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源自克隆cDNA的人核糖体蛋白S6的一级结构。

The primary structure of the human ribosomal protein S6 derived from a cloned cDNA.

作者信息

Heinze H, Arnold H H, Fischer D, Kruppa J

机构信息

Fraunhofer Institute for Toxicology and Aerosol Research, Hannover, Federal Republic of Germany.

出版信息

J Biol Chem. 1988 Mar 25;263(9):4139-44.

PMID:3279029
Abstract

Polyclonal antibodies directed against a synthetic octapeptide of the cAMP-dependent phosphorylation site of the ribosomal protein S6 of rat liver were used to screen a lambda gt11 cDNA expression library of human lymphoblasts. An S6 specific clone was isolated. It consists of the complete coding sequence of 747 base pairs and the 3' noncoding region of 40 base pairs. The sequence of 249 amino acids was deduced from the nucleotide sequence. The amino- and carboxyl-terminal regions are almost identical to the reported partial peptide sequences of rat liver S6. The yeast protein S10 is homologous to the human S6 with the exception of 3 amino acid insertions and a carboxyl-terminal extension of 10 amino acids within the human S6. The only two phosphorylation sites at the carboxyl terminus of yeast S10 are homologous to the two cAMP-dependent sites in human S6. Since there are additional phosphorylation sites in mammalian S6, one can assume that they are located in the cluster of 5 serines within the carboxyl-terminal extension. The sequence comparison of these two ribosomal proteins from evolutionarily distant eucaryotes, such as man and yeast, indicates that the structure and probably the function of the phosphoprotein S6 of the small ribosomal subunit has been highly conserved. The expression of the S6 gene has been investigated in proliferating lymphocytes stimulated by concanavalin A. During all stages of lymphoblast development the level of S6 mRNA appeared to be similar. Southern blot analysis of human genomic DNA suggests that multiple genes exist for the S6 protein.

摘要

用针对大鼠肝脏核糖体蛋白S6的cAMP依赖性磷酸化位点的合成八肽的多克隆抗体筛选人淋巴母细胞的λgt11 cDNA表达文库。分离出一个S6特异性克隆。它由747个碱基对的完整编码序列和40个碱基对的3'非编码区组成。从核苷酸序列推导了249个氨基酸的序列。氨基末端和羧基末端区域与报道的大鼠肝脏S6的部分肽序列几乎相同。酵母蛋白S10与人S6同源,只是人S6中有3个氨基酸插入和羧基末端延伸10个氨基酸。酵母S10羧基末端仅有的两个磷酸化位点与人S6中的两个cAMP依赖性位点同源。由于哺乳动物S6中还有其他磷酸化位点,可以推测它们位于羧基末端延伸区内的5个丝氨酸簇中。对来自进化上距离较远的真核生物(如人和酵母)的这两种核糖体蛋白的序列比较表明,小核糖体亚基的磷蛋白S6的结构以及可能的功能已经高度保守。在伴刀豆球蛋白A刺激的增殖淋巴细胞中研究了S6基因的表达。在淋巴母细胞发育的所有阶段,S6 mRNA的水平似乎相似。人基因组DNA的Southern印迹分析表明,S6蛋白存在多个基因。

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