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一种甘露聚糖结合凝集素参与铜绿微囊藻有毒菌株中的细胞间附着。

A mannan binding lectin is involved in cell-cell attachment in a toxic strain of Microcystis aeruginosa.

作者信息

Kehr Jan-Christoph, Zilliges Yvonne, Springer Andreas, Disney Matthew D, Ratner Daniel D, Bouchier Christiane, Seeberger Peter H, de Marsac Nicole Tandeau, Dittmann Elke

机构信息

Humboldt University, Institute of Biology, Department of Molecular Ecology, Chausseestr., 117, 10115 Berlin, Germany.

出版信息

Mol Microbiol. 2006 Feb;59(3):893-906. doi: 10.1111/j.1365-2958.2005.05001.x.

Abstract

Microcystin, a hepatotoxin that represents a serious health risk for humans and livestock, is produced by the bloom-forming cyanobacterium Microcystis aeruginosa in freshwater bodies worldwide. Here we describe the discovery of a lectin, microvirin (MVN), in M. aeruginosa PCC7806 that shares 33% identity with the potent anti-HIV protein cyanovirin-N from Nostoc ellipsosporum. Carbohydrate microarrays were employed to demonstrate the high specificity of the protein for high-mannose structures containing alpha(1-->2) linked mannose residues. Lectin binding analyses and phenotypic characterizations of MVN-deficient mutants suggest that MVN is involved in cell-cell recognition and cell-cell attachment of Microcystis. A binding partner of MVN was identified in the lipopolysaccharide fraction of M. aeruginosa PCC7806. MVN is differentially expressed in mutants lacking the hepatotoxin microcystin. Additionally, MVN-deficient mutants contain much lower amounts of microcystin than the wild-type cells. We discuss a possible functional correlation between microcystin and the lectin and possible implications on Microcystis morphotype formation. This study provides the first experimental evidence that microcystins may have an impact on Microcystis colony formation that is highly important for the competitive advantage of Microcystis over other phytoplankton species.

摘要

微囊藻毒素是一种肝毒素,对人类和牲畜的健康构成严重风险,它由全球淡水水体中形成水华的蓝藻铜绿微囊藻产生。在此,我们描述了在铜绿微囊藻PCC7806中发现的一种凝集素——微病毒素(MVN),它与来自椭圆念珠藻的强效抗HIV蛋白蓝藻素-N有33%的同源性。利用碳水化合物微阵列证明了该蛋白对含有α(1→2)连接甘露糖残基的高甘露糖结构具有高度特异性。对MVN缺陷型突变体的凝集素结合分析和表型特征表明,MVN参与了微囊藻的细胞间识别和细胞间附着。在铜绿微囊藻PCC7806的脂多糖部分鉴定出了MVN的一个结合伙伴。MVN在缺乏肝毒素微囊藻毒素的突变体中差异表达。此外,MVN缺陷型突变体中的微囊藻毒素含量比野生型细胞低得多。我们讨论了微囊藻毒素与凝集素之间可能的功能相关性以及对微囊藻形态型形成的可能影响。这项研究提供了首个实验证据,表明微囊藻毒素可能对微囊藻的群体形成产生影响,而这对微囊藻相对于其他浮游植物物种的竞争优势非常重要。

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