Noguchi Lisa M, Owor Maxensia, Mgodi Nyaradzo M, Gati Mirembe Brenda, Dadabhai Sufia, Horne Elizea, Gundacker Holly, Richardson Barbra A, Bunge Katherine, Scheckter Rachel, Song Mei, Marzinke Mark A, Anderson Peter L, Livant Edward, Jacobson Cindy, Piper Jeanna M, Chakhtoura Nahida, Hillier Sharon L, Balkus Jennifer E
Reproductive, Maternal, Newborn, Child, and Adolescent Health Unit, Jhpiego, Johns Hopkins University, Washington, DC, USA.
Makerere University-Johns Hopkins University, Kampala, Uganda.
Lancet HIV. 2025 Mar;12(3):e180-e190. doi: 10.1016/S2352-3018(24)00306-0. Epub 2025 Feb 12.
In 2021, WHO recommended dapivirine vaginal rings (DVRs) for HIV prevention, but noted evidence gaps for breastfeeding populations. This trial aimed to describe safety profiles associated with DVRs and oral pre-exposure prophylaxis (PrEP) use during breastfeeding and to summarise study-drug quantification and concentrations for mothers and infants.
Microbicide Trials Network (MTN)-043 was a phase 3b, open-label, randomised trial in which mother-infant pairs were recruited from local health facilities and enrolled at four HIV clinical trial sites in Malawi, South Africa, Uganda, and Zimbabwe. Eligible mothers (aged ≥18 years) were HIV-negative, exclusively breastfeeding one infant (aged 6-12 weeks, birthweight ≥2000 g), and had not been exposed to HIV post-exposure prophylaxis in the previous 6 months. Mother-infant pairs were randomly assigned (3:1) via a computer-generated sequence to 12 weeks of 25 mg monthly DVR or daily oral PrEP (200 mg emtricitabine and 300 mg tenofovir disoproxil fumarate), with stratification by site using a permuted block design. Participants and staff were aware of study product assignment. Primary outcomes were maternal and infant safety (all serious adverse events and grade 3 or worse adverse events) and drug concentrations, which were measured in maternal plasma, maternal blood, breastmilk, infant plasma, and infant blood. All mother-infant pairs who received at least one dose of study product were included in the primary safety analysis, and those with at least one post-enrolment drug concentration result were included in the drug quantification analysis. The trial was registered at ClinicalTrials.gov (NCT04140266).
Between Sept 24, 2020, and July 29, 2021, 197 mother-infant pairs enrolled (148 on DVR and 49 on PrEP), all of whom received at least one dose of study product and were included in the primary safety analysis. Two (1%) of 148 mothers in the DVR group had serious adverse events, and three (2%) in the DVR group and two (4%) in the oral PrEP group had a grade 3 or worse adverse event; four (3%) of 148 infants in the DVR group had a serious adverse event, and ten (7%) in the DVR group and one (2%) in the oral PrEP group had a grade 3 or worse adverse event. No mother or infant in the oral PrEP group had a serious adverse event. No HIV infections were detected. 144 participants in the DVR group and 48 in the oral PrEP group had at least one post-enrolment drug concentration result. Quantifiable median dapivirine concentrations ranged from 656·0 (IQR 407·0-878·0) pg/mL at week 1 to 558·5 (282·0-778·0) pg/mL at month 3, but were observed infrequently (5-15%) in specimens from infants, with median concentrations below the limit of quantification at all visits. Median tenofovir diphosphate concentrations ranged from 263·0 (193·0-363·0) fmol/punch at week 1 to 777·0 (381·0-1241·0) fmol/punch at month 3, but were not observed in specimens from infants, with all concentrations below the limit of quantification at all visits.
Increased risk of HIV acquisition in the postnatal period, favourable product safety profile, and low drug exposures among infants support the recommendation for DVRs as an additional HIV prevention choice during breastfeeding.
US National Institutes of Health.
2021年,世界卫生组织推荐使用达匹韦林阴道环(DVR)进行HIV预防,但指出母乳喂养人群的证据存在缺口。本试验旨在描述母乳喂养期间使用DVR和口服暴露前预防(PrEP)相关的安全性概况,并总结母婴的研究药物定量和浓度情况。
杀微生物剂试验网络(MTN)-043是一项3b期开放标签随机试验,母婴对从当地卫生机构招募,在马拉维、南非、乌干达和津巴布韦的四个HIV临床试验点入组。符合条件的母亲(年龄≥18岁)为HIV阴性,纯母乳喂养一名婴儿(年龄6-12周,出生体重≥2000g),且在过去6个月内未接受过HIV暴露后预防。母婴对通过计算机生成的序列随机分配(3:1),接受为期12周的每月25mg DVR或每日口服PrEP(200mg恩曲他滨和300mg替诺福韦酯),采用分层区组随机设计按地点分层。参与者和工作人员知晓研究产品分配情况。主要结局为母婴安全性(所有严重不良事件和3级或更严重不良事件)和药物浓度,在母亲血浆、母亲血液、母乳、婴儿血浆和婴儿血液中进行测量。所有接受至少一剂研究产品的母婴对纳入主要安全性分析,至少有一次入组后药物浓度结果的纳入药物定量分析。该试验在ClinicalTrials.gov注册(NCT04140266)。
在2020年9月24日至2021年7月29日期间,197对母婴入组(148对接受DVR,49对接受PrEP),所有母婴均接受了至少一剂研究产品并纳入主要安全性分析。DVR组148名母亲中有2名(1%)发生严重不良事件,DVR组3名(2%)和口服PrEP组2名(4%)发生3级或更严重不良事件;DVR组148名婴儿中有4名(3%)发生严重不良事件,DVR组10名(7%)和口服PrEP组1名(2%)发生3级或更严重不良事件。口服PrEP组无母亲或婴儿发生严重不良事件。未检测到HIV感染。DVR组144名参与者和口服PrEP组48名参与者至少有一次入组后药物浓度结果。可定量的达匹韦林浓度中位数在第1周为656.0(IQR 407.0-878.0)pg/mL,在第3个月为558.5(282.0-778.0)pg/mL,但在婴儿标本中很少观察到(5-15%),所有访视时的中位数浓度均低于定量下限。替诺福韦二磷酸浓度中位数在第1周为263.0(193.0-363.0)fmol/打孔,在第3个月为777.0(381.0-1241.0)fmol/打孔,但在婴儿标本中未观察到,所有访视时的浓度均低于定量下限。
产后HIV感染风险增加、产品安全性良好以及婴儿药物暴露量低,支持推荐DVR作为母乳喂养期间额外的HIV预防选择。
美国国立卫生研究院。
