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体外对H5ts125腺病毒DNA复制中温度敏感缺陷的互补作用。

Complementation of the temperature-sensitive defect in H5ts125 adenovirus DNA replication in vitro.

作者信息

Kaplan L M, Ariga H, Hurwitz J, Horwitz M S

出版信息

Proc Natl Acad Sci U S A. 1979 Nov;76(11):5534-8. doi: 10.1073/pnas.76.11.5534.

Abstract

Soluble extracts of adenovirus-infected HeLa cell nuclei support DNA replication on exogenous adenovirus DNA templates. Conditions of synthesis using both wild-type and temperature-sensitive extracts have been defined. Nuclear extracts prepared from cells permissively infected with the adenovirus mutant H5ts125 expressed the temperature-sensitive phenotype and could be inactivated at 37 degrees C in vitro. These extracts were completely complemented by the addition of wild-type adenovirus DNA binding protein but not by H5ts125 DNA binding protein. Enhancement by binding protein in the mutant extracts represents replication, as demonstrated by the production of full-sized products and orderly chain elongation originating, as in vivo, at both ends of the linear DNA. Replicative synthesis required the 5'-terminal protein bound covalently to template DNA and could be inhibited by denaturation of this 55,000-dalton protein. Various inhibitors of eukaryotic DNA polymerases, such as aphidicolin and 2',3'-dideoxythymidine triphosphate, inhibited replication of exogenous adenovirus templates in this system as they do in previously reported systems that only elongate endogenous replicating intermediates.

摘要

腺病毒感染的HeLa细胞核的可溶性提取物可支持外源腺病毒DNA模板上的DNA复制。已确定使用野生型和温度敏感型提取物的合成条件。从被腺病毒突变体H5ts125允许感染的细胞中制备的核提取物表现出温度敏感表型,并且在体外37℃下可被灭活。通过添加野生型腺病毒DNA结合蛋白可完全补充这些提取物,但添加H5ts125 DNA结合蛋白则不能。突变体提取物中结合蛋白的增强作用代表复制,如全尺寸产物的产生以及线性DNA两端如体内一样有序的链延伸所证明。复制性合成需要与模板DNA共价结合的5'-末端蛋白,并且该55,000道尔顿蛋白的变性可抑制复制。各种真核DNA聚合酶抑制剂,如阿非迪霉素和2',3'-二脱氧胸苷三磷酸,在该系统中可抑制外源腺病毒模板的复制,就像它们在先前报道的仅延长内源性复制中间体的系统中一样。

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