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鸟嘌呤脱氨酶的系统发育分析与分子进化:从鸟嘌呤到树突

Phylogenetic analysis and molecular evolution of guanine deaminases: from guanine to dendrites.

作者信息

Fernández José R, Byrne Bruce, Firestein Bonnie L

机构信息

Department of Cell Biology and Neuroscience, Rutgers, The State University of New Jersey, Nelson Biological Laboratories, 604 Allison Road, Piscataway, NJ 08854-8082, USA.

出版信息

J Mol Evol. 2009 Mar;68(3):227-35. doi: 10.1007/s00239-009-9205-x. Epub 2009 Feb 17.

Abstract

Guanine deaminase (GDA; guanase) is a ubiquitous enzyme that catalyzes the first step of purine metabolism by hydrolytic deamination of guanine, resulting in the production of xanthine. This hydrolase subfamily member plays an essential role in maintaining homeostasis of cellular triphosphate nucleotides for energy, signal transduction pathways, and nitrogen sources. In mammals, GDA protein levels can play a role in neuronal development by regulating dendritic arborization. We previously demonstrated that the most abundant alternative splice form of GDA in mammals, termed cypin (cytosolic PSD-95 interactor), interacts with postsynaptic density proteins, regulates microtubule polymerization, and increases dendrite number. Since purine metabolism and dendrite development were previously thought to be independent cellular processes, this multifunctional protein serves as a new target for the treatment of cognitive disorders characterized by aberrant neuronal morphology and purine metabolism. Although the enzymatic activity of GDA has been conserved during evolution from prokaryotes to higher eukaryotes, a detailed evolutionary assessment of the principal domains in GDA proteins has not yet been put forward. In this study, we perform a complete evolutionary analysis of the full-length sequences and the principal domains in guanine deaminases. Furthermore, we reconstruct the molecular phylogeny of guanine deaminases with neighbor-joining, maximum-likelihood, and UPGMA methods of phylogenetic inference. This study can act as a model whereby a universal housekeeping enzyme may be adapted to act also as a key regulator of a developmental process.

摘要

鸟嘌呤脱氨酶(GDA;鸟嘌呤酶)是一种普遍存在的酶,它通过鸟嘌呤的水解脱氨作用催化嘌呤代谢的第一步,产生黄嘌呤。这个水解酶亚家族成员在维持细胞三磷酸核苷酸的能量、信号转导途径和氮源的内稳态中起着至关重要的作用。在哺乳动物中,GDA蛋白水平可通过调节树突分支在神经元发育中发挥作用。我们之前证明,哺乳动物中最丰富的GDA可变剪接形式,称为cypin(胞质PSD - 95相互作用蛋白),与突触后致密蛋白相互作用,调节微管聚合,并增加树突数量。由于嘌呤代谢和树突发育以前被认为是独立的细胞过程,这种多功能蛋白成为治疗以异常神经元形态和嘌呤代谢为特征的认知障碍的新靶点。尽管GDA的酶活性在从原核生物到高等真核生物的进化过程中一直保守,但尚未对GDA蛋白的主要结构域进行详细的进化评估。在本研究中,我们对鸟嘌呤脱氨酶的全长序列和主要结构域进行了完整的进化分析。此外,我们用邻接法、最大似然法和UPGMA系统发育推断方法重建了鸟嘌呤脱氨酶的分子系统发育。这项研究可以作为一个模型,说明一种普遍的管家酶如何也能适应成为一个发育过程的关键调节因子。

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