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

Su, Chinh Tran-To; Koh, Darius Wen‐Shuo; Gan, Samuel Ken‐En

doi:10.3390/molecules24183243

Cited by 17 publications

(20 citation statements)

References 93 publications

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“…For a better study of HIV-1 RT, the mutation positions are important to provide mechanistic insights to the development of drug resistance [76]. The well-established mutation rate of HIV-1 RT is performed on lacZα [39][40][41][42][43][44][45]48,58,77], resulting in a gap of knowledge regarding how HIV-1 genes are mutated by RT.…”

Section: Studies On Hiv-1 Genesmentioning

confidence: 99%

“…For example, the M184V resistance mutation in HIV-1 RT is known to increase fidelity, impair viral fitness, and increase hyper-sensitization to NRTIs (such as amprenavir and efavirenz) [99]. Thus, it is possible to leverage on such features alongside structural understanding [76] to utilize combinatorial therapies to target the active site, using existing inhibitors to select for the mutation alongside other inhibitors to limit the escape mutations.…”

Section: Implications On Sagacious Drug Designmentioning

confidence: 99%

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The Determination of HIV-1 RT Mutation Rate, Its Possible Allosteric Effects, and Its Implications on Drug Resistance

Yeo

Goh

et al. 2020

Viruses

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The high mutation rate of the human immunodeficiency virus type 1 (HIV-1) plays a major role in treatment resistance, from the development of vaccines to therapeutic drugs. In addressing the crux of the issue, various attempts to estimate the mutation rate of HIV-1 resulted in a large range of 10−5–10−3 errors/bp/cycle due to the use of different types of investigation methods. In this review, we discuss the different assay methods, their findings on the mutation rates of HIV-1 and how the locations of mutations can be further analyzed for their allosteric effects to allow for new inhibitor designs. Given that HIV is one of the fastest mutating viruses, it serves as a good model for the comprehensive study of viral mutations that can give rise to a more horizontal understanding towards overall viral drug resistance as well as emerging viral diseases.

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Section: Studies On Hiv-1 Genesmentioning

confidence: 99%

Section: Implications On Sagacious Drug Designmentioning

confidence: 99%

The Determination of HIV-1 RT Mutation Rate, Its Possible Allosteric Effects, and Its Implications on Drug Resistance

Yeo

Goh

et al. 2020

Viruses

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“…A number of studies have attempted to establish Gag as a target. The design and development of drugs that target Gag could be approached in four broad ways, as reviewed by Su and colleagues ( 41 ). The first approach would involve screening and targeting of druggable allosteric sites present in Gag.…”

Section: Discussionmentioning

confidence: 99%

“…The third approach is the use of synergistic drugs to target multiple sites by chemically joining different potential Gag inhibitors to function as dual or triple inhibitors. The fourth approach is to design inhibitors to disrupt the conformational transition of Gag during viral maturation ( 41 ).…”

Section: Discussionmentioning

confidence: 99%

“…The use of a small-molecule approach was also adopted by Machara et al and led to the identification of two arylquinazolines which inhibited HIV-1 capsid assembly by binding to the C-terminal domain of capsid and blocking viral replication ( 44 ). Additionally, inhibitors could be synthesized to destabilize Gag assembly, thus slowing the viral maturation process ( 41 ).…”

Section: Discussionmentioning

confidence: 99%

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In Vivo Emergence of a Novel Protease Inhibitor Resistance Signature in HIV-1 Matrix

Datir

Kemp

Bouzidi

et al. 2020

mBio

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Protease inhibitors (PIs) are the second- and last-line therapy for the majority of HIV-infected patients worldwide. Only around 20% of individuals who fail PI regimens develop major resistance mutations in protease. We sought to explore the role of mutations in gag-pro genotypic and phenotypic changes in viruses from six Nigerian patients who failed PI-based regimens without known drug resistance-associated protease mutations in order to identify novel determinants of PI resistance. Target enrichment and next-generation sequencing (NGS) with the Illumina MiSeq system were followed by haplotype reconstruction. Full-length Gag-protease gene regions were amplified from baseline (pre-PI) and virologic failure (VF) samples, sequenced, and used to construct gag-pro-pseudotyped viruses. Phylogenetic analysis was performed using maximum-likelihood methods. Susceptibility to lopinavir (LPV) and darunavir (DRV) was measured using a single-cycle replication assay. Western blotting was used to analyze Gag cleavage. In one of six participants (subtype CRF02_AG), we found 4-fold-lower LPV susceptibility in viral clones during failure of second-line treatment. A combination of four mutations (S126del, H127del, T122A, and G123E) in the p17 matrix of baseline virus generated a similar 4-fold decrease in susceptibility to LPV but not darunavir. These four amino acid changes were also able to confer LPV resistance to a subtype B Gag-protease backbone. Western blotting demonstrated significant Gag cleavage differences between sensitive and resistant isolates in the presence of drug. Resistant viruses had around 2-fold-lower infectivity than sensitive clones in the absence of drug. NGS combined with haplotype reconstruction revealed that resistant, less fit clones emerged from a minority population at baseline and thereafter persisted alongside sensitive fitter viruses. We used a multipronged genotypic and phenotypic approach to document emergence and temporal dynamics of a novel protease inhibitor resistance signature in HIV-1 matrix, revealing the interplay between Gag-associated resistance and fitness.

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The impact of Gag non-cleavage site mutations on HIV-1 viral fitness from integrative modelling and simulations

Samsudin

Gan

Bond

2021

Computational and Structural Biotechnology Journal

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

Cited by 17 publications

References 93 publications

The Determination of HIV-1 RT Mutation Rate, Its Possible Allosteric Effects, and Its Implications on Drug Resistance

The Determination of HIV-1 RT Mutation Rate, Its Possible Allosteric Effects, and Its Implications on Drug Resistance

In Vivo Emergence of a Novel Protease Inhibitor Resistance Signature in HIV-1 Matrix

The impact of Gag non-cleavage site mutations on HIV-1 viral fitness from integrative modelling and simulations

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