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抗病毒和抗逆转录病毒药物进入中枢神经系统。

The entry of antiviral and antiretroviral drugs into the central nervous system.

作者信息

Groothuis D R, Levy R M

机构信息

Department of Neurology, Northwestern University Medical School, Evanston Hospital, Illinois 60201, USA.

出版信息

J Neurovirol. 1997 Dec;3(6):387-400. doi: 10.3109/13550289709031185.

Abstract

The ability of antiviral and antiretroviral drugs to enter the brain is a critical issue in the treatment of many viral brain diseases, including HIV-related neurologic disease. Much of the literature concerning nucleoside analog entry into the nervous system focuses on drug levels in the cerebrospinal fluid (CSF), equating these with drug levels in the brain extracellular fluid (ECF) as though the two compartments intermix freely. We review the anatomic and physiologic aspects of drug entry into CSF and into brain ECF, as well as the exchange processes between these two compartments. In most instances drug concentrations in the CSF and ECF compartments bear little relationship to one another and using CSF concentrations to extrapolate brain ECF concentrations may significantly overestimate the latter. Accepted terminology and methodology for making measurements of blood-brain barrier function are discussed. Studies of brain uptake that express results as brain:plasma ratios, or that have used microdialysis, may overestimate the amount of drug reaching the brain. Using published data, we present an estimate of the time course of Zidovudine (AZT) concentrations in brain ECF and show that brain concentrations of AZT will likely be below that necessary to inhibit HIV-1 replication when AZT is administered systemically. Antiviral nucleosides and oligonucleotides appear to have limited entry into the brain when given systemically, which may hinder therapy of viral brain diseases, while some of the protease inhibitors may enter the brain more readily. Alternative methods for increasing antiviral and antiretroviral drug delivery to brain are discussed.

摘要

抗病毒和抗逆转录病毒药物进入大脑的能力是治疗包括与HIV相关的神经疾病在内的许多病毒性脑部疾病的关键问题。许多关于核苷类似物进入神经系统的文献都集中在脑脊液(CSF)中的药物水平上,将其等同于脑细胞外液(ECF)中的药物水平,就好像这两个隔室可以自由混合一样。我们综述了药物进入脑脊液和脑细胞外液的解剖学和生理学方面,以及这两个隔室之间的交换过程。在大多数情况下,脑脊液和细胞外液隔室中的药物浓度彼此之间几乎没有关系,使用脑脊液浓度来推断脑细胞外液浓度可能会显著高估后者。讨论了测量血脑屏障功能的公认术语和方法。将脑摄取结果表示为脑:血浆比值或使用微透析的研究可能会高估到达大脑的药物量。利用已发表的数据,我们给出了齐多夫定(AZT)在脑细胞外液中的浓度随时间变化的估计,并表明当全身给药AZT时,其脑内浓度可能低于抑制HIV-1复制所需的浓度。全身给药时,抗病毒核苷和寡核苷酸进入大脑的能力似乎有限,这可能会阻碍病毒性脑部疾病的治疗,而一些蛋白酶抑制剂可能更容易进入大脑。还讨论了增加抗病毒和抗逆转录病毒药物向大脑递送的替代方法。

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