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脂质生物合成蛋白家族及磷脂结构变异分析

Analysis of a lipid biosynthesis protein family and phospholipid structural variations.

作者信息

Tanaka Michihiro, Moriya Yuki, Goto Susumu, Kanehisa Minoru

机构信息

Bioinformatics Center, Institute for Chemical Research, Kyoto University, Uji, Kyoto 611-0011, Japan.

出版信息

Genome Inform. 2010 Jan;22:191-201.

Abstract

Glycerophospholipids are major structural lipids in cellular membrane systems and play key roles as suppliers of the first and second messengers in the signal transduction and molecular recognition processes. The distribution of lipid components differs among organelles and cells. The distribution is controlled by two pathways in lipid metabolism: de nova and remodeling pathways. Glycerophospholipids including arachidonic and stearic acids are mostly produced in the remodeling pathway, whereas lipid chains are reconstructed from those synthesized in the de novo pathway. Recently lysophospholipid acyltransferases have been isolated as key enzymes in the remodeling pathway, and the substrate specificity has been investigated in terms of the chemical substructures of glycerophospholipids, such as the type of head groups and the length of aliphatic chains. These experimental studies have been reported for specific organisms, and only two representative sequence motifs are known for acyltransferases: a general pattern and the pattern for membrane-bound O-acyltransferase (MBOAT). Here we attempt to correlate the sequence patterns and the substrate specificity of lysophospholipid acyltransferases in 89 eukaryotic genomes in order to understand the roles of this enzyme family and underlying glycerophospholipid structural variations. Using phylogenetic and domain analyses, the lysophospholipid acyltransferase family was divided into 18 subtypes. Furthermore, we examined the occurrence of identified subtypes in eukaryotic genomes, and found the expansion of these subtypes in vertebrates. These findings may provide clues to understanding structural variations and distributions of glycerophospholipids in different organisms.

摘要

甘油磷脂是细胞膜系统中的主要结构脂质,在信号转导和分子识别过程中作为第一和第二信使的供应者发挥关键作用。脂质成分在细胞器和细胞之间的分布有所不同。这种分布由脂质代谢中的两条途径控制:从头合成途径和重塑途径。包括花生四烯酸和硬脂酸在内的甘油磷脂大多在重塑途径中产生,而脂质链则由从头合成途径中合成的脂质链重建而来。最近,溶血磷脂酰转移酶已被分离出来,作为重塑途径中的关键酶,并且已经根据甘油磷脂的化学亚结构,如头部基团的类型和脂肪链的长度,对其底物特异性进行了研究。这些实验研究是针对特定生物体进行报道的,并且对于酰基转移酶仅知道两种代表性的序列基序:一种通用模式和膜结合O-酰基转移酶(MBOAT)的模式。在这里,我们试图关联89个真核生物基因组中溶血磷脂酰转移酶的序列模式和底物特异性,以了解该酶家族的作用以及潜在的甘油磷脂结构变异。通过系统发育和结构域分析,溶血磷脂酰转移酶家族被分为18个亚型。此外,我们研究了已鉴定亚型在真核生物基因组中的出现情况,发现这些亚型在脊椎动物中有所扩展。这些发现可能为理解不同生物体中甘油磷脂的结构变异和分布提供线索。

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