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从海葵 U. crassicornis 中分离得到的一种新的磷脂酶 A2-其一级结构和系统发育分类。

A new phospholipase A2 isolated from the sea anemone Urticina crassicornis - its primary structure and phylogenetic classification.

机构信息

Biotechnical Faculty, Department of Biology, University of Ljubljana, Slovenia.

出版信息

FEBS J. 2010 Jun;277(12):2641-53. doi: 10.1111/j.1742-464X.2010.07674.x.

Abstract

Disulfide pairings and active site residues are highly conserved in secretory phospholipases A(2) (PLA(2)s). However, secretory PLA(2)s of marine invertebrates display some distinctive structural features. In this study, we report the isolation and characterization of a PLA(2) from the northern Pacific sea anemone, Urticina crassicornis (UcPLA(2)), containing a C27N substitution and a truncated C-terminal sequence. This novel cnidarian PLA(2) shares about 60% identity and almost 70% homology with two putative PLA(2)s identified in the starlet sea anemone (Nematostella vectensis) genome project. UcPLA(2) lacks hemolytic and neurotoxic activities. A search of available sequences revealed that Asn27-'type' PLA(2)s are present in a few other marine animal species, including some vertebrates. The possibility that the C27N replacement represents a structural adaptation for PLA(2) digestion/activity in the marine environment was not supported by experiments testing the influence of ionic strength on UcPLA(2) enzymatic activity. Because of the highly divergent sequences among invertebrate group I PLA(2)s, it is currently not possible to identify orthologous relationships. As the Asn27-containing PLA(2)s are scattered among the other invertebrate group I PLA(2)s, they do not constitute a new, monophyletic PLA(2) clade.

摘要

二硫键配对和活性位点残基在分泌型磷脂酶 A2(PLA2)中高度保守。然而,海洋无脊椎动物的分泌型 PLA2 显示出一些独特的结构特征。在这项研究中,我们报告了从北太平洋海葵(Urticina crassicornis)中分离和鉴定的 PLA2(UcPLA2),其含有 C27N 取代和截断的 C 末端序列。这种新型刺胞动物 PLA2 与在星状海葵(Nematostella vectensis)基因组计划中鉴定的两种假定的 PLA2 具有约 60%的同一性和近 70%的同源性。UcPLA2 缺乏溶血和神经毒性活性。对现有序列的搜索表明,Asn27-‘型’PLA2 存在于其他一些海洋动物物种中,包括一些脊椎动物。C27N 取代是否代表 PLA2 在海洋环境中消化/活性的结构适应的可能性,通过测试离子强度对 UcPLA2 酶活性的影响的实验未得到支持。由于无脊椎动物组 I PLA2 之间的序列高度分化,目前无法识别同源关系。由于含有 Asn27 的 PLA2 分散在其他无脊椎动物组 I PLA2 中,它们不构成一个新的、单系的 PLA2 分支。

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