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艾滋病预防中的药代动力学和药效学:现状与未来方向:美国国立过敏与传染病研究所艾滋病司(DAIDS)和比尔及梅琳达·盖茨基金会(BMGF)赞助的关于艾滋病预防中药代动力学(PK)/药效学(PD)的智库总结

Pharmacokinetics and pharmacodynamics in HIV prevention; current status and future directions: a summary of the DAIDS and BMGF sponsored think tank on pharmacokinetics (PK)/pharmacodynamics (PD) in HIV prevention.

作者信息

Romano Joseph, Kashuba Angela, Becker Stephen, Cummins James, Turpin Jim, Veronese Fulvia

机构信息

1 NWJ Group , LLC, Wayne, Pennsylvania.

出版信息

AIDS Res Hum Retroviruses. 2013 Nov;29(11):1418-27. doi: 10.1089/aid.2013.0122. Epub 2013 May 22.

Abstract

Thirty years after its beginning, the HIV/AIDS epidemic is still raging around the world. According to UNAIDS, in 2011 alone 1.7M deaths were attributable to AIDS, and 2.5M people were newly infected by the virus. Despite the success in treating HIV-infected people with potent antiretroviral drugs, preventing HIV infection is the key to ending the epidemic. Recently, the efficacy of topical and systemic antiviral chemoprophylaxis (i.e., preexposure prophylaxis or "PrEP"), using the same drugs used for HIV treatment, has been demonstrated in a number of clinical trials. However, results from other trials have been inconsistent, especially those evaluating PrEP in women. These inconsistencies may result from our incomplete understanding of pharmacokinetics (PK)/pharmacodynamics (PD) at the mucosal sites of sexual transmission: the male and female gastrointestinal and reproductive tracts. The drug concentrations used in these trials were derived from those used for treatment; however, we still do not know the relationship between the therapeutic and the preventive dose. This article presents the first comprehensive review of the available data in the HIV pharmacology field from animal models to human studies, and outlines gaps, challenges, and future directions. Addressing these pharmacological gaps and challenges will be critical in selecting and advancing future PrEP candidates and strategies with the greatest impact on the HIV epidemic.

摘要

艾滋病病毒/艾滋病疫情自爆发30年来仍在全球肆虐。据联合国艾滋病规划署称,仅在2011年,就有170万人死于艾滋病,250万人新感染该病毒。尽管使用强效抗逆转录病毒药物治疗艾滋病毒感染者取得了成功,但预防艾滋病毒感染仍是终结疫情的关键。最近,在多项临床试验中已证明,使用与治疗艾滋病毒相同的药物进行局部和全身抗病毒化学预防(即暴露前预防或“PrEP”)具有疗效。然而,其他试验的结果并不一致,尤其是在评估女性PrEP的试验中。这些不一致可能是由于我们对性传播黏膜部位(男性和女性的胃肠道及生殖道)的药代动力学(PK)/药效学(PD)了解不全面所致。这些试验中使用的药物浓度源自治疗用药浓度;然而,我们仍然不清楚治疗剂量与预防剂量之间的关系。本文首次全面综述了从动物模型到人体研究的艾滋病毒药理学领域的现有数据,并概述了差距、挑战及未来方向。解决这些药理学方面的差距和挑战对于选择和推进对艾滋病毒疫情影响最大的未来PrEP候选药物和策略至关重要。

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