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从进行性多灶性白质脑病患者中分离出的SV40变体的调控序列。

Regulatory sequences of SV40 variants isolated from patients with progressive multifocal leukoencephalopathy.

作者信息

Martin J D

机构信息

Mercer University School of Medicine, Macon, Georgia.

出版信息

Virus Res. 1989 Sep;14(1):85-94. doi: 10.1016/0168-1702(89)90072-5.

Abstract

Variants of the simian polyomavirus SV40 have been associated in humans with a small number of cases of progressive multifocal leukoencephalopathy (PML). Genomic regulatory regions of two independent isolates, SVPML-1 and -2 [L.P. Weiner et al., N. Engl. J. Med. 286, 385 (1972)], were analyzed to determine if they had acquired any sequences that are present in the genome of the human polyomavirus JC (JCV), the primary causative agent of PML. As compared to SV40 DNA, 83% of SVPML-1 and -2 cloned DNAs contained an apparent deletion of about 30 base pairs in the restriction fragment containing the regulatory region (type alpha); 17% had a deletion of about 60 base pairs (type beta). The regulatory sequences were identical in all four clones representative of SVPML-1 and -2 type alpha grown in human and monkey cells. Thus the primary genomes of two isolates of SV40 from PML are identical in the region that is highly heterogeneous in JCV. The SVPML-alpha-DNAs have a net deletion of 30 base pairs and rearrangements within the transcriptional enhancer. The transcriptional promoter and origin of DNA replication is unaltered from that of SV40. Therefore the human neurotropism of SVPML appears to be a consequence of important rearrangements of SV40 sequences rather than acquisition of JCV-like sequences.

摘要

猿猴多瘤病毒SV40的变体在人类中与少数进行性多灶性白质脑病(PML)病例有关。分析了两个独立分离株SVPML-1和-2 [L.P. 韦纳等人,《新英格兰医学杂志》286, 385 (1972)] 的基因组调控区域,以确定它们是否获得了人类多瘤病毒JC(JCV)基因组中存在的任何序列,JCV是PML的主要病原体。与SV40 DNA相比,83%的SVPML-1和-2克隆DNA在包含调控区域的限制性片段中出现了约30个碱基对的明显缺失(α型);17%有大约60个碱基对的缺失(β型)。在人类和猴细胞中生长的代表SVPML-1和-2 α型的所有四个克隆中,调控序列是相同的。因此,来自PML的两个SV40分离株的主要基因组在JCV中高度异质的区域是相同的。SVPML-α-DNAs在转录增强子内有30个碱基对的净缺失和重排。转录启动子和DNA复制起点与SV40的相同。因此,SVPML的人类嗜神经性似乎是SV40序列重要重排的结果,而不是获得JCV样序列的结果。

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