Your search keyword '"Parikh, Urvi M."' showing total 4 results

1. HIV-1 drug resistance among individuals who seroconverted in the ASPIRE dapivirine ring trial

Author

Parikh, Urvi M., Penrose, Kerri J., Heaps, Amy L., Halvas, Elias K., Goetz, B.Jay, Gordon, Kelley C., Hardesty, Russell, Sethi, Rahil, Schwarzmann, William, Szydlo, Daniel W., Husnik, Marla J., Chandran, Uma, Palanee-Phillips, Thesla, Baeten, Jared M., and Mellors, John W.

Subjects

Gene mutations -- Health aspects, Serology, Antiviral agents -- Testing, Drug resistance -- Genetic aspects, Anti-HIV agents -- Testing, Health

Abstract

Introduction: A potential concern with the use of dapivirine (DPV) for HIV prevention is the selection of a drug-resistant virus that could spread and reduce the effectiveness of non-nucleoside reverse transcriptase (NNRTI)-based first-line antiretroviral therapy. We evaluated HIV-1 seroconversions in MTN-020/ASPIRE for selection of drug resistance and evaluated the genetic basis for observed reductions in susceptibility to DPV. Methods: MTN-020/ASPIRE was a placebo-controlled, Phase III safety and effectiveness study of DPV ring for HIV-1 prevention conducted at 15 sites in South Africa, Zimbabwe, Malawi and Uganda between 2012 and 2015. Plasma from individuals who seroconverted in ASPIRE was analysed for HIV-1 drug resistance using both population Sanger sequencing and next-generation sequencing (NGS) with unique molecular identifiers to report mutations at [greater than or equal to]1% frequency. DPV susceptibility of plasma-derived recombinant HIV-1 containing bulk-cloned full-length reverse transcriptase sequences from MTN-020/ASPIRE seroconversions was determined in TZM-blcells. Statistical significance was calculated using the Fisher's exact test. Results: Plasma from all 168 HIV seroconversions were successfully tested by Sanger sequencing; 57 of 71 DPV arm and 82 of 97 placebo (PLB) arm participants had NGS results at 1% sensitivity. Overall, 18/168 (11%) had NNRTI mutations including K101E, K103N/S, V106M, V108I, E138A/G, V179D/I/T and H221Y. Five samples from both arms had low-frequency NNRTI mutations that were not detected by Sanger sequencing. The frequency of NNRTI mutations from the DPV arm (11%) was not different from the PLB arm (10%; p = 0.80). The E138A mutation was detected in both the DPV (3 of 71 [4.2%]) and PLB arm (5 of 97 [5.2%]) and conferred modest reductions in DPV susceptibility in some reverse transcriptase backgrounds but not others. Conclusions: HIV-1 drug resistance including NNRTI resistance did not differ between the DPV and placebo arms of the MTN-020/ASPIRE study, indicating that drug resistance was not preferentially acquired or selected by the DPV ring and that the preventive benefit of DPV ring outweighs resistance risk. Keywords: dapivirine; HIV-1 drug resistance; HIV-1 prevention; next-generation sequencing; non-nucleoside reverse transcriptase inhibitors (NNRTI); pre-exposure prophylaxis (PrEP), INTRODUCTION Women in Sub-Saharan Africa have a disproportionate risk of HIV infection [1], highlighting the pressing need for safe and effective prevention strategies that allow for agency and choice. Dapivirine [...]

Published

2021

2. PrEP use and HIV seroconversion rates in adolescent girls and young women from Kenya and South Africa: the POWER demonstration project

