Another AIDS breakthrough

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Justforfun000
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Another AIDS breakthrough

Post by Justforfun000 »

This looks even more promising if they can actually apply it in vivo.
Pathologists Believe They Have Pinpointed Achilles Heel Of HIV
Main Category: HIV / AIDS
Article Date: 16 Jul 2008 - 1:00 PDT



Human Immunodeficiency Virus (HIV) researchers at The University of Texas Medical School at Houston believe they have uncovered the Achilles heel in the armor of the virus that continues to kill millions.

The weak spot is hidden in the HIV envelope protein gp120. This protein is essential for HIV attachment to host cells, which initiate infection and eventually lead to Acquired Immunodeficiency Syndrome or AIDS. Normally the body's immune defenses can ward off viruses by making proteins called antibodies that bind the virus. However, HIV is a constantly changing and mutating virus, and the antibodies produced after infection do not control disease progression to AIDS. For the same reason, no HIV preventative vaccine that stimulates production of protective antibodies is available.

The Achilles heel, a tiny stretch of amino acids numbered 421-433 on gp120, is now under study as a target for therapeutic intervention. Sudhir Paul, Ph.D., pathology professor in the UT Medical School, said, "Unlike the changeable regions of its envelope, HIV needs at least one region that must remain constant to attach to cells. If this region changes, HIV cannot infect cells. Equally important, HIV does not want this constant region to provoke the body's defense system. So, HIV uses the same constant cellular attachment site to silence B lymphocytes - the antibody producing cells. The result is that the body is fooled into making abundant antibodies to the changeable regions of HIV but not to its cellular attachment site. Immunologists call such regions superantigens. HIV's cleverness is unmatched. No other virus uses this trick to evade the body's defenses."

Paul is the senior author on a paper about this theory in a June issue of the journal Autoimmunity Reviews. Additional data supporting the theory are to be presented at the XVII International AIDS Conference Aug. 3-8 in Mexico City in two studies titled "Survivors of HIV infection produce potent, broadly neutralizing IgAs directed to the superantigenic region of the gp120 CD4 binding site" and "Prospective clinical utility and evolutionary implication of broadly neutralizing antibody fragments to HIV gp120 superantigenic epitope."

First reported in the early 1980s, HIV has spread across the world, particularly in developing countries. In 2007, 33 million people were living with AIDS, according to a report by the World Health Organization and the United Nations.

Paul's group has engineered antibodies with enzymatic activity, also known as abzymes, which can attack the Achilles heel of the virus in a precise way. "The abzymes recognize essentially all of the diverse HIV forms found across the world. This solves the problem of HIV changeability. The next step is to confirm our theory in human clinical trials," Paul said.

Unlike regular antibodies, abzymes degrade the virus permanently. A single abzyme molecule inactivates thousands of virus particles. Regular antibodies inactivate only one virus particle, and their anti-viral HIV effect is weaker.

"The work of Dr. Paul's group is highly innovative. They have identified antibodies that, instead of passively binding to the target molecule, are able to fragment it and destroy its function. Their recent work indicates that naturally occurring catalytic antibodies, particularly those of the IgA subtype, may be useful in the treatment and prevention of HIV infection," said Steven J. Norris, Ph.D., holder of the Robert Greer Professorship in the Biomedical Sciences and vice chair for research in the Department of Pathology and Laboratory Medicine at the UT Medical School at Houston.

The abzymes are derived from HIV negative people with the autoimmune disease lupus and a small number of HIV positive people who do not require treatment and do not get AIDS. Stephanie Planque, lead author and UT Medical School at Houston graduate student, said, "We discovered that disturbed immunological events in lupus patients can generate abzymes to the Achilles heel of HIV. The human genome has accumulated over millions of years of evolution a lot of viral fragments called endogenous retroviral sequences. These endogenous retroviral sequences are overproduced in people with lupus, and an immune response to such a sequence that resembles the Achilles heel can explain the production of abzymes in lupus. A small minority of HIV positive people also start producing the abzymes after decades of the infection. The immune system in some people can cope with HIV after all."

Carl Hanson, Ph.D., who heads the Retrovirus Diagnostic Section of the Viral and Rickettsial Disease Laboratory of the California Department of Public Health, has shown that the abzymes neutralize infection of human blood cells by diverse strains of HIV from various parts of the world. Human blood cells are the only cells that HIV infects.

