Papp Eszter, Balogun Kayode, Banko Nicole, Mohammadi Hakimeh, Loutfy Mona, Yudin Mark H, Shah Rajiv, MacGillivray Jay, Murphy Kellie E, Walmsley Sharon L, Silverman Michael, Serghides Lena
Toronto General Research Institute, University Health Network.
Women's College Research Institute, Women's College Hospital Department of Medicine.
J Infect Dis. 2016 May 15;213(10):1532-40. doi: 10.1093/infdis/jiw004. Epub 2016 Jan 5.
It has been reported that pregnant women receiving protease inhibitor (PI)-based combination antiretroviral therapy (cART) have lower levels of progesterone, which put them at risk of adverse birth outcomes, such as low birth weight. We sought to understand the mechanisms involved in this decline in progesterone level.
We assessed plasma levels of progesterone, prolactin, and lipids and placental expression of genes involved in progesterone metabolism in 42 human immunodeficiency virus (HIV)-infected and 31 HIV-uninfected pregnant women. In vitro studies and a mouse pregnancy model were used to delineate the effect of HIV from that of PI-based cART on progesterone metabolism.
HIV-infected pregnant women receiving PI-based cART showed a reduction in plasma progesterone levels (P= .026) and an elevation in placental expression of the progesterone inactivating enzyme 20-α-hydroxysteroid dehydrogenase (20α-HSD; median, 2.5 arbitrary units [AU]; interquartile range [IQR], 1.00-4.10 AU), compared with controls (median, 0.89 AU; IQR, 0.66-1.26 AU;P= .002). Prolactin, a key regulator of 20α-HSD, was lower (P= .012) in HIV-infected pregnant women. We observed similar data in pregnant mice exposed to PI-based cART. In vitro inhibition of 20α-HSD activity in trophoblast cells reversed PI-based cART-induced decreases in progesterone levels.
Our data suggest that the decrease in progesterone levels observed in HIV-infected pregnant women exposed to PI-based cART is caused, at least in part, by an increase in placental expression of 20α-HSD, which may be due to lower prolactin levels observed in these women.
据报道,接受基于蛋白酶抑制剂(PI)的联合抗逆转录病毒疗法(cART)的孕妇孕酮水平较低,这使她们面临不良分娩结局的风险,如低出生体重。我们试图了解孕酮水平下降所涉及的机制。
我们评估了42名感染人类免疫缺陷病毒(HIV)的孕妇和31名未感染HIV的孕妇的血浆孕酮、催乳素和脂质水平,以及胎盘孕酮代谢相关基因的表达。体外研究和小鼠妊娠模型用于区分HIV与基于PI的cART对孕酮代谢的影响。
与对照组相比,接受基于PI的cART的HIV感染孕妇血浆孕酮水平降低(P = 0.026),孕酮失活酶20-α-羟基类固醇脱氢酶(20α-HSD)的胎盘表达升高(中位数,2.5任意单位[AU];四分位间距[IQR],1.00 - 4.10 AU),而对照组中位数为0.89 AU;IQR为0.66 - 1.26 AU;P = 0.002)。催乳素是20α-HSD的关键调节因子,在感染HIV的孕妇中较低(P = 0.012)。我们在接受基于PI的cART的妊娠小鼠中观察到了类似的数据。体外抑制滋养层细胞中的20α-HSD活性可逆转基于PI的cART诱导的孕酮水平降低。
我们的数据表明,在接受基于PI的cART的HIV感染孕妇中观察到的孕酮水平下降至少部分是由胎盘20α-HSD表达增加引起的,这可能是由于这些女性中观察到的催乳素水平较低所致。
