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Structurally sound: The neuraminidase protein of the H1N1 virus is particularly adept at mutating to avoid attack. In this crystal structure, the mutations that allow it to resist Tamiflu and other antiviral drugs are visible as multicolored stick structures.
Daniel Dadon and Jacob Durrant
Fragments of known drugs could lead to a more robust antiviral for H1N1 and other flu variants.
The flu virus is a wily target, constantly mutating to avoid attack from the immune system and from antiviral drugs like Tamiflu. But in research presented Sunday at the annual meeting of the American Society for Cell Biology (ASCB) in San Diego, scientists announced a new method for fighting pandemic influenzas such as H1N1 (swine) and H5N1 (avian).
The approach involves using massive amount of computer power to simulate never-before-seen conformations of a virus. Using the method, researchers at the University of California at San Diego have not only identified a new molecular target for influenza drugs, they have also found drugs already approved by the U.S. Food and Drug Administration that just might hit the target perfectly.
The target in question is a single, large protein called neuraminidase--one of two major proteins present on the surface of the influenza virus--that allows newly replicated viruses to be released into their host. Because most pandemic versions share the same neuraminidase subtype, N1, the protein is an ideal drug target.
Most molecular imaging or modeling focuses on determining the arrangement of atoms in a molecule's crystal structure--a lengthy, energy-intensive process that provides a precise way to capture the molecule's shape but only in one conformation, frozen at a single moment in time. In contrast, the new "relaxed complex" method models the virus protein molecule in a state that provides a better understanding of how the protein behaves and even revealing conformations that rarely occur.
Biochemist Andrew McCammon and undergraduate lab member Daniel Dadon used a sophisticated computer program to simulate all possible conformations--27 in all--of the H1N1 virus's flexible neuraminidase protein. Rather than forcing the protein into a single crystal structure's conformation, "[we] got a movie of how the protein would behave in nature," Dadon says. "It's like frames from a film, rather than a single photograph."
Dadon aligned each of those 27 neuraminidase conformations and found that all of them had a binding site that remained unchanged, a single spot that could act as a prime inhibitor target. The researchers then looked at a library of drugs already approved by the FDA. After breaking molecular models of the drugs down into small fragments, they ran them through a colossal search algorithm in order to find those molecules with the highest affinity for the neuraminidase binding site.
What about Internet and sharing information/ideas over it? Or simple search? Could you imagine finding latest information on recent discoveries of lets say "Toll-like receptor 8"? Without computers you would need to physically go library and manually search hundreds published peer review journals, handling thousands of issues. What if you 5 minutes after you finished your search decided to look for "Toll-like receptor 9" info?
What about CG? Shrek, Bolt, Avatar etc. and so on. You think art, in particular computer graphic do not affect our life too?
Did they actually test the affinity or was this all computational? This article is devoid of details.
Manufacturing in the United States is in trouble. That's bad news not just for the country's economy but for the future of innovation.
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Computers
As a computer programmer for 38 years I have lately come to wonder how much they have really helped our lives. The invention certainly hasn't lead to reduction in work hours despite the claim that computers increase productivity. It is fair to say that they have vastly increased computer-centric activity.
It is inspiring to see computers put to use this way. The value of computers in defending us against disease just might be where they actually pay off.
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