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去酪氨酸化α-微管蛋白的羧基末端肽提供了一个用于研究微管蛋白酪氨酸连接酶底物特异性的最小系统。

The carboxy-terminal peptide of detyrosinated alpha tubulin provides a minimal system to study the substrate specificity of tubulin-tyrosine ligase.

作者信息

Rüdiger M, Wehland J, Weber K

机构信息

Max-Planck-Institute for Biophysical Chemistry, Department of Biochemistry, Göttingen, Germany.

出版信息

Eur J Biochem. 1994 Mar 1;220(2):309-20. doi: 10.1111/j.1432-1033.1994.tb18627.x.

DOI:10.1111/j.1432-1033.1994.tb18627.x
PMID:7510228
Abstract

The ATP-dependent tubulin-tyrosine ligase (TTL) restores the carboxy-terminal tyrosine of alpha tubulin in alpha beta tubulin that has been previously detyrosinated. Here we show that the carboxy-terminal tetradecapeptide of detyrosinated alpha tubulin is used by TTL as a substrate, albeit at 50-fold lower efficiency than alpha beta tubulin. The minimal system provided by the TTL/peptide combination mirrors the TTL/tubulin system in all aspects tested, and shows a pronounced substrate inhibition. Synthetic peptides varying in length and/or containing single amino acid replacements were used to analyze the TTL specificity for the carboxy-terminal sequence of detyrosinated alpha tubulin. Peptides ending like alpha tubulin with the sequence Gly-Glu-Glu are optimally tyrosinated once a peptide length of 12 residues is reached. Position -1 of this recognition sequence, to which the tyrosine is added, must be glutamic acid. Position -2 accepts only an acidic amino acid but glutamic acid is by far preferred over aspartic acid. These results explain why a subpopulation of brain alpha tubulin, which ends with the sequence Gly-Glu, is not tyrosinated by TTL. The carboxy-terminal dodecapeptide of brain alpha tubulin with its polyglutamyl side-chain on position -6 shows the same substrate activity as the corresponding synthetic peptide lacking the side-chain. We discuss the substrate specificity of TTL for different alpha tubulins and speculate why tubulin is a better substrate than the optimal peptide covering the carboxy-terminal of detyrosinated alpha tubulin.

摘要

ATP 依赖性微管蛋白 - 酪氨酸连接酶(TTL)可恢复先前已去酪氨酸化的αβ微管蛋白中α微管蛋白的羧基末端酪氨酸。在此我们表明,去酪氨酸化的α微管蛋白的羧基末端十四肽被 TTL 用作底物,尽管其效率比αβ微管蛋白低 50 倍。TTL/肽组合所提供的最小系统在所有测试方面都反映了 TTL/微管蛋白系统,并表现出明显的底物抑制作用。使用长度不同和/或含有单个氨基酸替换的合成肽来分析 TTL 对去酪氨酸化的α微管蛋白羧基末端序列的特异性。一旦肽长度达到 12 个残基,以 Gly-Glu-Glu 序列结尾的类似α微管蛋白的肽就会被最佳酪氨酸化。添加酪氨酸的这个识别序列的 -1 位必须是谷氨酸。-2 位仅接受酸性氨基酸,但谷氨酸远比天冬氨酸更受青睐。这些结果解释了为什么以 Gly-Glu 序列结尾的脑α微管蛋白亚群不会被 TTL 酪氨酸化。脑α微管蛋白的羧基末端十二肽在 -6 位带有聚谷氨酰侧链,其底物活性与缺乏该侧链的相应合成肽相同。我们讨论了 TTL 对不同α微管蛋白的底物特异性,并推测为什么微管蛋白是比覆盖去酪氨酸化的α微管蛋白羧基末端的最佳肽更好的底物。

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