Health & the Fluid Genome
In her new book, Living
with the Fluid Genome , Mae-Wan Ho
writes,
"The
responsiveness of genes and genomes to the
environment makes clear that the only way to keep
genes and genomes constant and healthy is to have
a balanced ecology... On the other hand, it is
definitely futile to think that we can go on
ruining our ecosystem and stay healthy so long as
we have ‘good’ genes... Genes, unlike
diamonds, are not forever."
This miniseries
offers new insights into how major chronic
diseases arise from the inability to take the
fluid genome seriously, and how strategies to
combat the diseases are similarly misguided and
dangerous.
AIDS Vaccines Worse Than
Useless?
The US administration is
offering AIDS-ravaged nations support for
fighting AIDS tied to the purchase of GM
products. The main anti-AIDS
strategy is a class of vaccines that carries its
own risks. Prominent AIDS researchers have called
repeatedly for a moratorium as evidence of
hazards accumulates. Dr. Mae-Wan
Ho reports.
The complete
document with references, is available
in the ISIS members site. Full details here
George Bush has
taken Europe to the World Trade Organisation over
Europe’s de facto moratorium on GM
imports. In the week of the G8 summit in Evian,
France, Bush blasted Europe for perpetuating
starvation in Africa by blocking US food aid with
anti-GM policies, and announced his pledge of
$15bn to combat AIDS globally, especially in
Africa.
The UN
Population Division reported earlier this year
that by 2050, the population of the hardest hit
nations will have risen by 400 million less
than previously estimated because of AIDS.
"This estimate could be the first sign that
HIV-1 will cause extinction of human beings in
this millennium unless an effective AIDS vaccine
is developed," said a commentary by Veljko
Veljkovic and colleagues in the Lancet,
published in February.
The only AIDS
vaccine to have progressed past phase 3 trial,
made by VaxGen, took 5 years and involved 5108
gay men and 309 women. Unfortunately, it proved
ineffective, and may even be harmful.
In the 3003
white and Hispanic volunteers who received
VaxGen’s vaccine, a higher proportion
suffered breakthrough infections than in the 1508
controls: 6% vs 5%. Although the difference is
not significant, it could indicate a dangerous
trend. But the company is not releasing further
details on the trial results.
A few days
after Bush announced the AIDS package, US
Congress was denounced for tying support for
anti-AIDS research programmes in 50 countries to
their acceptance of GM products. This accusation came from
Julio Sanchez, representative of Mesoamerican
Trade. Introducing GM food to hungry,
malnourished nations ravaged by AIDS is bad
enough in terms of health risks, but AIDS
research programmes are heavily concentrated
towards vaccine development with a strategy that
introduces its own health hazards, as is becoming
increasingly clear. During the past decade, a
number of AIDS researchers, among whom Veljkovic
and his team in Yugoslavia, have been studying
the properties of the human immune deficiency
virus, HIV-1, especially its envelop glycoprotein,
gp120, which features in most of the AIDS
candidate vaccines.
The gp120
protein is strongly immunogenic, which is why it
is widely used in vaccines, in the hope that the
body will produce antibodies against the protein
and hence protect against the virus. But there
have been many worrying signs that this may have
just the opposite effect.
For although the
body mounts a strong immune reaction against the
protein, and produces antibodies against it,
those antibodies fail to protect against
the virus. One main reason is that the virus is
very mutable, and can readily mutate to escape
immune detection. In addition, the immune
reaction mounted against the original gp120
undermines the effectiveness of the immune system
by over-stimulating it, so that it is less
effective to cope with new infections.
A recombinant
gp120 vaccine tested in HIV-negative individuals
in phaseI/II trails, was not effective in
protecting against the disease. Not only that,
participants in the trials had significant levels
of circulating antibodies against the vaccine
before they became infected, and came down with
AIDS disease.
The vaccine
could also be dangerous. A vaccine based on the
gp120 from the strain SF2, actually suppressed
the production of antibodies that could
neutralise the later infecting virus, while
boosting the production of useless antibodies
that were specific for the vaccine strain, SF2.
