Jessica D. Church scite author profile

Background Single dose (SD) nevirapine (NVP) at birth plus NVP to the infant up to 6 weeks of age is superior to SD NVP alone for prevention of HIV vertical transmission through breastfeeding. We analyzed NVP resistance in HIV-infected Ugandan infants who received either SD NVP or extended NVP prophylaxis. Methods We tested plasma HIV using a genotyping assay (ViroSeq), a phenotypic resistance assay (PhenoSense), and sensitive point mutation assay (LigAmp, for K103N, Y181C, G190A). Results At 6 weeks, NVP resistance was detected by ViroSeq in a higher proportion of infants in the extended NVP arm than in the SD NVP arm (21/25=84% vs. 12/24=50%, p=0.01). Similar results were obtained with LigAmp and PhenoSense. Infants who were HIV-infected at birth had high rates of resistance in both study arms. In contrast, infants who were HIV-infected after birth were more likely to have resistance detected at 6 weeks in the extended NVP arm. Use of extended NVP prophylaxis was also associated with detection of NVP resistance by ViroSeq at 6 months (7/7=100% extended NVP arm vs. 1/6=16.7% SD NVP arm, p=0.005). Conclusions Use of extended NVP prophylaxis was associated with increased selection and persistence of NVP resistance in HIV-infected Ugandan infants.

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Quantitative Analysis of HIV-1 Variants With the K103N Resistance Mutation After Single-Dose Nevirapine in Women With HIV-1 Subtypes A, C, and D

Flys

Chen

Jones

et al. 2006

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Sensitivity of the ViroSeq HIV-1 Genotyping System for Detection of the K103N Resistance Mutation in HIV-1 Subtypes A, C, and D

Church¹,

Jones²,

Flys³

et al. 2006

The Journal of Molecular Diagnostics

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The US Food and Drug Administration-cleared ViroSeq HIV-1 Genotyping System (ViroSeq) and other population sequencing-based human immunodeficiency virus type 1 (HIV-1) genotyping methods detect antiretroviral drug resistance mutations present in the major viral population of a test sample. These assays also detect some mutations in viral variants that are present as mixtures. We compared detection of the K103N nevirapine resistance mutation using The US Food and Drug Administration-cleared ViroSeq HIV-1 Genotyping System (ViroSeq) and other population sequencing-based genotyping methods detect mutations present in the major viral population in a test sample. These assays also detect some mutations that are present at lower levels. Using recombinant viral stocks, we previously demonstrated that ViroSeq reliably detects drug resistance mutations present in 40% of the viral population in samples with viral loads from 2000 to 5000 copies/ml 1 , lower level mixtures were not evaluated in that study. In another study, ViroSeq detected the K103N mutation in a recombinant human immunodeficiency virus type 1 (HIV-1) strain at a level of 10%. 2HIV-1 variants with the K103N mutation are often selected in women who receive a single dose of the antiretroviral drug nevirapine for prevention of HIV-1 motherto-child transmission. 3,4 We evaluated the sensitivity of ViroSeq for detection of K103N in 305 clinical plasma samples collected from African women 6 to 8 weeks after single dose nevirapine administration. Samples were collected from women in the HIV Network for Prevention Trial (HIVNET) 012 trial 5,6 (Ugandan women, 146 subtype A samples and 95 subtype D samples) and the Nevirapine-

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HIV‐1 Tropism and Survival in Vertically Infected Ugandan Infants

Church

Huang²,

Mwatha

et al. 2008

J INFECT DIS

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Nevirapine Resistance in Women and Infants after First versus Repeated Use of Single‐Dose Nevirapine for Prevention of HIV‐1 Vertical Transmission

Flys

McConnell²,

Matovu

et al. 2008

J INFECT DIS

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Single dose (SD) nevirapine (NVP) significantly reduces HIV mother-to-child transmission. We analyzed NVP resistance after SD NVP in 57 previously SD NVP-naїve women, 34 SD NVP-experienced women, and 17 HIV-infected infants. The proportion of women with resistance, the types of mutations detected, and the frequency and level of K103N were similar in the two groups of women at 6 weeks and 6 months post-partum. NVP resistance was detected in a similar proportion of infants born to SD NVP-naїve versus SD NVP-experienced women. Repeated use of SD NVP to prevent HIV transmission does not appear to influence NVP resistance.

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Jessica D. Church

Analysis of Nevirapine (NVP) Resistance in Ugandan Infants Who Were HIV Infected Despite Receiving Single-Dose (SD) NVP versus SD NVP Plus Daily NVP Up to 6 Weeks of Age to Prevent HIV Vertical Transmission

Quantitative Analysis of HIV-1 Variants With the K103N Resistance Mutation After Single-Dose Nevirapine in Women With HIV-1 Subtypes A, C, and D

Sensitivity of the ViroSeq HIV-1 Genotyping System for Detection of the K103N Resistance Mutation in HIV-1 Subtypes A, C, and D

HIV‐1 Tropism and Survival in Vertically Infected Ugandan Infants

Nevirapine Resistance in Women and Infants after First versus Repeated Use of Single‐Dose Nevirapine for Prevention of HIV‐1 Vertical Transmission

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