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凝胶体积对 DuoGel-IQB4012(一种双室双药 HIV 杀微生物剂凝胶)阴道和直肠应用于长尾猕猴的药代动力学的影响。

Effects of gel volume on pharmacokinetics for vaginal and rectal applications of combination DuoGel-IQB4012, a dual chamber-dual drug HIV microbicide gel, in pigtailed macaques.

机构信息

LifeSource Biomedical LLC, Moffett Field, CA, USA.

Anyar Inc, Fort Walton Beach, FL, USA.

出版信息

Drug Deliv Transl Res. 2018 Oct;8(5):1180-1190. doi: 10.1007/s13346-018-0538-0.

Abstract

This study evaluated effects of differing gel volumes on pharmacokinetics (PK). IQB4012, a gel containing the non-nucleoside reverse transcriptase inhibitor IQP-0528 and tenofovir (TFV), was applied to the pigtailed macaque vagina and rectum. Vaginal gel volumes (1% loading of both drugs) were 0.5 or 1.5 ml; following wash-out, 1 or 4 ml of gel were then applied rectally. Blood, vaginal, and rectal fluids were collected at 0, 2, 4, and 24 h. Vaginal and rectal tissue biopsies were collected at 4 and 24 h. There were no statistically significant differences in concentrations for either drug between gel volumes within compartments at matched time points. After vaginal gel application, median IQP-0528 concentrations were ~ 10-10 ng/g, 10-10 ng/ml, and 10-10 ng/ml in vaginal tissues, vaginal fluids, and rectal fluids, respectively (over 24 h). Median vaginal TFV concentrations were 1-2 logs lower than IQP-0528 levels at matched time points. After rectal gel application, median IQP-0528 and TFV concentrations in rectal fluids were ~ 10-10 ng/ml and ~ 10-10 ng/ml, respectively. Concentrations of both drugs sampled in rectal tissues were low (~ 10-10 ng/g). For 1 ml gel, half of sampled rectal tissues had undetectable concentrations of either drug, and over half of sampled rectal fluids had undetectable TFV concentrations. These results indicate differences in drug delivery between the vaginal and rectal compartments, and that smaller vaginal gel volumes may not significantly compromise microbicide PK and prophylactic potential. However, effects of rectal gel volume on PK for both drugs were less definitive.

摘要

本研究评估了不同凝胶体积对药代动力学(PK)的影响。IQB4012 凝胶含有非核苷逆转录酶抑制剂 IQP-0528 和替诺福韦(TFV),应用于恒河猴阴道和直肠。阴道凝胶体积(两种药物的 1%负荷量)为 0.5 或 1.5ml;冲洗后,再直肠内应用 1 或 4ml 凝胶。在 0、2、4 和 24 小时时收集血液、阴道和直肠液。在 4 和 24 小时时收集阴道和直肠组织活检。在匹配时间点,两种药物在各隔室内的凝胶体积之间的浓度没有统计学差异。阴道凝胶应用后,阴道组织、阴道液和直肠液中 IQP-0528 浓度中位数分别约为 10-10ng/g、10-10ng/ml 和 10-10ng/ml(24 小时内)。在匹配时间点,阴道 TFV 浓度中位数比 IQP-0528 水平低 1-2 个对数。直肠凝胶应用后,直肠液中 IQP-0528 和 TFV 浓度中位数分别约为 10-10ng/ml 和 10-10ng/ml。直肠组织中两种药物的浓度均较低(~10-10ng/g)。对于 1ml 凝胶,一半的直肠组织样本中两种药物均无法检测到,超过一半的直肠液样本中无法检测到 TFV 浓度。这些结果表明,阴道和直肠隔室之间存在药物输送差异,较小的阴道凝胶体积可能不会显著影响杀微生物剂 PK 和预防潜力。然而,直肠凝胶体积对两种药物 PK 的影响不太明确。

相似文献

本文引用的文献

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Vaginal drug distribution modeling.阴道药物分布建模。
Adv Drug Deliv Rev. 2015 Sep 15;92:2-13. doi: 10.1016/j.addr.2015.04.017. Epub 2015 Apr 28.

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