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The success of antiretroviral (ARV) therapy for preventing maternal-to-child HIV transmission has been tempered by excess risk for preterm birth, especially among pregnant women who receive protease inhibitors (PIs). Various data have suggested that low progesterone may play a role. To further investigate this mechanism, investigators conducted a series of experiments in cell lines and mice and an observational study in 44 pregnant women with or without HIV infection.
When trophoblastic progesterone-producing cells were exposed to ARVs, protease inhibitors (except darunavir) but not nucleoside reverse transcriptase inhibitors (NRTIs) or non-NRTIs resulted in diminished progesterone release. Pregnant mice treated with PI-containing ARV combin…