In other words, gp120 acts as a molecular decoy
to disarm the body’s antiviral response,
leaving it more vulnerable, and increasing the
likelihood of rapid disease progression in those
vaccinated that later became infected. This
phenomenon is called "deceptive
imprinting" of the immune system.
Were those
effects predictable in advance of the clinical
trials? Veljkovic and his colleagues answer a
definite yes.
First of all,
the part of the gp120 molecule that plays the
dominant role in provoking an immune response is
the V3 loop. The V3 loop and flanking regions are
similar in base sequence and structure to the
antigen-binding region of the human
immunoglobulin (Ig) (antibody protein). And it
has been proposed since the early 1990s that this
immunoglobulin-like domain in gp120 may interfere
with the immune regulatory network. This is
strongly supported by later observations that the
anti-V3 and anti-Ig antibodies of healthy
individuals are similar in structure, and that
antibodies reacting to V3 are present in sera
that are HIV-negative.
In 1999, Howard
Urnovitz and colleagues identified a mysterious
case of AIDS in a French woman with no risk
factors. Analysis of the isolated HIV viral
envelope showed that it had homology to sequences
found on at least 14 different human chromosomes.
This opened a whole new can of worms. Was this
rare strain of HIV-1 the result of genetic
recombination (reshuffling) in the human genome,
similar to that found in veterans suffering from
Gulf War syndrome (see "Dynamic genomics", this series)?
Antibodies to human endogenous retroviruses were
found in the urine of patients with clinical
AIDS. Thus, vaccinating against HIV-1 may be
tentamount to vaccinating people against their
own genes (see "Endogenous retroviruses
& chronic disease", this series). Does that
mean genetic reshuffling and retroviral elements
in the human genome may have a key role to play
in AIDS disease, as in Gulf War Syndrome and
other chronic disease?
Another piece of
evidence implicating genetic recombination is
that the V3 loop and its flanking regions are
located between recombination signals similar to
those found in human immunoglobulins, and also
similar to the Chi recombination hotpots
found in many viruses and bacteria. Consequently,
the immunologically dominant region of gp120 may
be involved in recombining with human
immunoglobulin genes resulting in autoimmune
responses, and may also recombine with
co-infecting viruses and bacteria to generate new
pathogens. Evidence of such recombination has
subsequently been found in the sera of AIDS
patients.
Many other
observations have linked gp120 with
auto-antibodies that react against the
body’s own cells and enhance the infectivity
of HIV-1, and those researchers have also issued
warnings against AIDS vaccines.
In fact,
warnings against AIDS vaccines go back to Albert
Sabin, one of the most prominent viral vaccine
developers of the 20th century.
"The available data provide no basis for
testing any HIV vaccine in human beings either
before or after infection," Sabin stated.
The current
issue of Vaccine carries an article
evaluating the long-term safety of a range of
AIDS vaccines involving 3189 HIV uninfected,
healthy volunteers who were enrolled into 51
NIAID (NIH) - sponsored Phase I and II clinical
trials. It concluded that there were no adverse
effects. Veljkovic remarks, "This conclusion
was based on analysis of many important
parameters ….Unfortunately, the key
information - comparison of the health status
between breakthrough infected vaccinated
volunteers and control subjects who participated
in these trials - was not reported, just as it
was not reported by VaxGen in the results of
their Phase III clinical trial."
Unless this
information is reported, says Veljkovic, the
companies and institutions that organized these
clinical trials are in danger of committing a
scientific and ethical misconduct.
It is pertinent
to point out that transgenic DNA in GM food and
feed also carry recombination hotspots, such as
the ones associated with the CaMV 35S promoter
and the left and right borders of the Agrobacterium
T-DNA used as vector to introduce transgenic DNA
into the plant genome. These recombination
hotspots enhance horizontal gene transfer and
recombination. Furthermore, as Veljkovic said,
the recombination hotspots in transgenic DNA may
interact with the recombination signals flanking
the V3 loop of the gp120 gene in AIDS vaccines to
generate yet more exotic viruses.
Veljkovic and
his colleagues have repeated their call for an
immediate moratorium on the current clinical
trials of HIV-1 gp120/160 vaccines.
http://www.i-sis.org.uk/
The complete
document with references, is available
in the ISIS members site.
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