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NIH/瑞士小鼠DNA中的大多数鼠白血病病毒序列由两个密切相关的前病毒组成,每个前病毒都重复了几次。

Most of the murine leukemia virus sequences in the DNA of NIH/swiss mice consist of two closely related proviruses, each repeated several times.

作者信息

Steffen D L, Mural R, Cowing D, Mielcarz J, Young J, Roblin R

出版信息

J Virol. 1982 Jul;43(1):127-35. doi: 10.1128/JVI.43.1.127-135.1982.

Abstract

The structure of the endogenous murine leukemia virus (MuLV) sequences of NIH/Swiss mice was analyzed by restriction endonuclease digestion, gel electrophoresis, and hybridization to an MuLV nucleic acid probe. Digestion of mouse DNA with certain restriction endonucleases revealed two classes of fragments. A large number of fragments (about 30) were present at a relatively low concentration, indicating that each derived from a sequence present once in the mouse genome. A smaller number of fragments (one to five) were present at a much higher concentration and must have resulted from sequences present multiple times in the mouse genome. These results indicated that the endogenous MuLV sequences represent a family of dispersed repetitive sequences. Hybridization of these same digested mouse DNAs to nucleic acid probes representing different portions of the MuLV genome allowed construction of a map of the sites where restriction endonucleases cleave the endogenous MuLV sequences. Several independent recombinant DNA clones of endogenous MuLV sequences have been isolated from C3H mice (Roblin et al., J. Virol. 43:113-126, 1982). Analysis of these sequences shows that they have the structure of MuLV proviruses. The sites at which restriction endonucleases cleave within these proviruses appeared to be similar or identical to the sites at which these nucleases cleaved within the MuLV sequences of NIH/Swiss mice. This identity was confirmed by parallel electrophoresis. We conclude that the apparently complex pattern of endogenous MuLV sequences of NIH/Swiss mice consists largely of only two kinds of provirus, each repeated multiple times at dispersed sites in the mouse genome.

摘要

通过限制性内切酶消化、凝胶电泳以及与鼠白血病病毒(MuLV)核酸探针杂交,对NIH/Swiss小鼠的内源性MuLV序列结构进行了分析。用某些限制性内切酶消化小鼠DNA后,发现了两类片段。大量片段(约30个)以相对较低的浓度存在,这表明每个片段都源自小鼠基因组中仅出现一次的序列。少量片段(1至5个)以高得多的浓度存在,必定是由小鼠基因组中多次出现的序列产生的。这些结果表明,内源性MuLV序列代表了一个分散的重复序列家族。将这些相同的消化小鼠DNA与代表MuLV基因组不同部分的核酸探针杂交,从而构建了限制性内切酶切割内源性MuLV序列的位点图谱。已经从C3H小鼠中分离出了几个内源性MuLV序列的独立重组DNA克隆(Roblin等人,《病毒学杂志》43:113 - 126,1982年)。对这些序列的分析表明,它们具有MuLV前病毒的结构。限制性内切酶在这些前病毒内切割的位点似乎与它们在NIH/Swiss小鼠的MuLV序列内切割的位点相似或相同。这种一致性通过平行电泳得到了证实。我们得出结论,NIH/Swiss小鼠内源性MuLV序列看似复杂的模式主要仅由两种前病毒组成,每种前病毒在小鼠基因组的分散位点重复多次。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7751/256103/86343fc9c957/jvirol00154-0140-a.jpg

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