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在确定艾滋病毒风险与激素避孕之间生物学联系方面的研究空白。

Research gaps in defining the biological link between HIV risk and hormonal contraception.

作者信息

Murphy Kerry, Irvin Susan C, Herold Betsy C

机构信息

Albert Einstein College of Medicine, Bronx, NY, USA.

出版信息

Am J Reprod Immunol. 2014 Aug;72(2):228-35. doi: 10.1111/aji.12209. Epub 2014 Feb 19.

Abstract

Epidemiologic data suggest an association between depot medroxyprogesterone acetate (DMPA), a progesterone-based hormonal contraceptive, and increased risk of HIV acquisition and transmission. DMPA is highly effective and is among the most commonly used form of hormonal contraception in areas of high HIV prevalence. Thus, defining the biological mechanisms that contribute to the potential negative synergy between DMPA and HIV is key and may facilitate the identification of alternative contraceptive strategies. Proposed mechanisms include thinning or disruption of the cervicovaginal epithelial barrier, induction of mucosal inflammation, interference with innate and adaptive soluble and cellular immune responses, and/or alterations in the vaginal microbiome. DMPA may also indirectly increase the risk of HIV by promoting genital herpes or other sexually transmitted infections. However, there is a paucity of rigorous in vitro, animal model and clinical data to support these potential mechanisms highlighting the need for future research.

摘要

流行病学数据表明,醋酸甲羟孕酮长效避孕针(DMPA)这种基于孕激素的激素避孕药与感染和传播HIV的风险增加之间存在关联。DMPA非常有效,是HIV高流行地区最常用的激素避孕方式之一。因此,确定导致DMPA与HIV之间潜在负面协同作用的生物学机制至关重要,这可能有助于确定替代避孕策略。提出的机制包括宫颈阴道上皮屏障变薄或破坏、黏膜炎症的诱导、对先天性和适应性可溶性及细胞免疫反应的干扰,和/或阴道微生物群的改变。DMPA还可能通过促进生殖器疱疹或其他性传播感染而间接增加感染HIV的风险。然而,缺乏严格的体外、动物模型和临床数据来支持这些潜在机制,这凸显了未来研究的必要性。

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