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人巨细胞病毒感染的人二倍体成纤维细胞中核苷类似物9-[(2-羟基-1-(羟甲基)乙氧基]甲基)鸟嘌呤的代谢活化作用

Metabolic activation of the nucleoside analog 9-[( 2-hydroxy-1-(hydroxymethyl)ethoxy]methyl)guanine in human diploid fibroblasts infected with human cytomegalovirus.

作者信息

Biron K K, Stanat S C, Sorrell J B, Fyfe J A, Keller P M, Lambe C U, Nelson D J

出版信息

Proc Natl Acad Sci U S A. 1985 Apr;82(8):2473-7. doi: 10.1073/pnas.82.8.2473.

Abstract

9-[( 2-Hydroxy-1-(hydroxymethyl)ethoxy]-methyl)guanine (BW B759U) is a more potent inhibitor of human cytomegalovirus (HCMV) in vitro than is the related nucleoside analog acyclovir (ACV). BW B759U was selectively activated to the 5'-triphosphate (BW B759U-triphosphate) in cells infected with HCMV to levels at least 10-fold higher than those measured for ACV-triphosphate and up to as much as 100-fold higher than the levels found in uninfected cells. BW B759U-triphosphate accumulated in HCMV-infected cells with time; the rate of this increase was dependent upon the drug dose and virus multiplicity of infection. Enzyme activities that catalyzed the phosphorylation of thymidine and 2'-deoxycytidine increased 3- to 7-fold in extracts of cells early after HCMV infection but thereafter declined. No concomitant increase in the rate of BW B759U phosphorylation was detected under these assay conditions. Maximal rate of accumulation of both BW B759U-triphosphate and ACV-triphosphate after a short exposure to drug occurred in the late phase of the infective cycle, as the titer of extracellular virus reached a peak in untreated cultures, but after the decline of stimulated host deoxypyrimidine kinase activities. Once formed, the BW B759U-triphosphate pool decreased very slowly and thus it persisted for several days in both HCMV-infected and uninfected cells.

摘要

9-[(2-羟基-1-(羟甲基)乙氧基]-甲基)鸟嘌呤(BW B759U)在体外对人巨细胞病毒(HCMV)的抑制作用比相关核苷类似物阿昔洛韦(ACV)更强。在感染HCMV的细胞中,BW B759U被选择性激活为5'-三磷酸(BW B759U-三磷酸),其水平比阿昔洛韦三磷酸(ACV-三磷酸)至少高10倍,比未感染细胞中的水平高出多达100倍。随着时间的推移,BW B759U-三磷酸在HCMV感染的细胞中积累;这种增加的速率取决于药物剂量和病毒感染复数。在HCMV感染早期,催化胸苷和2'-脱氧胞苷磷酸化的酶活性在细胞提取物中增加了3至7倍,但随后下降。在这些测定条件下,未检测到BW B759U磷酸化速率的相应增加。在感染周期后期,短暂接触药物后,BW B759U-三磷酸和ACV-三磷酸的最大积累速率出现,此时未处理培养物中细胞外病毒滴度达到峰值,但在刺激的宿主脱氧嘧啶激酶活性下降之后。一旦形成,BW B759U-三磷酸池下降非常缓慢,因此它在HCMV感染和未感染的细胞中都持续存在数天。

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