Author

Celum, Connie L., Bukusi, Elizabeth A., Bekker, Linda Gail, Delany?Moretlwe, Sinead, Kidoguchi, Lara, Omollo, Victor, Rousseau, Elzette, Travill, Danielle, Morton, Jennifer F., Mogaka, Felix, O'Malley, Gabrielle, Barnabee, Gena, Straten, Ariane, Donnell, Deborah, Parikh, Urvi M., Kudrick, Lauren, Anderson, Peter L., Haberer, Jessica E., Wu, Linxuan, Heffron, Renee, Johnson, Rachel, Morrison, Susan, Baeten, Jared M., Odoyo, Josephine, Machafu, Hilda, Osore, Mary?Josephine, Osome, Ethel, Omondi, Fredrick, Kwach, Ben, Ang'Awa, David, Nyerere, Bernard, Awuor, Merceline, Dola, Annabel, Tsetso, John Bosco, Odek, Sherine, Mugalla, Sylvia, Momanyi, Vincent, Otieno, Peris, Misiko, Brenda, Odondi, Joel, Obuya, Calvin, Otieno, Boblief, Seda, Eric, Obiero, Alfred, Mwakisha, Rachel, Njenga, Petronilla, Zakariya, Dorothy, Nonjinge, Lindile, Julies, Robin, Fuzile, Pamela, Xeketwana, Thando, Thami, Lwazi, Futshane, Nkosiyabo, Raqa, Desmond, Mkatshana, Nomvuyiseko, Mpanda, Yolanda, Tlou, Thapelo, Kgabo, Kefilwe, Mbele, Samukelo, Nyamane, Phumzile, Lunika, Lerato, Gumede, Sanele, Ndlovu, Melt, and Khoza, Nomhle

Subjects

HIV seropositivity -- Distribution -- Demographic aspects, Young women -- Health aspects, Teenage girls -- Health aspects, Company distribution practices, Health

Abstract

: Introduction: HIV incidence remains high among African adolescent girls and young women (AGYW). The primary objective of this study is to assess pre‐exposure prophylaxis (PrEP) initiation, use, persistence and HIV acquisition among African AGYW offered PrEP in order to inform PrEP scale‐up. Methods: POWER was a prospective implementation science evaluation of PrEP delivery for sexually active HIV‐negative AGYW ages 16–25 in family planning clinics in Kisumu, Kenya and youth and primary healthcare clinics in Cape Town and Johannesburg, South Africa. Follow‐up visits occurred at month 1 and quarterly for up to 36 months. PrEP users were defined based on the month 1 refill. PrEP persistence through month 6 was assessed using Kaplan–Meier survival analysis among AGYW with a month 1 visit, defining non‐persistence as an ≥15 day gap in PrEP availability for daily dosing. PrEP execution was evaluated in a subset with PrEP supply from the prior visit sufficient for daily dosing by measuring blood tenofovir diphosphate (TFV‐DP) levels. Results: From June 2017 to September 2020, 2550 AGYW were enrolled (1000 in Kisumu, 787 in Cape Town and 763 in Johannesburg). Median age was 21 years, 66% had a sexual partner of unknown HIV status, and 29% had chlamydia and 10% gonorrhoea. Overall, 2397 (94%) initiated PrEP and 749 (31%) had a refill at 1 month. Of AGYW who could reach 6 months of post‐PrEP initiation follow‐up, 128/646 (20%) persisted with PrEP for 6 months and an additional 92/646 (14%) had a gap and restarted PrEP. TFV‐DP levels indicated that 47% (91/193) took an average of ≥4 doses/week. Sixteen HIV seroconversions were observed (incidence 2.2 per 100 person‐years, 95% CI 1.2, 3.5); 13 (81%) seroconverters either did not have PrEP dispensed in the study interval prior to seroconversion or TFV‐DP levels indicated Conclusions: In this study of PrEP integration with primary care and reproductive health services for African AGYW, demand for PrEP was high. Although PrEP use decreased in the first months, an important fraction used PrEP through 6 months. Strategies are needed to simplify PrEP delivery, support adherence and offer long‐acting PrEP options to improve persistence and HIV protection., INTRODUCTION African adolescent girls and young women (AGYW) have had HIV incidence rates of 4% in recent HIV prevention research cohorts [1–3]. Oral tenofovir‐based pre‐exposure prophylaxis (PrEP) confers >90% protection [...]

Published

2022

3. Dapivirine vaginal ring for HIV prevention: modelling health outcomes, drug resistande and cost-effectiveness

Author

Glaubius, Robert, Ding, Yajun, Penrose, Kerri J., Hood, Greg, Engquist, Erik, Mellors, John W., Parikh, Urvi M., and Abbas, Ume L.

