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首页> 外文期刊>Journal of Virology >The T-antigen-binding domain of the simian virus 40 core origin of replication.
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The T-antigen-binding domain of the simian virus 40 core origin of replication.

机译:Simian病毒40核复制的T-抗原结合结构域。

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The simian virus 40 origin of replication contains a 27-base-pair palindrome with the sequence 5'-CA-GAGGC-C-GAGGC-G-GCCTC-G-GCCTC-TG-3'. The four 5'-GAGGC-3'/5'-GCCTC-3' pentanucleotides are known contact sites for simian virus 40 T-antigen binding in vitro. We used oligonucleotide-directed cassette mutagenesis to identify features of this palindrome that are important for the initiation of DNA replication in vivo. Each base pair of a pentanucleotide is crucial for DNA replication. In contrast, sequences adjacent to pentanucleotides have little or no effect on replication. Thus, the pentanucleotide is the basic functional unit, not only for T-antigen binding but also for DNA replication. All four pentanucleotides are indispensable in the initiation process. The spacing of pentanucleotides is crucial because duplication of the single base pair between binding sites has a far greater effect on replication than does substitution of the same base pair. Inversion of any pentanucleotide blocks DNA synthesis. Thus, the pentanucleotide is not a functionally symmetrical unit. We propose that each pentanucleotide positions a monomer of T antigen at the proper distance, rotation, and orientation relative to other T-antigen monomers and to other origin domains and that such positioning leads to subsequent events in replication.
机译:Simian病毒40复制起源含有27-碱基对序列的序列5'-CA-GAGGC-C-GAGGC-G-GCCTC-G-GCCTC-TG-3'。四个5'-GAGGC-3'/ 5'-GCCTC-3'偏核核苷酸是SIMIAN病毒40 T-抗原在体外结合的已知接触位点。我们使用寡核苷酸定向的盒式诱变诱变,以鉴定这种回文的特征,这对于在体内启动DNA复制是重要的。每个碱基对核核苷酸对DNA复制至关重要。相反,与五核苷酸相邻的序列对复制很少或没有影响。因此,戊核苷酸是基本功能单元,不仅适用于T-抗原结合,而且还用于DNA复制。所有四个五核苷酸在起始过程中是必不可少的。五核苷酸的间隔至关重要,因为结合位点之间的单个碱对的复制对复制的效果远小于同一碱基对的取代。任何五核苷酸的反转阻断DNA合成。因此,戊核苷酸不是功能性对称的单元。我们提出每个偏核苷酸在相对于其他T-抗原单体和其他原点域的适当距离,旋转和取向处定位一个T抗原的单体,并且这种定位导致随后的复制事件。

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