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通过逻辑回归分析和内在无序检查揭示的转谷氨酰胺酶2的底物偏好

Substrate preference of transglutaminase 2 revealed by logistic regression analysis and intrinsic disorder examination.

作者信息

Csosz Eva, Bagossi Peter, Nagy Zoltan, Dosztanyi Zsuzsanna, Simon Istvan, Fesus Laszlo

机构信息

Department of Biochemistry and Molecular Biology, University of Debrecen, Egyetem ter 1, Life Science Building, 4010 Debrecen, Hungary.

出版信息

J Mol Biol. 2008 Nov 7;383(2):390-402. doi: 10.1016/j.jmb.2008.08.026. Epub 2008 Aug 22.

Abstract

Tissue transglutaminase (TG2) catalyzes the Ca(2+)-dependent posttranslational modification of proteins via formation of isopeptide bonds between their glutamine and lysine residues. Although substrate specificity of TG2 has been studied repeatedly at the sequence level, no clear consensus sequences have been determined so far. With the use of the extensive structural information on TG2 substrate proteins listed in TRANSDAB Wiki database, a slight preference of TG2 for glutamine and lysine residues situated in turns could be observed. When the spatial environment of the favored glutamine and lysine residues was analyzed with logistic regression, the presence of specific amino acid patterns was identified. By using the occurrence of the predictor amino acids as selection criteria, several polypeptides were predicted and later identified as novel in vitro substrates for TG2. By studying the sequence of TG2 substrate proteins lacking available crystal structure, the strong favorable influence on substrate selection of the presence of substrate glutamine and lysine residues in intrinsically disordered regions could also be revealed. The collected structural data have provided novel understanding of how this versatile enzyme selects its substrates in various cell compartments and tissues.

摘要

组织转谷氨酰胺酶(TG2)通过在蛋白质的谷氨酰胺和赖氨酸残基之间形成异肽键来催化Ca(2+)依赖的蛋白质翻译后修饰。尽管TG2的底物特异性已在序列水平上被反复研究,但到目前为止尚未确定明确的共有序列。利用TRANSDAB Wiki数据库中列出的关于TG2底物蛋白的大量结构信息,可以观察到TG2对位于转角处的谷氨酰胺和赖氨酸残基有轻微偏好。当用逻辑回归分析有利的谷氨酰胺和赖氨酸残基的空间环境时,确定了特定氨基酸模式的存在。通过将预测氨基酸的出现作为选择标准,预测了几种多肽,随后将其鉴定为TG2的新型体外底物。通过研究缺乏可用晶体结构的TG2底物蛋白的序列,还可以揭示内在无序区域中底物谷氨酰胺和赖氨酸残基的存在对底物选择的强烈有利影响。收集到的结构数据为这种多功能酶如何在各种细胞区室和组织中选择其底物提供了新的认识。

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