Subjects

Highly active antiretroviral therapy -- Economic aspects -- Analysis -- Health aspects, HIV infections -- Prevention -- Economic aspects -- Analysis -- Health aspects, Emtricitabine -- Economic aspects -- Analysis -- Health aspects, Microbial drug resistance -- Prevention -- Economic aspects -- Analysis -- Health aspects, HIV -- Prevention -- Economic aspects -- Analysis -- Health aspects, Infection -- Prevention -- Economic aspects -- Analysis -- Health aspects, Epidemiology -- Economic aspects -- Analysis -- Health aspects, Sexually transmitted disease prevention -- Economic aspects -- Analysis -- Health aspects, Sex oriented businesses -- Economic aspects -- Analysis -- Health aspects, Circumcision -- Economic aspects -- Analysis -- Health aspects, Health, United Nations, World Health Organization

Abstract

Introduction: A vaginal ring containing dapivirine is effective for HIV prevention as pre-exposure prophylaxis (PrEP). We evaluated the potential epidemiological impact and cost-effectiveness of dapivirine vaginal ring PrEP among 22- to 45-year-old women in KwaZulu-Natal, South Africa. Methods: Using mathematical modelling, we studied dapivirine vaginal ring PrEP implementation, either unprioritized, or prioritized based on HIV incidence (>3% per year), age (22 to 29 years) or female sex worker status, alongside the implementation of voluntary medical male circumcision and antiretroviral therapy scaled-up to UNAIDS Fast-Track targets. Outcomes over the intervention (2019 to 2030) and lifetime horizons included cumulative HIV infections, life-years lived, costs and cost-effectiveness. We assessed the incremental cost-effectiveness ratios against the revealed willingness to pay ($500) and the standard (2017 per capita gross domestic product; $6161) cost-effectiveness thresholds for South Africa. Results: Compared to a reference scenario without PrEP, implementation of dapivirine vaginal ring PrEP, assuming 56% effectiveness and covering 50% of 22 to 29-year-old or high-incidence women, prevented 10% or 11% of infections by 2030 respectively. Equivalent, unprioritized coverage (30%) prevented fewer infections (7%), whereas 50% coverage of female sex workers had the least impact (4%). Drug resistande attributable to PrEP was modest (2% to 4% of people living with drug-resistant HIV). Over the lifetime horizon, dapivirine PrEP implementation among female sex workers was cost-saving, whereas incidence-based PrEP cost $1898 per life-year gained, relative to PrEP among female sex workers and $989 versus the reference scenario. In a scenario of 37% PrEP effectiveness, PrEP had less impact, but prioritization to female sex workers remained cost-saving. In uncertainty analysis, female sex worker PrEP was consistently cost-saving; and over the lifetime horizon, PrEP cost less than $6161 per life-year gained in over 99% of simulations, whereas incidence- and age-based PrEP cost below $500 per life-year gained in 61% and 49% of simulations respectively. PrEP adherence and efficacy, and the effectiveness of antiretroviral therapy for HIV prevention, were the principal drivers of uncertainty in the cost-effectiveness of PrEP. Conclusions: Dapivirine vaginal ring PrEP would be cost-saving in KwaZulu-Natal if prioritized to female sex workers. PrEP's impact on HIV prevention would be increased, with potential affordability if prioritized to women by age or incidence. Keywords: HIV prevention; pre-exposure prophylaxis/Preexposure prophylaxis/PrEP; dapivirine/DPV; vaginal ring; cost-effectiveness; drug resistande; mathematical mode, 1 | INTRODUCTION Pre-exposure prophylaxis (PrEP), the use of antiretrovirals by HIV-negative individuals to block HIV acquisition, is promising for HIV prevention. Oral PrEP is protective across populations, including men [...]

Published

2019

4. Dapivirine vaginal ring forHIVprevention: modelling health outcomes, drug resistance and cost‐effectiveness

Author

Glaubius, Robert, primary, Ding, Yajun, additional, Penrose, Kerri J, additional, Hood, Greg, additional, Engquist, Erik, additional, Mellors, John W, additional, Parikh, Urvi M, additional, and Abbas, Ume L, additional

Published

2019