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Safety and Pharmacokinetics of Quick-Dissolving Polymeric Vaginal Films Delivering the Antiretroviral IQP-0528 for Preexposure Prophylaxis

机译:速溶性高分子阴道膜的安全性和药代动力学可提供抗逆转录病毒IQP-0528来预防暴露前

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摘要

For human immunodeficiency virus (HIV) prevention, microbicides or drugs delivered as quick-dissolving films may be more acceptable to women than gels because of their compact size, minimal waste, lack of an applicator, and easier storage and transport. This has the potential to improve adherence to promising products for preexposure prophylaxis. Vaginal films containing IQP-0528, a nonnucleoside reverse transcriptase inhibitor, were evaluated for their pharmacokinetics in pigtailed macaques. Polymeric films (22 by 44 by 0.1 mm; providing 75% of a human dose) containing IQP-0528 (1.5%, wt/wt) with and without poly(lactic-co-glycolic acid) (PLGA) nanoparticle encapsulation were inserted vaginally into pigtailed macaques in a crossover study design (n = 6). With unencapsulated drug, the median (range) vaginal fluid concentrations of IQP-0528 were 160.97 (2.73 to 2,104), 181.79 (1.86 to 15,800), and 484.50 (8.26 to 4,045) μg/ml at 1, 4, and 24 h after film application, respectively. Median vaginal tissue IQP-0528 concentrations at 24 h were 3.10 (0.03 to 222.58) μg/g. The values were similar at locations proximal, medial, and distal to the cervix. The IQP-0528 nanoparticle-formulated films delivered IQP-0528 in vaginal tissue and secretions at levels similar to those obtained with the unencapsulated formulation. A single application of either formulation did not disturb the vaginal microflora or the pH (7.24 ± 0.84 [mean ± standard deviation]). The high mucosal IQP-0528 levels delivered by both vaginal film formulations were between 1 and 5 log higher than the in vitro 90% inhibitory concentration (IC90) of 0.146 μg/ml. The excellent coverage and high mucosal levels of IQP-0528, well above the IC90, suggest that the films may be protective and warrant further evaluation in a vaginal repeated low dose simian-human immunodeficiency virus (SHIV) transmission study in macaques and clinically in women.
机译:为了预防人类免疫缺陷病毒(HIV),杀菌剂或速溶膜形式的药物比凝胶剂更适合女性使用,因为它们的体积小,浪费少,没有涂药器且易于储存和运输。这有可能提高对有前途的产品的依从性,以进行预暴露预防。评估了含有IQP-0528(一种非核苷类逆转录酶抑制剂)的阴道膜在尾巴猕猴中的药代动力学。将含有和不含有聚乳酸-乙醇酸(PLGA)纳米颗粒封装的IQP-0528(1.5%,wt / wt)的聚合物薄膜(22 x 44 x 0.1毫米;提供人类剂量的75%)插入阴道在交叉研究设计中(n = 6)进入尾巴的猕猴。对于未封装的药物,在1、4和24小时后,IQP-0528的阴道液中位数(范围)为160.97(2.73至2,104),181.79(1.86至15,800)和484.50(8.26至4,045)μg/ ml电影应用程序。阴道组织IQP-0528在24小时时的中位浓度为3.10(0.03至222.58)μg/ g。在子宫颈近端,中间和远端的位置值相似。 IQP-0528纳米颗粒配制的薄膜在阴道组织和分泌物中的递送IQP-0528的水平与未封装制剂所获得的水平相似。任一种制剂的单次施用都不会干扰阴道菌群或pH(7.24±0.84 [平均值±标准偏差])。两种阴道膜制剂所递送的高粘膜IQP-0528水平均比0.190μg/ ml的体外90%抑制浓度(IC90)高1至5 log。 IQP-0528的极佳覆盖率和高粘膜水平(远高于IC90)表明,这些膜可能具有保护性,并有必要在猕猴和女性临床上反复进行的多次阴道低剂量猿猴-人类免疫缺陷病毒(SHIV)传播研究中进一步评估。

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