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蛋白质序列同源性研究。VII. 与大肠杆菌L7/L12和L10等效的核糖体蛋白的互补分子协同进化。

Examination of protein sequence homologies. VII. The complementary molecular coevolution of ribosomal proteins equivalent to Escherichia coli L7/L12 and L10.

作者信息

Otaka E, Suzuki K, Hashimoto T

机构信息

Department of Biochemistry and Biophysics, Hiroshima University, Japan.

出版信息

Protein Seq Data Anal. 1990 Mar;3(1):11-9.

PMID:2179947
Abstract

Recently reported P1, P2 and metabacteria line sequences of transposition-type 'A' proteins, equivalent to Escherichia coli ribosomal protein L7/L12, were examined using a correlation method which evaluates the sequence similarity quantitatively. As the sequences could be aligned along the alignment previously constructed for 25 various 'A' proteins, the inclusive alignment further supports the previous claims concerning the rule of "preservation units" and the transpositional regeneration for metabacterial and eukaryotic 'A' proteins. Yeasts contain multispecies of P1 and P2 line genes and their P1 line sequences show low correlation coefficient values compared to other P1 line sequences, indicating a great evolutionary distance between lower and higher eukaryotes. Five sequences of protein P0 from metabacteria, yeast, and human, of which about 20 residues at the C termini are homologous with those of their own transposition-type 'A' proteins, were similarly examined. The N-terminal three-quarters of the sequences align naturally and the first two-thirds of the alignment could involve the E. coli L10 (EL10) sequence. An alignment of the remaining sequences at the C termini was established, relying on the well-matching sequence similarities between the metabacteria 'A' protein and their P0 protein sequences. Finally, the C-terminal halves of P0 protein sequences corresponded with almost overall sequences of the transposition-type 'A' proteins. The gene fusion of a protein might have resulted in the formation of the P0 proteins. A coupling of this gene fusion and the transposition of prototype 'A' proteins may have given rise to the complementary molecular transformations required for the development toward higher organism cells.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

最近报道的转座型“A”蛋白的P1、P2和元细菌系序列,等同于大肠杆菌核糖体蛋白L7/L12,使用一种定量评估序列相似性的相关方法进行了检测。由于这些序列可以沿着先前为25种不同“A”蛋白构建的比对进行排列,这种包容性比对进一步支持了先前关于“保存单位”规则以及元细菌和真核“A”蛋白转座再生的说法。酵母含有多种P1和P2系基因,与其他P1系序列相比,它们的P1系序列显示出较低的相关系数值,这表明低等和高等真核生物之间存在很大的进化距离。对来自元细菌、酵母和人类的蛋白质P0的五个序列进行了类似检测,这些序列的C末端约20个残基与其自身的转座型“A”蛋白的残基同源。序列的N端四分之三自然对齐,并且对齐的前三分之二可能涉及大肠杆菌L10(EL10)序列。依靠元细菌“A”蛋白与其P0蛋白序列之间良好匹配的序列相似性,建立了C末端其余序列的比对。最后,P0蛋白序列的C末端一半几乎与转座型“A”蛋白的整个序列相对应。蛋白质的基因融合可能导致了P0蛋白的形成。这种基因融合与原型“A”蛋白的转座相结合,可能产生了向高等生物细胞发育所需的互补分子转变。(摘要截短于250字)

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