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腺病毒DNA结合蛋白的结构与功能:源自相应基因核苷酸序列的Ad5和Ad12蛋白氨基酸序列的比较

Structure and function of adenovirus DNA binding protein: comparison of the amino acid sequences of the Ad5 and Ad12 proteins derived from the nucleotide sequence of the corresponding genes.

作者信息

Kruijer W, van Schaik F M, Speijer J G, Sussenbach J S

出版信息

Virology. 1983 Jul 15;128(1):140-53. doi: 10.1016/0042-6822(83)90325-2.

Abstract

The adenoviral DNA binding protein (DBP) is a multifunctional protein involved in DNA replication and gene expression. In order to investigate the relation between structure and function of DBP, the amino acid sequences of the serotypes 5 and 12 (Ad5 and Ad12) have been compared. The amino acid sequence of Ad5 DBP was previously established by nucleotide sequence analysis of the Ad5 DBP gene (W. Kruijer, F. M. A. Van Schaik, and J. S. Sussenbach, Nucl. Acids Res. 9, 4439-4457, 1981). In this study the analysis of the Ad5 DBP gene and adjacent regions by determination of the sequence of the first leader in late DBP mRNA's and the splice point between the tripartite leader and the main body of the mRNA encoding the 100-kDa protein has been extended. The nucleotide sequence of the Ad12 DBP gene is also described. From the nucleotide sequence and RNA mapping data of Ad12 DBP mRNA's (I. Saito, J. Sato H. Handa, K. Shiraki, and H. Shimojo, Virology 114, 379-398, 1981) the complete Ad12 DBP amino acid sequence could be deduced. Ad12 DBP contains 484 amino acids and has an actual Mr of 54,992. It is 45 amino acids shorter than Ad5 DBP. Comparison of the Ad12 and Ad5 DBP amino acid sequences shows that several longer deletions are present in the N-terminal 125 amino acid residues of Ad12 DBP. In contrast, only a single amino acid deletion and insertion is found in the C-terminal 359 amino acids of Ad12 DBP. The N- and C-terminal domains of Ad12 and Ad5 DBP are 45 and 80% homologous, respectively. This suggests that both domains of DBP are subjected to different evolutionary pressures. Analysis of various Ad5 mutants with an altered DBP gene, has indicated that the C-terminal domain is involved in DNA replication and early gene expression, while the N-terminal domain has a role in late gene expression in monkey cells. These results are discussed in relation to the structure and function of adenovirus DBP.

摘要

腺病毒DNA结合蛋白(DBP)是一种参与DNA复制和基因表达的多功能蛋白。为了研究DBP的结构与功能之间的关系,对5型和12型血清型(Ad5和Ad12)的氨基酸序列进行了比较。Ad5 DBP的氨基酸序列先前已通过对Ad5 DBP基因的核苷酸序列分析确定(W. Kruijer,F. M. A. Van Schaik,和J. S. Sussenbach,《核酸研究》9,4439 - 4457,1981)。在本研究中,通过测定晚期DBP mRNA中第一个前导序列的序列以及编码100 kDa蛋白的mRNA的三联体前导序列与主体之间的剪接位点,对Ad5 DBP基因及其相邻区域的分析得到了扩展。还描述了Ad12 DBP基因的核苷酸序列。根据Ad12 DBP mRNA的核苷酸序列和RNA图谱数据(I. Saito,J. Sato,H. Handa,K. Shiraki,和H. Shimojo,《病毒学》114,379 - 398,1981),可以推导Ad12 DBP完整的氨基酸序列。Ad12 DBP含有484个氨基酸,实际分子量为54,992。它比Ad5 DBP短45个氨基酸。Ad12和Ad5 DBP氨基酸序列的比较表明,Ad12 DBP的N端125个氨基酸残基中存在几个较长的缺失。相比之下,在Ad12 DBP的C端359个氨基酸中仅发现一个氨基酸缺失和插入。Ad12和Ad5 DBP的N端和C端结构域分别有45%和80%的同源性。这表明DBP的两个结构域受到不同进化压力的影响。对具有改变的DBP基因的各种Ad5突变体的分析表明,C端结构域参与DNA复制和早期基因表达,而N端结构域在猴细胞的晚期基因表达中起作用。结合腺病毒DBP的结构和功能对这些结果进行了讨论。

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