HIV mutation literature information.


  Management of a human immunodeficiency virus case with discordant antiviral drug resistance profiles in cerebrospinal fluid compared with plasma: a case report.
 PMID: 35164871       2022       Journal of medical case reports
Conclusion: During subsequent years, the plasma resistance pattern reverted to susceptible for the NRTI/NNRTIs; however the PI mutation L89V appeared, only later to revert to fully susceptible again.
Conclusion: The PI L89V mutation may contribute to reduced PI susceptibility.


  Detection of Gag C-terminal mutations among HIV-1 non-B subtypes in a subset of Cameroonian patients.
 PMID: 35082353       2022       Scientific reports
Introduction: Following the Stanford algorithm (mutation list), minor resistance mutations (L10F, V11I, K20TV, L23I, L33F, K43T, F53L, Q58E, A71IL, G73STCA, T74P, N83D, and L89V) are assumed to have ancillary roles such as compensation for lower efficiency of proteolysis caused by major mutations; major resistance mutations (V32I, M46IL, I47VA, G48VM,  PMID: 35061671       2022       PloS one
Table: L89V


  Temporal Trends in HIV-1 Mutations Used for the Surveillance of Transmitted Drug Resistance.
 PMID: 34064774       2021       Viruses
Abstract: Three candidate PI-SDRMs were accessory darunavir-resistance mutations (L10F, T74P, L89V).
Result: T74P and L89V were considered to be accessory mutations based on analyses of phenotypic and clinical data derived from the POWER studies that led the FDA approval of darunavir.
Result: Figure 3 shows the locations of the PI-SDRMs and the three candidate mutations (L10F, T74P, and L89V) within the three-dimensional structure of HIV-1 protease.


  Genotyping and antiretroviral drug resistance of human immunodeficiency Virus-1 in Jazan, Saudi Arabia.
 PMID: 33285702       2020       Medicine
Abstract: Mutations associated with antiretroviral drugs include (V82A+I84IV), (L10F+Q58E), (L10F+V82Y), L10FV, L33LF, L89LMV, M184V, E138A, V106I, and V179VD.
Result: Among the observed resistance mutations, 4/57 (7.0%) had conferring resistance to PI, other detected mutations were (L10F + V82Y), L10FV, L33LF, and  PMID: 32119691       2020       PloS one
Table: L89V


  Molecular Determinants of Epistasis in HIV-1 Protease: Elucidating the Interdependence of L89V and L90M Mutations in Resistance.
 PMID: 31386353       2019       Biochemistry
1Abstract: The focus of our investigation is a patient-derived isolate, with 24 mutations that we call ""KY""; this variant includes the L89V and L90M mutations."
Abstract: In this study, we investigated the interdependence between the L89V and L90M mutations and their effects on DRV binding.
Abstract: When a leucine to valine mutation at residue 89 is present simultaneously with the L90M mutation, a rescue of catalytic efficiency is observed.


  Mechanism of Darunavir (DRV)'s High Genetic Barrier to HIV-1 Resistance: A Key V32I Substitution in Protease Rarely Occurs, but Once It Occurs, It Predisposes HIV-1 To Develop DRV Resistance.
 PMID: 29511083       2018       mBio
Discussion: reported that 11 amino acid substitutions, V11I, V32I, L33F, I47V, I50V, I54L/M, G73S, L76V, I84V, and L89V, which appear to be associated with HIV-1 resistance against DRV, were identified among HIV-1 variants isolated from patients treated with DRV-including regimens on POWER studies.


  Emergence of HIV-1 drug resistance mutations in mothers on treatment with a history of prophylaxis in Ghana.
 PMID: 30223845       2018       Virology journal
Result: The major DRAMs to PIs seen in the group was I84V; the minor drug resistance mutations seen were A71V, L89 V and M46MV.


  Next generation sequencing of HIV-1 protease in the PIVOT trial of protease inhibitor monotherapy.
 PMID: 29428459       2018       Journal of clinical virology
Abstract: NGS revealed previously unidentified minority variant protease mutations (G73D, I54T, L89V) in three samples, at frequencies ranging between 2% and 10%.
Result: The L89V mutation (frequency 5%), which predicts resistance to fosamprenavir, was detected at 41 weeks in patient C.
Table: L89V



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