Reviewing HIV-1 Gag Mutations in Protease Inhibitors Resistance: Insights for Possible Novel Gag Inhibitor Designs

被引:15
|
作者
Su, Chinh Tran-To [1 ]
Koh, Darius Wen-Shuo [1 ]
Gan, Samuel Ken-En [1 ,2 ]
机构
[1] ASTAR, Antibody & Prod Dev Lab, Bioinformat Inst, Singapore 138671, Singapore
[2] ASTAR, P53 Lab, Singapore 138648, Singapore
来源
MOLECULES | 2019年 / 24卷 / 18期
关键词
HIV-1; Gag; Gag inhibitors; protease; protease inhibitors; drug resistance mutations; drug design; AMINO-ACID SUBSTITUTIONS; VIRUS TYPE-1 GAG; DRUG-RESISTANCE; CLEAVAGE SITES; MATURATION INHIBITOR; HIGH PREVALENCE; VIRAL FITNESS; BEVIRIMAT; POLYMORPHISMS; MUTANTS;
D O I
10.3390/molecules24183243
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
HIV protease inhibitors against the viral protease are often hampered by drug resistance mutations in protease and in the viral substrate Gag. To overcome this drug resistance and inhibit viral maturation, targeting Gag alongside protease rather than targeting protease alone may be more efficient. In order to successfully inhibit Gag, understanding of its drug resistance mutations and the elicited structural changes on protease binding needs to be investigated. While mutations on Gag have already been mapped to protease inhibitor resistance, there remain many mutations, particularly the non-cleavage mutations, that are not characterized. Through structural studies to unravel how Gag mutations contributes to protease drug resistance synergistically, it is thus possible to glean insights to design novel Gag inhibitors. In this review, we discuss the structural role of both novel and previously reported Gag mutations in PI resistance, and how new Gag inhibitors can be designed.
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页数:13
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