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氧杂环丁烷菌素G的三磷酸衍生物及相关化合物对真核生物和病毒DNA聚合酶以及人类免疫缺陷病毒逆转录酶的抑制作用。

Inhibitory effects of triphosphate derivatives of oxetanocin G and related compounds on eukaryotic and viral DNA polymerases and human immunodeficiency virus reverse transcriptase.

作者信息

Izuta S, Shimada N, Kitagawa M, Suzuki M, Kojima K, Yoshida S

机构信息

Laboratory of Cancer Cell Biology, Nagoya University School of Medicine, Aichi.

出版信息

J Biochem. 1992 Jul;112(1):81-7. doi: 10.1093/oxfordjournals.jbchem.a123870.

Abstract

In order to clarify the biological activities of (-)-oxetanocin G, and (-)-oxetanocin A and its carbocyclic analogue, (-)-carboxetanocin G, the inhibitory effects of triphosphate derivatives of these compounds (OXT-GTP, OXT-ATP, and C-OXT-GTP) on eukaryotic and viral DNA polymerases were examined. DNA polymerase alpha purified from calf thymus was weakly inhibited by OXT-GTP and OXT-ATP but strongly by C-OXT-GTP, the Ki value being 0.22 microM. On the other hand, rat DNA polymerase beta was not affected by these analogues. DNA polymerase gamma purified from bovine testes was very weakly inhibited by OXT-GTP and OXT-ATP, but not by C-OXT-GTP. DNA polymerase from herpes simplex virus type-II (HSV-II) was strongly inhibited by all three analogues, the Ki values ranging from 0.5 to 1.0 microM. Human immunodeficiency virus-encoded reverse transcriptase (HIV RT) was also strongly inhibited by these three analogues, the Ki value of C-OXT-GTP being slightly smaller than that of OXT-GTP or OXT-ATP. Analysis of products synthesized on singly primed M13 single-stranded DNA by DNA polymerase alpha, HSV-II DNA polymerase or HIV RT in the presence of the analogues revealed that OXT-GTP and C-OXT-GTP were incorporated into DNA and caused chain termination mainly at sites one or two nucleotides beyond the cytosine bases on the template.

摘要

为阐明(-)-氧杂环丁烷霉素G、(-)-氧杂环丁烷霉素A及其碳环类似物(-)-羧基氧杂环丁烷霉素G的生物活性,研究了这些化合物的三磷酸衍生物(OXT-GTP、OXT-ATP和C-OXT-GTP)对真核和病毒DNA聚合酶的抑制作用。从小牛胸腺纯化的DNA聚合酶α受到OXT-GTP和OXT-ATP的弱抑制,但受到C-OXT-GTP的强抑制,Ki值为0.22微摩尔。另一方面,大鼠DNA聚合酶β不受这些类似物的影响。从牛睾丸纯化的DNA聚合酶γ受到OXT-GTP和OXT-ATP的极弱抑制,但不受C-OXT-GTP的抑制。来自II型单纯疱疹病毒(HSV-II)的DNA聚合酶受到所有三种类似物的强烈抑制,Ki值范围为0.5至1.0微摩尔。人类免疫缺陷病毒编码的逆转录酶(HIV RT)也受到这三种类似物的强烈抑制,C-OXT-GTP的Ki值略小于OXT-GTP或OXT-ATP。在类似物存在的情况下,对DNA聚合酶α、HSV-II DNA聚合酶或HIV RT在单链引物M13单链DNA上合成的产物进行分析,结果显示OXT-GTP和C-OXT-GTP被掺入DNA中,并主要在模板上胞嘧啶碱基后一两个核苷酸处导致链终止。

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