Literature DB >> 18560011

Enzymatic and structural analysis of the I47A mutation contributing to the reduced susceptibility to HIV protease inhibitor lopinavir.

Klára Grantz Sasková1, Milan Kozísek, Martin Lepsík, Jirí Brynda, Pavlína Rezácová, Jana Václavíková, Ron M Kagan, Ladislav Machala, Jan Konvalinka.   

Abstract

Lopinavir (LPV) is a second-generation HIV protease inhibitor (PI) designed to overcome resistance development in patients undergoing long-term antiviral therapy. The mutation of isoleucine at position 47 of the HIV protease (PR) to alanine is associated with a high level of resistance to LPV. In this study, we show that recombinant PR containing a single I47A substitution has the inhibition constant (K(i) ) value for lopinavir by two orders of magnitude higher than for the wild-type PR. The addition of the I47A substitution to the background of a multiply mutated PR species from an AIDS patient showed a three-order-of-magnitude increase in K(i) in vitro relative to the patient PR without the I47A mutation. The crystal structure of I47A PR in complex with LPV showed the loss of van der Waals interactions in the S2/S2' subsites. This is caused by the loss of three side-chain methyl groups due to the I47A substitution and by structural changes in the A47 main chain that lead to structural changes in the flap antiparallel beta-strand. Furthermore, we analyzed possible interaction of the I47A mutation with secondary mutations V32I and I54V. We show that both mutations in combination with I47A synergistically increase the relative resistance to LPV in vitro. The crystal structure of the I47A/I54V PR double mutant in complex with LPV shows that the I54V mutation leads to a compaction of the flap, and molecular modeling suggests that the introduction of the I54V mutation indirectly affects the strain of the bound inhibitor in the PR binding cleft.

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Year:  2008        PMID: 18560011      PMCID: PMC2525523          DOI: 10.1110/ps.036079.108

Source DB:  PubMed          Journal:  Protein Sci        ISSN: 0961-8368            Impact factor:   6.725


  46 in total

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Authors:  Jirí Brynda; Pavlína Rezácová; Milan Fábry; Magdalena Horejsí; Renata Stouracová; Milan Soucek; Martin Hradílek; Jan Konvalinka; Juraj Sedlácek
Journal:  Acta Crystallogr D Biol Crystallogr       Date:  2004-10-20

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7.  Structural analysis of an HIV-1 protease I47A mutant resistant to the protease inhibitor lopinavir.

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Journal:  Protein Sci       Date:  2005-06-03       Impact factor: 6.725

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2.  Crystallographic study of multi-drug resistant HIV-1 protease lopinavir complex: mechanism of drug recognition and resistance.

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3.  Molecular characterization of clinical isolates of human immunodeficiency virus resistant to the protease inhibitor darunavir.

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8.  Prediction and molecular field view of drug resistance in HIV-1 protease mutants.

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9.  Drug resistance conferred by mutations outside the active site through alterations in the dynamic and structural ensemble of HIV-1 protease.

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10.  Acquired HIV-1 Protease Conformational Flexibility Associated with Lopinavir Failure May Shape the Outcome of Darunavir Therapy after Antiretroviral Therapy Switch.

Authors:  Simeon Eche; Ajit Kumar; Nelson Sonela; Michelle L Gordon
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