"This is an entirely new finding. It is a novel antibody that appears to be very effective in killing the HIV virus. The main question now is if this can be applied to developing vaccine and possibly used as a microbicide to prevent sexual transmission," said David C. Montefiori, Ph.D., director of the Laboratory for AIDS Vaccine Research & Development at Duke University Medical Center. The abzymes are now under development for HIV immunotherapy by infusion into blood. They could also be used to guard against sexual HIV transmission as topical vaginal or rectal formulations.

"HIV is an international priority because we have no defense against it," Paul said. "Left unchecked, it will likely evolve into even more virulent forms. We have learned a lot from this research about how to induce the production of the protective abzymes on demand. This is the Holy Grail of HIV research -- development of a preventative HIV vaccine."

Major contributors to the research from the UT Medical School include Yasuhiro Nishiyama, Ph.D., and Hiroaki Taguchi, Ph.D., both with the Department of Pathology and Laboratory Medicine, and Miguel Escobar, M.D., of the Department of Pediatrics. Maria Salas and Hanson, both with the Viral and Rickettsial Disease Laboratory, contributed.

The journal article is titled "Catalytic antibodies to HIV: Physiological role and potential clinical utility". The research was funded by the National Institutes of Health and the Texas Higher Education Coordinating Board.

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Admiral Valdemar
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Post by Admiral Valdemar »

I could probably dig up papers from the late eighties, early nineties with similar "breakthrough" titles. While I'm cautiously optimistic, if you believe even half of these headlines, then you'd start to question why we still die at all, let alone suffer disease.
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Post by Justforfun000 »

I could probably dig up papers from the late eighties, early nineties with similar "breakthrough" titles. While I'm cautiously optimistic, if you believe even half of these headlines, then you'd start to question why we still die at all, let alone suffer disease.
Well, this is true. However discovering a part of the virus that does not ever mutate is a very promising path to go down. That's been the singular main reason we haven't had any success at curing or preventing this disease. Everything has been targeting mutable portions of the virus. Hopefully they can target this newly discovered weakness.
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Post by Admiral Valdemar »

I think the other thread, with that "suntanning" technique, sounds more promising in the immediate term. A big part of my work is moving into biologics now, where the use of smart molecules is preferred over standard compounds for inhibition etc. The best way to deal with this kind of threat is to bolster the body's own, already advanced defences in such a way that they can matter, which we all know HIV cleverly targets beforehand.
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Justforfun000
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Post by Justforfun000 »

Yes I thought that too. It's already on the way to practical treatment and as you said, our best hope at the moment is boosting our own immune system.

This almost sounds similar to a method of alternative treatment where they heated the blood outside the body to a very high level and put it back in you under the basis of the virus being killed at a high enough level of heat. Supposedly though it didn't pan out in the long run, so this new innovation is exciting.
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Alyrium Denryle
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Post by Alyrium Denryle »

Justforfun000 wrote:Yes I thought that too. It's already on the way to practical treatment and as you said, our best hope at the moment is boosting our own immune system.

This almost sounds similar to a method of alternative treatment where they heated the blood outside the body to a very high level and put it back in you under the basis of the virus being killed at a high enough level of heat. Supposedly though it didn't pan out in the long run, so this new innovation is exciting.
HIV is really really fragile. I dont know what intensity the UV they use in the other one is, but one idea would be to put HIV patients on a a heart/lung machine, and as the blood is being circulated, bath ever ml of it in UV.

The downside to that is of course damage to the blood.... but if the intensity is low enough you could attenuate the HIV without significant damage to your blood cells, which have high turnover rates away....

Bear in mind, I work with evolutionary questions, I dont know if that is possible....
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Max
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Post by Max »

Even if you could 'suntan' the blood cells, isn't HIV found in other, non-blood cells? I may be missing something obvious, so forgive me in advance..
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Admiral Valdemar
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Post by Admiral Valdemar »

Max wrote:Even if you could 'suntan' the blood cells, isn't HIV found in other, non-blood cells? I may be missing something obvious, so forgive me in advance..
It is, but this is just to keep the virus particle count down.

Incidentally, one of the drug trials has been cancelled, as per the NYT today, due to insufficient data.
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