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Analysis of the Costructure of the Simian Virus 40 T-Antigen Origin Binding Domain with Site I Reveals a Correlation between GAGGC Spacing and Spiral Assembly

机译:具有位点I的猿猴病毒40 T抗原起源结合域的结构分析揭示了GAGGC间距和螺旋装配之间的相关性。

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摘要

Polyomavirus origins of replication contain multiple occurrences of G(A/G)GGC, the high-affinity binding element for the viral initiator T-antigen (T-ag). The site I regulatory region of simian virus 40, involved in the repression of transcription and the enhancement of DNA replication initiation, contains two GAGGC sequences arranged head to tail and separated by a 7-bp AT-rich sequence. We have solved a 3.2-Å costructure of the SV40 origin-binding domain (OBD) bound to site I. We have also established that T-ag assembly on site I is limited to the formation of a single hexamer. These observations have enabled an analysis of the role(s) of the OBDs bound to the site I pentanucleotides in hexamer formation. Of interest, they reveal a correlation between the OBDs bound to site I and a pair of OBD subunits in the previously described hexameric spiral structure. Based on these findings, we propose that spiral assembly is promoted by pentanucleotide pairs arranged in a head-to-tail manner. Finally, the possibility that spiral assembly by OBD subunits accounts for the heterogeneous distribution of pentanucleotides found in the origins of replication of polyomaviruses is discussed.
机译:多瘤病毒的复制起点包含多次出现的G(A / G)GGC,这是病毒引发剂T抗原(T-ag)的高亲和力结合元件。猿猴病毒40的位点I调控区,参与转录的抑制和DNA复制起始的增强,包含两个GAGGC序列,它们从头到尾排列并被富含7bp AT的序列隔开。我们已经解决了与位点I结合的SV40起源结合域(OBD)的3.2-Å共结构。我们还确定,位点I上的T-ag组装仅限于单个六聚体的形成。这些观察结果使得能够分析与六聚体形成中的五核苷酸I位点结合的OBD的作用。有趣的是,它们揭示了结合至位点I的OBD与先前描述的六聚螺旋结构中的一对OBD亚基之间的相关性。基于这些发现,我们提出以头到尾的方式排列的五核苷酸对促进螺旋装配。最后,讨论了OBD亚基的螺旋装配解释了在多瘤病毒复制起点中发现的五核苷酸异质分布的可能性。

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