literature

HIV mutation literature information.

HIV-genetic diversity and drug resistance transmission clusters in Gondar, Northern Ethiopia, 2003-2013.

PMID: 30304061 2018 PloS one

Result: Taken together, the G190A/S/E mutations were most prominent (seven of the 12 NNRTI mutations), followed by the K103N, Y181I/C and K101E substitutions (two, two and one, respectively).

Result: Two had K103N, one G190S and one Y181C, all representing resistance to non-nucleoside reverse transcriptase inhibitors (NNRTI).

Table: Y181C

Discussion: The specific NNRTI associated mutations found in this study (K103N, G109S and

PMID: 30314470 2018 BMC infectious diseases

Discussion: However, some studies have shown that NVP-containing ARVs have repercussions on the response to etravirine for selecting the Y181C and G190A mutations, whereas the K103 mutation associated with EFV does not interfere with etravirine susceptibility.

Research on the treatment effects and drug resistances of long-term second-line antiretroviral therapy among HIV-infected patients from Henan Province in China.

PMID: 30442114 2018 BMC infectious diseases

Table: Y181C

Long-term virological outcome in children receiving first-line antiretroviral therapy.

PMID: 30477526 2018 AIDS research and therapy

Abstract: At the time of virologic failure, multiple NNRTI-associated mutations were observed: 80%-K103N and Y181C being the major NNRTI mutations-observed.

Result: K103N (48%), Y181C (37%), G190A/S (25%), Y188C/L (10%), V106M/A (8%), K65R (8%) and L100I (4%) were the major NNRTI DRMs observed in these 52 childre

Discussion: Among those who developed VF, M184V, K103N, and Y181C were the most common DRMs observed as in South Africa.

HIV-1 subtype diversity, transmission networks and transmitted drug resistance amongst acute and early infected MSM populations from Coastal Kenya.

PMID: 30562356 2018 PloS one

Result: One volunteer had dual-class NRTI (M184V) and NNRTI (Y181C) resistance mutations.

Table: Y181C

Recent trends and patterns in HIV-1 transmitted drug resistance in the United Kingdom.

PMID: 27476929 2017 HIV medicine

Result: The most frequently detected mutations were T215 revertants (not F/Y) (268; 1.6%) and other TAMs [M41L (141; 0.9%) and K219Q/N (104; 0.6%)] conferring resistance to the NRTI drug class; K103N (354; 2.2%) and Y181C (66; 0.4%) conferring resistance to the NNRTI drug class, and L90M (111; 0.7%) and M46L (48; 0.3%) conferring resistance to the PI drug class.

Surveillance of Transmitted Drug Resistance in HIV-1-Infected Youths Aged 16 to 25 Years, a Decade After Scale-up of Antiretroviral Therapy in Hebei, China.

PMID: 27750023 2017 AIDS research and human retroviruses

Abstract: All TDR mutations (M46L/I, Y181C, K101E, and G190E) were found only in youths infected with HIV-1 through sexual activity.

Abstract: TDR mutations resided in CRF01_AE (M46I/L and G190E) and subtype B (Y181C and K101E).

Discovery of novel piperidine-substituted indolylarylsulfones as potent HIV NNRTIs via structure-guided scaffold morphing and fragment rearrangement.

PMID: 27750153 2017 European journal of medicinal chemistry

Abstract: Furthermore, most compounds maintained high activity agaist various single HIV-1 mutants (L100I, K103N, E138K, Y181C) as well as one double mutant (F227L/V106A) with EC50 values in low-micromolar to double-digit nanomolar concentration ranges.

Rapid Detection of Common HIV-1 Drug Resistance Mutations by Use of High-Resolution Melting Analysis and Unlabeled Probes.

PMID: 27795333 2017 Journal of clinical microbiology

Abstract: The analytical sensitivities of the HRMA assays were 5% of mixed species for K103N and Y181C and 20% for M184V.

Abstract: When applied to 153 HIV-1 patient specimens previously genotyped by Sanger population sequencing, HRMA correctly assigned drug sensitivity or resistance profiles to 80% of the samples at codon 103 (K103K/N) (Cohen's kappa coefficient [kappa] > 0.6; P < 0.05), 90% at 181 (Y181Y/C) (kappa > 0.74, P < 0.05), and 80% at 184 (M184M/V) (kappa > 0.62; P < 0.05).

Use of Capillary Electrophoresis to Study the Binding Interaction of Aptamers with Wild-Type, K103N, and Double Mutant (K103N/Y181C) HIV-1 RT : Studying the Binding Interaction of Wild-Type, K103N, and Double Mutant (K103N/Y181C) HIV-1 RT with Aptamers by Performing the Capillary Electrophoresis.

PMID: 27900665 2017 Applied biochemistry and biotechnology

Abstract: Therefore, we utilized non-equilibrium capillary electrophoresis of equilibrium mixture (NECEEM) to study the interaction of three HIV-1 RTs (wild type, K103N, and double mutant (K103N/Y181C)) with RT1t49 and RT12 aptamers.

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