不能检测奈非那韦的脑脊液中HIV-1感染的患者伴或不伴艾滋病痴呆复合物。

F Aweeka, A Jayewardene, S Staprans, S E Bellibas, B Kearney, P Lizak, T Novakovic-Agopian, R W Price
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引用次数: 105

摘要

目的:探讨HIV-1蛋白酶抑制剂奈非那韦在脑脊液中的渗透作用。设计:奈非那韦是一种常用的HIV-1蛋白酶抑制剂(PI),对降低血浆病毒载量非常有效。它在临床上与其他抗逆转录病毒药物联合使用,包括核苷和非核苷逆转录酶抑制剂(NRTIs和NNRTIs)。尽管其效力基于血浆HIV-1 RNA结果,但其在降低中枢神经系统(CNS)中HIV-1 RNA水平(即病毒载量)方面的有效性尚不确定。我们将脑脊液作为脑的替代物取样,因为这种液体也通过一种自由扩散的屏障——血-脑脊液屏障(BCB)与血液分离,它与血-脑屏障(BBB)具有相同的特性。这些奈非那韦脑脊液药代动力学研究利用了来自个体研究对象的多个脑脊液样本,这些研究的主要目的是比较抗病毒治疗后脑脊液和血液中的病毒动力学。方法:6例研究对象,其中4例有艾滋病性痴呆,2例无艾滋病性痴呆,进行了多次腰椎穿刺(LP)。给药后脑脊液取样的间隔时间不同(奈非那韦给药后0.48小时至10.3小时),以定量整个稳态给药间隔内的奈非那韦浓度。在四名研究对象中,脑脊液取样的同时评估了LP前后血浆中奈非那韦的水平,而在另外两名研究对象中,在LP前后获得了单一的血浆样本。总共分析了25份脑脊液样本。采用高效液相色谱法测定脑脊液和血浆中奈非那韦的浓度,定量限分别为25和50 ng/ml。结果:LP前后血药浓度平均分别为2420+/-1365 ng/ml和2528+/-1132 ng/ml。在脑脊液样本中未检测到奈非那韦,脑脊液中未出现>25 ng/ml的水平。因此,奈非那韦的标准治疗不会导致大多数HIV-1分离株的CSF药物浓度达到或超过IC95水平。然而,高脑脊液病毒载量的研究对象在联合用药方案(包括奈非那韦)的情况下经历了显著的减少,两名受试者显示出与血浆相当的脑脊液反应。结论:奈非那韦对脑脊液渗透性不明显。这一观察结果的临床重要性尚不确定,因为在4名开始使用奈非那韦联合其他抗逆转录病毒治疗的研究对象中,在开始治疗后4周或更晚取样时,脑脊液和血液中都获得了相当程度的病毒抑制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Failure to detect nelfinavir in the cerebrospinal fluid of HIV-1--infected patients with and without AIDS dementia complex.

Objective: To assess the penetration of the HIV-1 protease inhibitor, nelfinavir, into cerebrospinal fluid (CSF).

Design: Nelfinavir, a commonly used HIV-1 protease inhibitor (PI), is highly effective for reducing plasma viral load. It is deployed clinically in combination with other antiretroviral agents, including nucleoside and nonnucleoside reverse transcriptase inhibitors (NRTIs and NNRTIs). Despite its potency based on plasma HIV-1 RNA results, its effectiveness in reducing HIV-1 RNA levels (i.e., viral load) in the central nervous system (CNS) is less certain. We sampled the CSF as a surrogate for brain because this fluid also is separated from the blood by a barrier to free diffusion, the blood-CSF barrier (BCB), which shares properties with the blood-brain barrier (BBB). These studies of nelfinavir CSF pharmacokinetics exploited the multiple CSF samples derived from individual study subjects who were enrolled in studies the primary objective of which was to compare viral kinetics in CSF and blood in response to antiviral therapy.

Methods: Six study subjects, four with and two without AIDS dementia complex, underwent multiple lumbar punctures (LP). Intervals of CSF sampling after drug dosing were varied (from 0.48 hours to 10.3 hours after nelfinavir administration) to quantitate nelfinavir concentrations throughout the steady-state dosing interval. In four study subjects, CSF sampling was accompanied by assessment of nelfinavir levels in plasma before and after LP, whereas in the other two subjects, a single plasma sample was obtained before or after the LP. In total, 25 CSF samples were analyzed. Nelfinavir concentrations in CSF and plasma were determined using an high-performance liquid chromatography (HPLC) method with a limit of quantitation of 25 and 50 ng/ml, respectively.

Results: Plasma concentrations before and after LP averaged 2420+/-1365 ng/ml and 2528+/-1132 ng/ml, respectively. Nelfinavir was not detected in any of the CSF samples and levels >25 ng/ml were not present in the CSF. Thus, standard therapy with nelfinavir does not result in CSF drug concentrations at or exceeding the IC95 level for most HIV-1 isolates. However, study subjects with high CSF viral loads experienced a marked reduction in the context of the combination-drug regimen including nelfinavir with two subjects showing a comparable CSF response with that in plasma.

Conclusions: Nelfinavir does not appreciably penetrate into the CSF. The clinical importance of this observation is not certain, in that in four study subjects who initiated nelfinavir in combination with other antiretroviral therapy, a comparable degree of viral suppression was obtained in both the CSF and the blood when sampled 4 weeks or later after initiating therapy.

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