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Formulation, pharmacokinetics and pharmacodynamics of topical microbicides

机译:局部杀菌剂的配方,药代动力学和药效学

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The development of safe topical microbicides that effectively prevent human immunodeficiency virus (HIV) infection is a major goal in curbing the human immunodeficiency virus pandemic. A number of past failures resulting from mucosal toxicity or lack of efficacy have informed the field. Products that caused toxicity to the female genital tract mucosa, and thereby increased the likelihood of HIV acquisition, included nonoxynol 9, cellulose sulfate, and C31 G vaginal gel Savvy?. Topical products that were ineffective in preventing HIV infection include BufferGel?, Carraguard?, and PRO 2000?. Antiretroviral drugs such as tenofovir and dapivirine formulated into microbicide products have shown promise, but there is much to learn about ideal product formulation and acceptability, and drug distribution and disposition (pharmacokinetics). Current formulations for water-soluble molecules include vaginally or rectally applied gels, vaginal rings, films and tablets. Dosing strategies (e.g. coitally dependent or independent) will be based on the pharmacokinetics of the active ingredient and the tolerance for less than perfect adherence.
机译:有效预防人类免疫缺陷病毒(HIV)感染的安全局部杀菌剂的开发是遏制人类免疫缺陷病毒大流行的主要目标。过去因粘膜毒性或功效不足而导致的许多失败已经为该领域提供了信息。对女性生殖道粘膜产生毒性并因此增加HIV感染可能性的产品包括壬诺酚9,硫酸纤维素和C31 G阴道凝胶Savvy?。不能有效预防HIV感染的局部用药包括BufferGel?,Carraguard?和PRO 2000?。配制为杀微生物剂产品的抗逆转录病毒药物,如替诺福韦和达匹韦林,已显示出希望,但要了解理想的产品配方和可接受性,以及药物的分布和处置(药代动力学),还有很多东西要学习。当前用于水溶性分子的制剂包括阴道或直肠施用的凝胶,阴道环,薄膜和片剂。给药策略(例如,依从地或独立地)将基于活性成分的药代动力学和对不完全粘附的耐受性。

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