peripheral tissues; (iv)
decreased binding of the T4 antibody as a result of changes in their
surface, that is, due to "down regulation" of the CD4 receptor. To
illustrate that at present this is accepted even by HIV/AIDS experts it
suffices to quote two papers published last year and one more
recently:
"This article discusses the importance of alterations in the CD4+ and
CD8+ cell migration in regulating blood lymphocyte levels and questions
the extent of virus-mediated CD4+ cell destruction";26 "Along with other
recent analyses and experimental developments these considerations also
suggest a need to re-evaluate current concepts about HIV pathogenesis,
including the concept that a systemic depletion of CD4+ T cells is the
hallmark of the disease";27. "CD4+ T-cell lymphopenia is due to both
shortened survival time and a failure to increase the production of
circulating CD4+ T-cells,28.
(6) A most important prediction was that the tissues of AIDS patients
and those at risk would be oxidised, in general, and in particular they
would have low sulphydryl (-SH) group levels. In recent years there have
been hundreds of papers confirming this prediction. The first was
published by German researchers who, for reason(s) not stated, undertook
experiments to determine the level of reduced thiols (-SH) in the blood of
"HIV" infected individuals. They found that: "Blood plasma samples from
HIV-1 infected persons contain elevated glutamate concentrations up to
6-fold the normal level and relatively low concentrations of acid-soluble
thiol (i.e. decreased cysteine concentrations). The intracellular
glutathione concentration in peripheral blood-mononuclear cells (PBMC) and
monocytes from HIV antibody-positive persons are also significantly
decreased",29. Last year a book published with Luc Montagnier as principal
editor further confirms the involvement of oxidative stress in
AIDS,30.
(7) The 10th of July 1986 letter of re-submission to Nature was
accompanied by a response to the reasons given by the Journal for
rejection. The response ended with the following: "If my paper does
nothing other than draw attention to the oxidative nature of the risk
factors and its biological importance, then it offers what is so far the
only hope of treatment which will arrest and reverse the otherwise
invariable fatal course of the disease. In my opinion this alone would
more than justify its publication".
Indeed the most important practical prediction of the theory was that
AIDS can be prevented and treated by stopping exposure to the oxidising
risk factors and by using "currently available therapeutic [antioxidants
in general and SH-containing, in particular] substances". The best
confirmation of this comes from researchers at Stanford University, USA.
In 1997 discussing their results they wrote: "In essence, we have shown
that GSH levels are lower in subjects with CD4 T cell counts below 200/ml
(CD4 <200) than in subjects at earlier stages of HIV disease; that
among subjects with CD4 <200, lower levels of GSB (a FACS measure of
GSH in CD4 T cells) predict decreased survival; and that the probability
of surviving 2-3 years increases dramatically as GSB levels approach
normal range. In addition, we have presented preliminary evidence
suggesting that oral administration of NAC, which supplies the cysteine
required to replenish GSH, may be associated with improved survival of
subjects with very low GSH levels" (GSH-reduced glutathione),31.
Last year they stated: "We have shown that GSH depletion is associated
with impaired survival; the greater the depletion, the worse the prospects
for survival...By replenishing GSH, NAC or other agents we may be able to
modulate such adverse effects of GSH depletion",30. However, although the
authors are most probably aware of our work (the publications of the Perth
group were sent to them a few years ago and are indexed in the Medlines
under oxidative stress), for some unknown reason, they state:
"HIV-infected individuals would be better served if we could identify the
mechanism that underlines the GSH depletion and intervene, if possible, to
prevent its occurrence". The best advice they can give in this regard is:
"it may be prudent for those individuals to avoid excessive exposure to UV
irradiation and unnecessary use of drugs that can deplete GSH - e.g.,
alcohol and prescription or over-the-counter formulations containing
acetominophen [paracetamol]".
(6) Perhaps the boldest claims and predictions were made regarding the
existence of HIV. I wrote HIV, "has never been isolated from fresh AIDS
tissues". Furthermore, HIV "has never been isolated as an independent
stable particle". That is, HIV had not been isolated from either fresh
tissues or culture, which means that its existence had not been proven and
this situation has not changed up to the present day. At least Montagnier
in his 1997 interview to Djamel Tahi admitted that he had not isolated HIV
and in his view neither had Gallo,32. I presented evidence that the
observed phenomena (particles, reverse transcriptase, antibody/antigen
reactions) which were said to prove the existence of HIV were not specific
to a specific retrovirus nor even to retroviruses in general. Unlike
Gallo, Montagnier when interviewed by Djamel Tahi, eventually reluctantly
admitted that these phenomena were not retrovirus specific. I cited
examples of evidence which, taken together, led to the conclusion that
oxidising agents were causing not only AIDS but also gave rise to the
phenomena which were interpreted by the Montagnier and Gallo school as
indicating the presence of HIV. As far back as 1986 Montagnier knew that
the phenomena could not be obtained unless the cultures were stimulated,
although he did not know that the stimulants were oxidising agents,33. In
1991 Anthony Fauci proved that the "HIV" phenomena could be inhibited by
antioxidants,34.
CONCLUSION
It is over twenty years since I conceived the redox theory of
cellular function and nearly as long since its specific application to the
problem of AIDS appeared in Medical Hypotheses. I look back over this time
with very mixed feelings. Naturally I am proud that as a scientific theory
every prediction concerning AIDS has materialised. However, I am saddened
that there are forces at work which have consistently prevented purposeful
but friendly debate. To me and my group the problematic nature of the HIV
theory was apparent from the very beginning. It is now my fervent hope
that, as the HIV theory continues to fail the many patients who are
diagnosed with antibodies to "HIV" and AIDS, the time is rapidly
approaching when scientists and physicians will be eager to examine our
contribution.
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