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home :: AIDS :: Closing_of_the_Flaps.txt

Wed, 24 May 2006


Closing of the Flaps of HIV-1 Protease Induced by Substrate Binding: A Model of a Flap Closing Mechanism in Retroviral Aspartic Proteases.

Biochemistry 2006 May 30; 45(21): 6606-14 (Read article online)
Tóth G, Borics A

The active site of aspartic proteases is covered by one or more flaps, which control access to the active site and play a significant role in the binding of the substrate. An extensive conformational change of the flaps takes place upon binding of substrate to the active site. A long molecular dynamics simulation was performed on the complex consisting of a peptide (CA-p2) from a natural substrate cleavage site of the gag/pol polyprotein placed in the active site of HIV-1 protease (PR) with an open flap conformation. During the simulation, the substrate induced the closing of the flaps into the closed conformation in an asymmetrical way through a hydrophobic intermediate state cluster. The nature of the residues of HIV-1 PR identified to be important in the flap closing mechanism is conserved across known structures of retroviral aspartic proteases family. The flap closing mechanism described in HIV-1 PR is proposed to be a general model for flap closing in retroviral aspartic proteases.

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