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关于无脊椎动物激肽原的首次报道。

The first report of kininogen from invertebrates.

作者信息

Zhou Zuohong, Yang Hailong, Xu Xueqing, Wang Xu, Lai Ren

机构信息

Key Laboratory of Microbiological Engineering of Agricultural Environment, Ministry of Agriculture, Life Sciences College of Nanjing Agricultural University, Nanjing, Jiangsu 210095, China.

出版信息

Biochem Biophys Res Commun. 2006 Sep 8;347(4):1099-102. doi: 10.1016/j.bbrc.2006.07.024. Epub 2006 Jul 14.

Abstract

The hornet possesses highly toxic venom, which is rich in toxin, enzymes, and biologically active peptides. Several bradykinin-like peptides, vespakinins, have been found in wasp venoms since 1970s, but the mode of biosynthesis of these peptides is unknown. In the present study, a vespakinin M was purified from venom of Vespa magnifica. Its primary sequence was established as GRPPGFSPFRID. The cDNA encoding the vespakinin M was cloned from the cDNA library of V. magnifica venom gland. The cDNA structure of vespakinin M was found to contain a coding region of 168 nucleotides. The encoded precursor of vespakinin M is composed of a signal peptide, an acidic peptide, and a mature peptide of vespakinin M. This is the first kininogen from insects; it is also the first kininogen from invertebrates. The cDNA structure encoding vespakinin M suggests that the generation mode of bradykinin-related peptides in wasp is different from amphibian skin and mammalian blood system.

摘要

黄蜂拥有剧毒毒液,其富含毒素、酶和生物活性肽。自20世纪70年代以来,在黄蜂毒液中发现了几种类缓激肽肽,即黄蜂激肽,但这些肽的生物合成模式尚不清楚。在本研究中,从大胡蜂毒液中纯化出一种黄蜂激肽M。其一级序列确定为GRPPGFSPFRID。编码黄蜂激肽M的cDNA从大胡蜂毒腺的cDNA文库中克隆得到。发现黄蜂激肽M的cDNA结构包含一个168个核苷酸的编码区。编码的黄蜂激肽M前体由一个信号肽、一个酸性肽和一个黄蜂激肽M成熟肽组成。这是昆虫中的首个激肽原;也是无脊椎动物中的首个激肽原。编码黄蜂激肽M的cDNA结构表明,黄蜂中缓激肽相关肽的产生模式不同于两栖动物皮肤和哺乳动物血液系统。

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