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3ggu is a drug resistant HIV protease. Shown is a patient's variant in complex with darunavir.
3ggu is a drug resistant HIV protease. Shown is a patient's variant in complex with darunavir.
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HIV proteases are essential for the functioning of the retrovirus that causes AIDS. HIV needs active proteases to process Gag & Gap - Polymerase polyprotein precursors into mature structural proteins and replicative enzymes.
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HIV proteases(PR) are essential for the functioning of the retrovirus that causes AIDS. HIV needs active proteases to process Gag & Gap - Polymerase polyprotein precursors into mature structural proteins and replicative enzymes.
HIV proteases contain a highly conserved region Asp - Thr - Gly (Asp25, Thr26 and Gly27), with the aspartic residue beeing the active site in the aspartyl protease.[[(1)]]
HIV proteases contain a highly conserved region Asp - Thr - Gly (Asp25, Thr26 and Gly27), with the aspartic residue beeing the active site in the aspartyl protease.[[(1)]]
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Because of its importance for the life-cycle of the retrovirus, HIV-PR are the major target for anit-HIV treatment.
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HIV protease inhibitors are the most potent agens used in anti-HIV treatment. However it occurs that HIV PR develops a resistance to the inhibitor. [[(2)]]
== '''Activity''' ==
== '''Activity''' ==

Revision as of 12:32, 27 December 2012

Template:Sandbox ESBS 2012

3ggu

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Contents

Description

3ggu is a drug resistant HIV protease. Shown is a patient's variant in complex with darunavir.

HIV proteases(PR) are essential for the functioning of the retrovirus that causes AIDS. HIV needs active proteases to process Gag & Gap - Polymerase polyprotein precursors into mature structural proteins and replicative enzymes. HIV proteases contain a highly conserved region Asp - Thr - Gly (Asp25, Thr26 and Gly27), with the aspartic residue beeing the active site in the aspartyl protease.(1) Because of its importance for the life-cycle of the retrovirus, HIV-PR are the major target for anit-HIV treatment. HIV protease inhibitors are the most potent agens used in anti-HIV treatment. However it occurs that HIV PR develops a resistance to the inhibitor. (2)

Activity

Structure

Applications

External Resources

References

(1) Kohl, N. E., E. A. Emini, W. A. Schleif, L. J. Davis, J. C. Heimbach, R. A. F. Dixon, E. M. Scolnick, and I. S. Sigal. 1988. Active human immunodeficiency virus protease is required for viral infectivity. Proc. Natl. Acad. Sci. USA 85:4686-4690.

Contributors

Julia Baaske, Angelika Wackerl

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