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石鱼毒素是一种来自玫瑰毒鲉毒液的新型致死因子。cDNA克隆及特性分析。

Stonustoxin is a novel lethal factor from stonefish (Synanceja horrida) venom. cDNA cloning and characterization.

作者信息

Ghadessy F J, Chen D, Kini R M, Chung M C, Jeyaseelan K, Khoo H E, Yuen R

机构信息

Department of Biochemistry, Faculty of Medicine, National University of Singapore, 10 Kent Ridge Crescent, Singapore 119260, USA.

出版信息

J Biol Chem. 1996 Oct 11;271(41):25575-81. doi: 10.1074/jbc.271.41.25575.

Abstract

Stonustoxin (SNTX) is a multifunctional lethal protein isolated from venom elaborated by the stonefish, Synanceja horrida. It comprises two subunits, termed alpha and beta, which have respective molecular masses of 71 and 79 kDa. SNTX elicits an array of biological responses both in vitro and in vivo, particularly a potent hypotension that appears to be mediated by the nitric oxide pathway. As a prelude to structure-function studies, we have isolated and sequenced cDNA clones encoding the alpha- and beta-subunits of SNTX from a venom gland cDNA library. The deduced amino acid sequence of neither subunit shows significant homology with any known protein. Protein sequence alignment does, however, show the subunits to be 50% homologous to each other and implies that they may have arisen from a common ancestor. The subunits of this novel toxin lack typical N-terminal signal sequences commonly found in proteins that are secreted via the endoplasmic reticulum-Golgi apparatus pathway, indicating the possibility of its being secreted by a non-classical pathway, which is not clearly understood. The SNTX subunits have been expressed in Escherichia coli as cleavable fusion proteins that cross-react with antibodies raised against the native toxin. To the best of our knowledge, this is the first complete sequence of a fish-derived protein toxin to be reported.

摘要

石鱼毒素(SNTX)是一种从毒鲉(Synanceja horrida)分泌的毒液中分离出的多功能致死蛋白。它由两个亚基组成,分别称为α和β,分子量分别为71 kDa和79 kDa。SNTX在体外和体内均可引发一系列生物学反应,尤其是一种明显由一氧化氮途径介导的强效低血压。作为结构 - 功能研究的前奏,我们从毒腺cDNA文库中分离并测序了编码SNTXα和β亚基的cDNA克隆。两个亚基的推导氨基酸序列与任何已知蛋白质均无显著同源性。然而,蛋白质序列比对显示这两个亚基彼此同源性为50%,这意味着它们可能起源于共同的祖先。这种新型毒素的亚基缺乏通常在通过内质网 - 高尔基体途径分泌的蛋白质中发现的典型N端信号序列,这表明其可能通过一种尚不清楚的非经典途径分泌。SNTX亚基已在大肠杆菌中作为可切割的融合蛋白表达,该融合蛋白可与针对天然毒素产生的抗体发生交叉反应。据我们所知,这是首次报道的鱼类来源蛋白毒素的完整序列。

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