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通过腺苷脱氨酶激活的6-卤代双脱氧嘌呤前药实现2',3'-双脱氧肌苷对中枢神经系统的靶向作用。

Central nervous system targeting of 2',3'-dideoxyinosine via adenosine deaminase-activated 6-halo-dideoxypurine prodrugs.

作者信息

Morgan M E, Chi S C, Murakami K, Mitsuya H, Anderson B D

机构信息

Department of Pharmaceutics, University of Utah, Salt Lake City 84124.

出版信息

Antimicrob Agents Chemother. 1992 Oct;36(10):2156-65. doi: 10.1128/AAC.36.10.2156.

Abstract

AIDS dementia complex is a neurologic disorder, characterized by increasingly severe cognitive, behavioral, and motor impairment, which is associated with human immunodeficiency virus (HIV) infection in the central nervous system (CNS). Many of the dideoxynucleosides effective systemically in the treatment of HIV infections, such as 2',3'-dideoxyinosine (ddI), exhibit limited penetration into the CNS and limited or variable effectiveness in reversing the symptoms of AIDS dementia. Thus, approaches for increasing the CNS uptake of ddI and other dideoxynucleosides are needed. The CNS uptake of a series of 6-halo-2',3'-dideoxypurine ribofuranosides (6-halo-ddPs) previously shown to be active against HIV because of their conversion to ddI through the action of adenosine deaminase was examined in rats. In vitro studies in rat blood and brain tissue homogenate suggested a favorable selectivity for bioconversion in brain tissue, but with bioconversion half-lives varying widely within the series. In vivo infusions of 6-chloro-ddP (6-Cl-ddP), 6-bromo-ddP (6-Br-ddP), and 6-iodo-ddP (6-I-ddP) resulted in significant increases (20- to 34-fold) in the ddI concentration ratios in brain parenchyma/plasma when compared with those after an infusion of ddI alone. Absolute concentrations of ddI in brain parenchyma were increased 10- and 4-fold, respectively, following 30-min infusions of 6-Cl-ddP or 6-Br-ddP, but were 2.4-fold lower after an infusion of 6-I-ddP relative to that after a control infusion of ddI. Detailed studies of the plasma pharmacokinetics, CNS uptake kinetics, and bioconversion of 6-Cl-ddP were conducted to compare in vivo transport and bioconversion parameters with those predicted from in vitro measurements and to rationalize the efficiency of CNS delivery of ddI from 6-Cl-ddP. The results show that increased lipophilicity alone does not ensure that a given prodrug will deliver higher levels of a parent compound to the CNS. Both the selectivity and absolute rate of bioconversion in the brain are important factors.

摘要

艾滋病痴呆综合征是一种神经系统疾病,其特征为认知、行为和运动功能障碍日益严重,与中枢神经系统(CNS)中的人类免疫缺陷病毒(HIV)感染有关。许多在全身有效治疗HIV感染的双脱氧核苷,如2',3'-双脱氧肌苷(ddI),在CNS中的渗透有限,在逆转艾滋病痴呆症状方面效果有限或不稳定。因此,需要增加ddI和其他双脱氧核苷在CNS中摄取的方法。在大鼠中研究了一系列先前显示因其通过腺苷脱氨酶作用转化为ddI而对HIV有活性的6-卤代-2',3'-双脱氧嘌呤核糖苷(6-卤代-ddP)在CNS中的摄取。大鼠血液和脑组织匀浆的体外研究表明在脑组织中生物转化具有良好的选择性,但该系列中生物转化半衰期差异很大。与单独输注ddI后相比,体内输注6-氯-ddP(6-Cl-ddP)、6-溴-ddP(6-Br-ddP)和6-碘-ddP(6-I-ddP)导致脑实质/血浆中ddI浓度比显著增加(20至34倍)。在输注6-Cl-ddP或6-Br-ddP 30分钟后,脑实质中ddI的绝对浓度分别增加了10倍和4倍,但输注6-I-ddP后相对于对照输注ddI后降低了2.4倍。对6-Cl-ddP的血浆药代动力学、CNS摄取动力学和生物转化进行了详细研究,以比较体内转运和生物转化参数与体外测量预测的参数,并阐明从6-Cl-ddP向CNS递送ddI的效率。结果表明,仅增加亲脂性并不能确保给定的前药将更高水平的母体化合物递送至CNS。脑中生物转化的选择性和绝对速率都是重要因素。

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