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来自食鱼蝮蛇毒液的赖氨酸-49磷脂酶A2。其结构和功能与其他磷脂酶A2的关系。

The lysine-49 phospholipase A2 from the venom of Agkistrodon piscivorus piscivorus. Relation of structure and function to other phospholipases A2.

作者信息

Maraganore J M, Heinrikson R L

出版信息

J Biol Chem. 1986 Apr 15;261(11):4797-804.

PMID:3082870
Abstract

A new class of phospholipases A2 that have a lysine at position 49 differ from the more conventional Asp-49 enzymes with respect to the sequential binding of the essential cofactor, calcium, and the substrate, phospholipid, in the formation of the catalytic complex (Maraganore, J.M., Merutka, G., Cho, W., Welches, W., Kézdy, F.J., and Heinrikson, R.L. (1984) J. Biol. Chem. 259, 13839-13843). We report here the complete amino acid sequence of the Lys-49 enzyme from Agkistrodon piscivorus piscivorus. The sequence was determined by automated Edman degradation of the intact, S-carboxymethylcysteinyl protein and of peptides derived therefrom by cleavage with cyanogen bromide, chymotrypsin, trypsin, and endoproteinase Lys-C. Despite several changes at amino acid residues previously considered to be invariant, the Lys-49 enzymes are homologous to the Asp-49 phospholipases. Homology is especially apparent in the following: 1) the pattern of 14 half-cystine residues, 2) conservation of hydrophobic residues which have been shown to encircle the active site, and 3) conservation of Asp-99 and His-48 which have been implicated in the catalytic reaction itself. These observations together with kinetic and binding data imply that the Lys-49 phospholipases have a catalytic mechanism and a three-dimensional architecture similar to those of the Asp-49 enzymes. Modeling of the Lys-49 enzyme based upon the structure of bovine pancreatic phospholipase reveals that the epsilon-amino group of Lys-49 can fit easily in the calcium-binding site and, moreover, that this orientation of a cationic side chain at position 49 could account for the characteristic and novel feature of the Lys-49 phospholipases, i.e. that they are able to form complexes with phospholipid in the absence of calcium.

摘要

一类在第49位氨基酸残基为赖氨酸的新型磷脂酶A2,在催化复合物形成过程中,与更为常见的第49位天冬氨酸的酶在必需辅因子钙和底物磷脂的顺序结合方面存在差异(Maraganore, J.M., Merutka, G., Cho, W., Welches, W., Kézdy, F.J., and Heinrikson, R.L. (1984) J. Biol. Chem. 259, 13839 - 13843)。我们在此报告来自食鱼蝮蛇(Agkistrodon piscivorus piscivorus)的第49位赖氨酸的酶的完整氨基酸序列。该序列通过对完整的S - 羧甲基半胱氨酰化蛋白质以及用溴化氰、胰凝乳蛋白酶、胰蛋白酶和内肽酶Lys - C切割产生的肽段进行自动Edman降解来确定。尽管先前认为不变的氨基酸残基有几处变化,但第49位赖氨酸的酶与第49位天冬氨酸的磷脂酶是同源的。同源性在以下方面尤为明显:1)14个半胱氨酸残基的模式;2)已证明环绕活性位点的疏水残基的保守性;3)参与催化反应本身的天冬氨酸 - 99和组氨酸 - 48的保守性。这些观察结果连同动力学和结合数据表明,第49位赖氨酸的磷脂酶具有与第49位天冬氨酸的酶相似的催化机制和三维结构。基于牛胰磷脂酶结构对第49位赖氨酸的酶进行建模显示,第49位赖氨酸的ε - 氨基可以轻松地适配于钙结合位点,而且,第49位阳离子侧链的这种取向可以解释第49位赖氨酸的磷脂酶的特征性和新颖特性,即它们能够在没有钙的情况下与磷脂形成复合物。

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