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在感染人类免疫缺陷病毒1型且患有腹泻和/或消瘦综合征的患者中,沙奎那韦的暴露量增加。

Enhanced saquinavir exposure in human immunodeficiency virus type 1-infected patients with diarrhea and/or wasting syndrome.

作者信息

Trout Hervé, Mentré France, Panhard Xavière, Kodjo Alissi, Escaut Lélia, Pernet Pascal, Gobert Jean-Gérard, Vittecoq Daniel, Knellwolf Anne-Laure, Caulin Charles, Bergmann Jean-François

机构信息

Laboratoire de Toxicologie et Pharmacologie Clinique, Service de Pharmacie, Hôpital Lariboisière, Paris, France.

出版信息

Antimicrob Agents Chemother. 2004 Feb;48(2):538-45. doi: 10.1128/AAC.48.2.538-545.2004.

Abstract

The protease inhibitor saquinavir was administered to 100 human immunodeficiency virus type 1 (HIV-1)-infected patients as a single 600-mg oral dose (hard gelatin capsules) with a standard breakfast, including 200 ml of grapefruit juice, during an open-label trial to assess whether diarrhea and/or wasting syndrome has consequences on its pharmacokinetics. Three groups of patients were enrolled: group 1, asymptomatic patients (n = 30); group 2, AIDS symptomatic patients without body weight loss or diarrhea (n = 37); and group 3, AIDS symptomatic patients with severe body weight loss and/or diarrhea (n = 33). Clinical and biological data (covariates) were collected. A population approach was performed with three blood samples per patient to estimate the mean population pharmacokinetic parameters (clearance [CL]/oral bioavailability [F], V/F, k(a), and lag time) and the derived ones (k(el), C(max), T(max), and area under the curve [AUC]). The relationships between groups, exposure (i.e., estimated individual post hoc AUCs), and covariates were explored by using multiple linear regressions. A significant increase in median AUCs (165, 349, and 705 ng. h. ml(-1) for groups 1, 2, and 3, respectively [P < 0.0001]) was observed. The enhancement in saquinavir exposure could be due to the destruction of the transporters in enterocytes and/or to the enlargement of their tight junctions, allowing a paracellular crossing of saquinavir as the illness spreads. Because of grapefruit juice intake by every patient, no implication of CYP3A4 could be assessed. These results strongly suggest that, despite its low intrinsic oral bioavailability, saquinavir can be considered as a relevant treatment for HIV-1-infected patients with diarrhea and/or wasting syndrome. This must be evaluated in a long-term period.

摘要

在一项开放标签试验中,蛋白酶抑制剂沙奎那韦以单次600毫克口服剂量(硬明胶胶囊)与标准早餐(包括200毫升葡萄柚汁)一起给予100名1型人类免疫缺陷病毒(HIV-1)感染患者,以评估腹泻和/或消瘦综合征是否对其药代动力学有影响。招募了三组患者:第1组,无症状患者(n = 30);第2组,有症状但无体重减轻或腹泻的艾滋病患者(n = 37);第3组,有严重体重减轻和/或腹泻的艾滋病患者(n = 33)。收集了临床和生物学数据(协变量)。采用群体方法,每位患者采集三份血样,以估计群体平均药代动力学参数(清除率[CL]/口服生物利用度[F]、V/F、k(a)和滞后时间)以及派生参数(k(el)、C(max)、T(max)和曲线下面积[AUC])。通过多元线性回归探索组间、暴露(即事后估计的个体AUC)和协变量之间的关系。观察到中位数AUC显著增加(第1、2和3组分别为165、349和705纳克·小时·毫升⁻¹ [P < 0.0001])。沙奎那韦暴露的增加可能是由于肠细胞中转运蛋白的破坏和/或其紧密连接的扩大,随着病情发展允许沙奎那韦通过细胞旁路穿过。由于每位患者都摄入了葡萄柚汁,无法评估CYP3A4的影响。这些结果强烈表明,尽管沙奎那韦的口服生物利用度较低,但对于患有腹泻和/或消瘦综合征的HIV-1感染患者,它可被视为一种有效的治疗方法。这必须在长期内进行评估。

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