Maternal depression treatment in HIV (M-DEPTH) | Zendy

Glenn Wagner | Zendy; Ryan McBain | Zendy; Dickens Akena | Zendy; Victoria K. Ngo | Zendy; Janet Nakigudde | Zendy; Juliet Nakku | Zendy; Harriet Chemusto | Zendy; Jolly Beyeza-Kashesya | Zendy; Violet Gwokyalya | Zendy; Laura J. Faherty | Zendy; Leticia Kyohangirwe | Zendy; Linda Nabitaka | Zendy; Hafsa Lukwata | Zendy; Sebastian Linnemayr | Zendy; Bonnie Ghosh-Dastidar | Zendy; Juliet Businge | Zendy; Barbara Mukasa | Zendy; Rhoda K. Wanyenze | Zendy

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Maternal depression treatment in HIV (M-DEPTH)

Author(s) -

Glenn Wagner,

Ryan McBain,

Dickens Akena,

Victoria K. Ngo,

Janet Nakigudde,

Juliet Nakku,

Harriet Chemusto,

Jolly Beyeza-Kashesya,

Violet Gwokyalya,

Laura J. Faherty,

Leticia Kyohangirwe,

Linda Nabitaka,

Hafsa Lukwata,

Sebastian Linnemayr,

Bonnie Ghosh-Dastidar,

Juliet Businge,

Barbara Mukasa,

Rhoda K. Wanyenze

Publication year - 2019

Publication title -

medicine

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 0.59

H-Index - 148

eISSN - 1536-5964

pISSN - 0025-7974

DOI - 10.1097/md.0000000000016329

Subject(s) - medicine , pregnancy , depression (economics) , pediatrics , randomized controlled trial , obstetrics , genetics , biology , economics , macroeconomics

Over one-third of human immunodeficiency virus (HIV)-infected pregnant women are clinically depressed, increasing the risk of mother-to-child transmission (MTCT) of HIV, as well as negative birth and child development outcomes. This study will evaluate the efficacy and cost-effectiveness of an evidence-based stepped care treatment model for perinatal depression (maternal depression treatment in HIV [M-DEPTH]) to improve adherence to prevention of MTCT care among HIV+ women in Uganda. Methods: Eight antenatal care (ANC) clinics in Uganda will be randomized to implement either M-DEPTH (n=4) or usual care (n=4) for perinatal depression among 400 pregnant women (n=50 per clinic) between June 2019 and August 2022. At each site, women who screen positive for potential depression will be enrolled and followed for 18 months post-delivery, assessed in 6-month intervals: baseline, within 1 month of child delivery or pregnancy termination, and months 6, 12, and 18 following delivery. Primary outcomes include adherence to the prevention of mother-to-child transmission (PMTCT) care continuum—including maternal antiretroviral therapy and infant antiretrovial prophylaxis, and maternal virologic suppression; while secondary outcomes will include infant HIV status, post-natal maternal and child health outcomes, and depression treatment uptake and response. Repeated-measures multivariable regression analyses will be conducted to compare outcomes between M-DEPTH and usual care, using 2-tailed tests and an alpha cut-off of P <.05. Using a micro-costing approach, the research team will relate costs to outcomes, examining the incremental cost-effectiveness ration (ICER) of M-DEPTH relative to care as usual. Discussion: This cluster randomized controlled trial will be one of the first to compare the effects of an evidence-based depression care model versus usual care on adherence to each step of the PMTCT care continuum. If determined to be efficacious and cost-effective, this study will provide a model for integrating depression care into ANC clinics and promoting adherence to PMTCT. Trial Registration: NIH Clinical Trial Registry NCT03892915 (clinicaltrials.gov).

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