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Cervical and systemic concentrations of long acting hormonal contraceptive (LARC) progestins depend on delivery method: Implications for the study of HIV transmission

机译:长效激素避孕药(LARC)的宫颈和全身浓度取决于分娩方法:对HIV传播研究的意义

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摘要

Progestin-only long-acting reversible contraceptives (LARCs) are increasingly popular among women seeking contraception; however, recent epidemiological studies suggest that systemically administered medroxyprogesterone acetate (MPA) may increase HIV acquisition. In order to determine the exact mechanisms underlying increases in transmission specific to MPA use and to test safer, alternative contraceptive progestin types and delivery methods, in vitro modeling studies must be performed. To achieve this, it is imperative that accurate hormone concentrations be utilized when modeling progestin-mediated outcomes, as the down-stream effects are dose-dependent. The local concentrations of progestins to which the lower female genital tract tissues are exposed after initiation of LARCs are unknown, but they likely differ from peripheral concentrations, dependent upon the progestin type and delivery method. Here, we measured in vivo endocervical and plasma concentrations of (1) systemically-delivered depo MPA (DMPA), (2) levonorgestrel (LNG) delivered via intrauterine system (IUS) and (3) etonogestrel (ETG) delivered via vaginal ring in women who recently initiated contraception treatment. Levels of ETG and LNG in cervical secretions were 100–200 fold higher than plasma levels. In contrast, measurable MPA levels were approximately 10-fold higher in plasma compared to cervical secretions. These results will inform the design of accurate in vitro studies on the influence of progestins on epithelial cells, tissue explants, and peripheral blood cells, to be able to better predict in vivo outcomes. Subsequent observations will aid in determining how MPA might influence HIV acquisition and may facilitate identification of optimal progestin-containing LARC alternatives for women at high risk for HIV infection.
机译:纯黄体酮长效可逆避孕药(LARCs)在寻求避孕的女性中越来越受欢迎。但是,最近的流行病学研究表明,全身使用醋酸甲羟孕酮(MPA)可能会增加艾滋病毒的获取。为了确定特定于MPA使用的传播增加背后的确切机制,并测试更安全的替代性孕激素类型和递送方法,必须进行体外模型研究。为了实现这一点,当建模孕激素介导的结果时,必须使用准确的激素浓度,因为下游效应是剂量依赖性的。 LARC引发后,女性下生殖器官组织所暴露的孕激素的局部浓度是未知的,但取决于孕激素类型和递送方法,它们可能与外周浓度不同。在这里,我们测量了(1)通过子宫内系统(IUS)递送的全身递送的Depo MPA(DMPA),(2)左炔诺孕酮(LNG)和通过阴道环递送的(3)依托孕酮(ETG)的体内子宫颈和血浆浓度。最近开始避孕治疗的女性。宫颈分泌物中的ETG和LNG含量比血浆水平高100-200倍。相反,血浆中可测量的MPA水平比宫颈分泌物高约10倍。这些结果将为孕激素对上皮细胞,组织外植体和外周血细胞的影响进行准确的体外研究设计提供信息,从而能够更好地预测体内结果。随后的观察将有助于确定MPA如何影响艾滋病毒的获取,并可能有助于确定高感染HIV风险妇女的最佳孕激素替代LARC替代品。

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