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一种新型蓝藻 Nostocyclopeptide 是一种针对微囊藻毒素的有效解毒剂。

A novel cyanobacterial nostocyclopeptide is a potent antitoxin against microcystins.

机构信息

Department of Food and Environmental Sciences, Division of Microbiology, University of Helsinki, P. O. Box 56, 00014 Helsinki, Finland.

出版信息

Chembiochem. 2010 Jul 26;11(11):1594-9. doi: 10.1002/cbic.201000179.

DOI:10.1002/cbic.201000179
PMID:20575133
Abstract

Cyanobacterial hepatotoxins (microcystins and nodularins) cause numerous animal poisonings worldwide each year and are threats to human health. However, we found that extracts from several cyanobacteria isolates failed to induce hepatotoxicity even if they contained high concentrations of the liver toxin microcystin. The antitoxic activity abolishes all morphological hallmarks of microcystin-induced apoptosis, and therefore invalidates cell-based assays of the microcystin content of bloom-forming cyanobacteria. The antitoxin was purified from a cyanobacterial isolate (Nostoc sp. XSPORK 13A) from the Baltic Sea, and the activity was shown to reside in a novel cyclic peptide of the nostocyclopeptide family (nostocyclopeptide M1, Ncp-M1) that consists of seven amino acids (Tyr1-Tyr2-D-HSe3-L-Pro4-L-Val5-(2S,4S)-4-MPr6-Tyr7; MW=881) with an imino linkage between Tyr1 and Tyr7. Ncp-M1 did not compete with labelled microcystin for binding to protein phosphatase 2A; this explains why the antitoxin did not interfere with phosphatase-based microcystin assays. Currently used agents that interfere with microcystin action, such as inhibitors of ROS formation, microcystin uptake and Cam-kinase activity, are themselves inherently toxic. Since Ncp-M1 is potent and nontoxic it promises to become a useful mechanistic tool as soon as its exact cellular target is elucidated.

摘要

蓝藻肝毒素(微囊藻毒素和节球藻毒素)每年在全球范围内导致许多动物中毒,对人类健康构成威胁。然而,我们发现,即使含有高浓度肝毒素微囊藻毒素,来自几种蓝藻分离物的提取物也未能引起肝毒性。这种抗毒素消除了微囊藻诱导的细胞凋亡的所有形态学特征,因此使基于细胞的蓝藻藻华形成微囊藻毒素含量的测定无效。该抗毒素从波罗的海的蓝藻分离物(念珠藻属 XSPORK 13A)中纯化而来,其活性被证明存在于一种新型的环肽家族( Nostocyclopeptide M1,Ncp-M1)中,由七个氨基酸(Tyr1-Tyr2-D-HSe3-L-Pro4-L-Val5-(2S,4S)-4-MPr6-Tyr7;MW=881)组成, Tyr1 和 Tyr7 之间存在亚氨基键。Ncp-M1 不与标记的微囊藻毒素竞争与蛋白磷酸酶 2A 的结合;这解释了为什么抗毒素不干扰基于磷酸酶的微囊藻毒素测定。目前用于干扰微囊藻毒素作用的试剂,如 ROS 形成抑制剂、微囊藻毒素摄取抑制剂和 Cam-激酶活性抑制剂,本身就具有内在毒性。由于 Ncp-M1 既有效又无毒,因此一旦确定其确切的细胞靶标,它有望成为一种有用的机制工具。

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