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抑霉素(一种真核生物中DNA复制的高度特异性抑制剂)对单纯疱疹病毒和痘苗病毒DNA聚合酶的抑制机制

Mechanism of inhibition of herpes simplex virus and vaccinia virus DNA polymerases by aphidicolin, a highly specific inhibitor of DNA replication in eucaryotes.

作者信息

Pedrali-Noy G, Spadari S

出版信息

J Virol. 1980 Nov;36(2):457-64. doi: 10.1128/JVI.36.2.457-464.1980.

DOI:10.1128/JVI.36.2.457-464.1980
PMID:6253671
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC353662/
Abstract

The inhibition in vitro of herpes simplex virus 1 and vaccinia virus DNA polymerases by aphidicolin is primarily noncompetitive with dGTP, dATP, dTTP, DNA, and Mg2+ and competitive with dCTP in analogy with the mode of inhibition of cellular alpha-polymerase. The degree of inhibition of viral or cellular growth in vivo can be quantitatively predicted by the degree of inhibition of the isolated replicative DNA polymerases at the same concentration of aphidicolin in suitable conditions (limiting dCTP concentration). Thus, the only in vivo target for aphidicolin is probably the replicative DNA polymerase, and aphidicolin is a highly specific inhibitor of replicative nuclear DNA synthesis in eucaryotes. This, coupled with the lack of mutagenic effect, represents a valuable property for an anticancer drug. The specificity of inhibition (contrary to the aspecific effect on almost all DNA polymerases by a true competitive inhibitor, such as 1-beta-D-arabinofuranosylcytidine 5'-triphosphate) and the structure of the drug, which does not resemble that of the triphosphates, suggest that aphidicolin must recognize a site common only to the replicative DNA polymerases of eucaryotes and different from the binding site for deoxyribonucleic triphosphates and DNA, which should be similar in reparative and procaryote-type DNA polymerase; the aphidicolin binding site is probably very near to, or even overlaping with, the binding site for dCTP so that the drug mimics a competitive effect with this nucleotide.

摘要

在体外,抑癌菌素对单纯疱疹病毒1和痘苗病毒DNA聚合酶的抑制作用主要与dGTP、dATP、dTTP、DNA和Mg2+呈非竞争性,与dCTP呈竞争性,这与对细胞α-聚合酶的抑制模式类似。在合适的条件下(dCTP浓度受限),在相同浓度的抑癌菌素下,通过对分离的复制性DNA聚合酶的抑制程度,可以定量预测体内病毒或细胞生长的抑制程度。因此,抑癌菌素在体内的唯一靶点可能是复制性DNA聚合酶,并且抑癌菌素是真核生物中复制性核DNA合成的高度特异性抑制剂。这一点,再加上缺乏诱变作用,是抗癌药物的一个有价值的特性。抑制的特异性(与真正的竞争性抑制剂如1-β-D-阿拉伯呋喃糖基胞嘧啶5'-三磷酸对几乎所有DNA聚合酶的非特异性作用相反)以及药物的结构,该结构与三磷酸酯不同,表明抑癌菌素必须识别仅真核生物复制性DNA聚合酶共有的一个位点,且不同于脱氧核糖核酸三磷酸和DNA的结合位点,修复性和原核生物型DNA聚合酶的该结合位点应相似;抑癌菌素结合位点可能非常靠近dCTP的结合位点,甚至与之重叠,因此该药物模拟了与该核苷酸的竞争作用。

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Mechanism of inhibition of herpes simplex virus and vaccinia virus DNA polymerases by aphidicolin, a highly specific inhibitor of DNA replication in eucaryotes.抑霉素(一种真核生物中DNA复制的高度特异性抑制剂)对单纯疱疹病毒和痘苗病毒DNA聚合酶的抑制机制
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本文引用的文献

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Studies on the mode of action of nalidixic acid.萘啶酸作用模式的研究。
Eur J Biochem. 1972 Feb 15;25(2):359-65. doi: 10.1111/j.1432-1033.1972.tb01704.x.
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Antiviral effects of aphidicolin, a new antibiotic produced by Cephalosporium aphidicola.头孢蚜霉菌产生的一种新型抗生素——阿非科林的抗病毒作用
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