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首页> 外文期刊>Scientific reports. >Predicting HIV Pre-exposure Prophylaxis Efficacy for Women using a Preclinical Pharmacokinetic-Pharmacodynamic In Vivo Model
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Predicting HIV Pre-exposure Prophylaxis Efficacy for Women using a Preclinical Pharmacokinetic-Pharmacodynamic In Vivo Model

机译:在体内模型中使用临床前药代动力学 - 药物动力学预测艾滋病毒预接触预防妇女的疗效

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The efficacy of HIV pre-exposure prophylaxis (PrEP) relies on adherence and may also depend on the route of HIV acquisition. Clinical studies of systemic tenofovir disoproxil fumarate (TDF) PrEP revealed reduced efficacy in women compared to men with similar degrees of adherence. To select the most effective PrEP strategies, preclinical studies are critically needed to establish correlations between drug concentrations (pharmacokinetics [PK]) and protective efficacy (pharmacodynamics [PD]). We utilized an in vivo preclinical model to perform a PK-PD analysis of systemic TDF PrEP for vaginal HIV acquisition. TDF PrEP prevented vaginal HIV acquisition in a dose-dependent manner. PK-PD modeling of tenofovir (TFV) in plasma, female reproductive tract tissue, cervicovaginal lavage fluid and its intracellular metabolite (TFV diphosphate) revealed that TDF PrEP efficacy was best described by plasma TFV levels. When administered at 50?mg/kg, TDF achieved plasma TFV concentrations (370?ng/ml) that closely mimicked those observed in humans and demonstrated the same risk reduction (70%) previously attained in women with high adherence. This PK-PD model mimics the human condition and can be applied to other PrEP approaches and routes of HIV acquisition, accelerating clinical implementation of the most efficacious PrEP strategies.
机译:艾滋病毒预曝光预防(PREP)依赖于依从性的疗效,也可能取决于艾滋病毒的途径。与具有相似程度的粘附程度的男性相比,全身崇高罗西毒性富马酸莫氏菌(TDF)Prep的临床研究表明,女性的疗效降低。为了选择最有效的预备策略,临床前进研究是批判性的,以确定药物浓度(药代动力学[PK])与保护效率(药效学[PD])之间的相关性。我们利用了体内临床前模型,对阴道艾滋病毒采集进行全身TDF准备的PK-PD分析。 TDF PREP预防剂量依赖性方式防止阴道艾滋病病毒。紫罗脂(TFV)在血浆,雌性生殖道组织,宫颈灌洗液及其细胞内代谢物(TFV二磷酸盐)中的PK-PD造型显示,血浆TFV水平最佳地描述TDF预备疗效。当以50μmg/ kg施用时,TDF达到血浆TFV浓度(370μg/ ml),其紧密地模仿在人类中观察到的那些,并证明了高粘附性妇女以前获得的相同风险降低(70%)。这种PK-PD模型模拟人体状况,可应用于其他预备方法和艾滋病毒习得途径,加速临床实施最有效的预备策略。

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