Hepatic purine and pyrimidine metabolism: implications for antiviral chemotherapy of viral hepatitis.

T Shaw, S A Locarnini
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引用次数: 56

Abstract

The use of nucleoside analogues as antiviral agents is expanding. For most nucleoside analogues, intracellular phosphorylation is the major prerequisite for activity. Antiviral activity may be limited by poor uptake, absence of appropriate activating enzymes, catabolism, and competition from endogenous nucleotides. Appreciation of these factors, which are species-, tissue- and cell-specific is important in the understanding of the pharmacology and toxicology of nucleoside analogues. The use of nucleoside analogues against the agents of viral hepatitis is inherently problematic for many reasons including active hepatic nucleoside catabolism, probable absence of virus-specific activating enzymes, competition from endogenous nucleotides synthesised de novo or derived from RNA turnover, and factors related to mitochondrial toxicity. Despite these drawbacks, some nucleoside analogues have been found efficacious against hepatitis B virus and it is likely that as knowledge of their mechanism of action accumulates, their efficacy can be improved both by rational drug design and by use in combination with other drugs, including interferon.

肝嘌呤和嘧啶代谢:对病毒性肝炎抗病毒化疗的影响。
核苷类似物作为抗病毒药物的使用正在扩大。对于大多数核苷类似物,细胞内磷酸化是活性的主要先决条件。抗病毒活性可能受到摄取不良、缺乏适当的激活酶、分解代谢和内源性核苷酸竞争的限制。了解这些物种、组织和细胞特异性的因素对于理解核苷类似物的药理学和毒理学非常重要。使用核苷类似物治疗病毒性肝炎本身就存在问题,原因有很多,包括肝核苷分解代谢活跃、可能缺乏病毒特异性激活酶、来自内源性核苷酸的竞争,以及与线粒体毒性有关的因素。尽管存在这些缺陷,一些核苷类似物已被发现对乙型肝炎病毒有效,随着对其作用机制的了解的积累,它们的功效可能会通过合理的药物设计和与其他药物(包括干扰素)联合使用来提高。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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