Virus Dataset Sample Info

> Dataset: 32434561 Search Result


Summary
Item Summary
Project 32434561
Virus Name HIV
Sample Number 27
Disease AIDS/HIV
Country Malawi

Sample
ID Sample ID Age Gender Origin Detail
1 36 F Malawi View
2 41 F Malawi View
3 25 F Malawi View
4 46 F Malawi View
5 42 M Malawi View
6 36 F Malawi View
7 32 F Malawi View
8 51 M Malawi View
9 33 F Malawi View
10 42 M Malawi View
11 60 M Malawi View
12 31 M Malawi View
13 32 F Malawi View
14 25 F Malawi View
15 23 F Malawi View
16 40 F Malawi View
17 29 F Malawi View
18 34 F Malawi View
19 22 F Malawi View
20 28 F Malawi View
21 30 M Malawi View
22 29 F Malawi View
23 25 F Malawi View
24 26 F Malawi View
25 43 M Malawi View
26 28 F Malawi View
27 45 F Malawi View

Literature
Item Summary
PMID 32434561
Title Pretreatment resistance mutations and treatment outcomes in adults living with HIV-1: a cohort study in urban Malawi.
Abstract BACKGROUND: Pre-treatment drug resistance (PDR) among antiretroviral drug-naive people living with HIV (PLHIV) represents an important indicator for the risk of treatment failure and the spread of drug resistant HIV variants. We assessed the prevalence of PDR and treatment outcomes among adults living with HIV-1 in Lilongwe, Malawi. METHODS: We selected 200 participants at random from the Lighthouse Tenofovir Cohort Study (LighTen). Serum samples were drawn prior to treatment initiation in 2014 and 2015, frozen, and later analyzed for the presence of HIV-1 drug resistance mutations. Amplicons were sequenced and interpreted by Stanford HIVdb interpretation algorithm 8.4. We assessed treatment outcomes by evaluating clinical outcome and viral suppression at the end of the follow-up period in October 2019. RESULTS: PDR testing was successful in 197 of 200 samples. The overall NNRTI- PDR prevalence was 13.7% (27/197). The prevalence of intermediate or high level NNRTI- PDR was 11.2% (22/197). The most common mutation was K103N (5.6%, 11/197), followed by Y181C (3.6%, 7/197). In one case, we detected an NRTI resistance mutation (M184V), in combination with multiple NNRTI resistance mutations. All HIV-1 isolates analyzed were of subtype C. Of the 27 patients with NNRTI- PDR, 9 were still alive, on ART, and virally suppressed at the end of follow-up. CONCLUSION: The prevalence of NNRTI- PDR was above the critical level of 10% suggested by the Global Action Plan on HIV Drug Resistance. The distribution of drug resistance mutations was similar to that seen in previous studies from the region, and further supports the introduction of integrase inhibitors in first-line treatment in Malawi. Furthermore, our findings underline the need for continued PDR surveillance and pharmacovigilance in Sub-Saharan Africa.