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重组对虾抗菌肽penaeidin-3的溶液结构

Solution structure of the recombinant penaeidin-3, a shrimp antimicrobial peptide.

作者信息

Yang Yinshan, Poncet Joël, Garnier Julien, Zatylny Céline, Bachère Evelyne, Aumelas André

机构信息

Centre de Biochimie Structurale, CNRS UMR 5048, INSERM U414, Université Montpellier 1, Faculté de Pharmacie, 15 avenue Charles Flahault, 34093 Montpellier Cedex 5, France.

出版信息

J Biol Chem. 2003 Sep 19;278(38):36859-67. doi: 10.1074/jbc.M305450200. Epub 2003 Jul 3.

DOI:10.1074/jbc.M305450200
PMID:12842879
Abstract

Penaeidins are a family of antimicrobial peptides of 47-63 residues isolated from several species of shrimp. These peptides display a proline-rich domain (N-terminal part) and a cysteine-rich domain (C-terminal part) stabilized by three conserved disulfide bonds whose arrangement has not yet been characterized. The recombinant penaeidin-3a of Litopenaeus vannamei (63 residues) and its [T8A]-Pen-3a analogue were produced in Saccharomyces cerevisiae and showed similar antimicrobial activity. The solution structure of the [T8A]-Pen-3a analogue was determined by using two-dimensional 1H NMR and simulated annealing calculations. The proline-rich domain, spanning residues 1-28 was found to be unconstrained. In contrast, the cysteine-rich domain, spanning residues 29-58, displays a well defined structure, which consists of an amphipathic helix (41-50) linked to the upstream and the downstream coils by two disulfide bonds (Cys32-Cys47 and Cys48-Cys55). These two coils are in turn linked together by the third disulfide bond (Cys36-Cys54). Such a disulfide bond packing, which is in agreement with the analysis of trypsin digests by ESI-MS, contributes to the highly hydrophobic core. Side chains of Arg45 and Arg50, which belong to the helix, and side chains of Arg37 and Arg53, which belong to the upstream and the downstream coils, are located in two opposite parts of this globular and compact structure. The environment of these positively charged residues, either by hydrophobic clusters at the surface of the cysteine-rich domain or by sequential hydrophobic residues in the unconstrained proline-rich domain, gives rise to the amphipathic character required for antimicrobial peptides. We hypothesize that the antimicrobial activity of penaeidins can be explained by a cooperative effect between the proline-rich and cysteine-rich features simultaneously present in their sequences.

摘要

对虾抗菌肽是从几种虾中分离出的一类由47至63个残基组成的抗菌肽。这些肽具有一个富含脯氨酸的结构域(N端部分)和一个富含半胱氨酸的结构域(C端部分),后者由三个保守的二硫键稳定,但其排列方式尚未得到表征。凡纳滨对虾的重组对虾抗菌肽-3a(63个残基)及其[T8A]-Pen-3a类似物在酿酒酵母中产生,并表现出相似的抗菌活性。通过二维1H NMR和模拟退火计算确定了[T8A]-Pen-3a类似物的溶液结构。发现跨越残基1至28的富含脯氨酸的结构域不受限制。相反,跨越残基29至58的富含半胱氨酸的结构域呈现出明确的结构,它由一个两亲性螺旋(41至50)通过两个二硫键(Cys32-Cys47和Cys48-Cys55)与上游和下游的螺旋相连组成。这两个螺旋又通过第三个二硫键(Cys36-Cys54)连接在一起。这种二硫键的排列方式与通过电喷雾电离质谱对胰蛋白酶消化产物的分析结果一致,有助于形成高度疏水的核心。属于螺旋的Arg45和Arg50的侧链,以及属于上游和下游螺旋的Arg37和Arg53的侧链,位于这个球状紧密结构的两个相对部分。这些带正电荷残基的环境,要么通过富含半胱氨酸结构域表面的疏水簇,要么通过无限制的富含脯氨酸结构域中的连续疏水残基,产生了抗菌肽所需的两亲性特征。我们假设对虾抗菌肽的抗菌活性可以通过其序列中同时存在的富含脯氨酸和富含半胱氨酸特征之间的协同作用来解释。

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