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    Eur J Biochem. 2004 Apr;271(8):1516-24.

    Crystal structures of HIV protease V82A and L90M mutants reveal changes in the indinavir-binding site.

    Mahalingam B, Wang YF, Boross PI, Tozser J, Louis JM, Harrison RW, Weber IT.

    Department of Biology, Georgia State University, PO Box 4010, Atlanta, GA 30302-4010, USA.

    The crystal structures of the wild-type HIV-1 protease (PR) and the two resistant variants, PR(V82A) and PR(L90M), have been determined in complex with the antiviral drug, indinavir, to gain insight into the molecular basis of drug resistance. V82A and L90M correspond to an active site mutation and nonactive site mutation, respectively. The inhibition (K(i)) of PR(V82A) and PR(L90M) was 3.3- and 0.16-fold, respectively, relative to the value for PR. They showed only a modest decrease, of 10-15%, in their k(cat)/K(m) values relative to PR. The crystal structures were refined to resolutions of 1.25-1.4 A to reveal critical features associated with inhibitor resistance. PR(V82A) showed local changes in residues 81-82 at the site of the mutation, while PR(L90M) showed local changes near Met90 and an additional interaction with indinavir. These structural differences concur with the kinetic data.

    PMID: 15066177 [PubMed - indexed for MEDLINE]

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    • Indinavir (Crixivan®)

      Indinavir is used to treat human immunodeficiency virus (HIV) infection in adults. It belongs to a class of drugs called protease inhibitors, which slow the spread of HIV infection in the body. It is usually taken with o...

    • Source: AHFS Consumer Medication Information

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