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兔脑炎微孢子虫假定的几丁质脱乙酰酶:一种与微孢子虫孢子壁形成有关的表面蛋白。

The putative chitin deacetylase of Encephalitozoon cuniculi: a surface protein implicated in microsporidian spore-wall formation.

作者信息

Brosson Damien, Kuhn Lauriane, Prensier Gérard, Vivarès Christian P, Texier Catherine

机构信息

Equipe Parasitologie Moléculaire et Cellulaire, LBP, UMR CNRS 6023, Université Blaise Pascal, Aubière, France.

出版信息

FEMS Microbiol Lett. 2005 Jun 1;247(1):81-90. doi: 10.1016/j.femsle.2005.04.031.

DOI:10.1016/j.femsle.2005.04.031
PMID:15927751
Abstract

Microsporidia are fungal-like unicellular eukaryotes which develop as obligate intracellular parasites. They differentiate into resistant spores that are protected by a thick cell wall composed of glycoproteins and chitin. Despite an extensive description of the fibrillar structure of this wall, very little is known about its protein components and deposit mechanisms. In this study on the human pathogen Encephalitozoon cuniculi, we identify by mass spectrometry the target of polyclonal antibodies previously raised against a 33-kDa protein located at the outer face of the parasite plasma membrane. This 254-amino acid protein is encoded by the ECU11_0510 open reading frame and presents two isoforms of 33 and 55 kDa. Sequence analysis supports an assignment to the polysaccharide deacetylase family with a suspected chitin deacetylase activity (EcCDA). As demonstrated by TEM studies, EcCDA is present at the plasma membrane of the early stages of E. cuniculi life-cycle. At the sporoblast stage, the enzyme accumulates especially in paramural bodies which are convolutions of the plasma membrane opened to the wall. The identification of an EcCDA homologue in the insect parasite Antonospora locustae (ex Nosema locustae) suggests a widespread distribution of this enzyme among Microsporidia. This characterization of a new microsporidian surface protein creates new perspectives to understand spore wall formation and spore resistance.

摘要

微孢子虫是类似真菌的单细胞真核生物,作为专性细胞内寄生虫生长。它们分化为抗性孢子,这些孢子由糖蛋白和几丁质组成的厚细胞壁保护。尽管对这种壁的纤维状结构已有广泛描述,但对其蛋白质成分和沉积机制却知之甚少。在这项针对人类病原体兔脑炎微孢子虫的研究中,我们通过质谱鉴定了先前针对位于寄生虫质膜外表面的一种33 kDa蛋白产生的多克隆抗体的靶标。这种由254个氨基酸组成的蛋白质由ECU11_0510开放阅读框编码,呈现出33 kDa和55 kDa两种异构体。序列分析支持将其归类于多糖脱乙酰酶家族,具有疑似几丁质脱乙酰酶活性(EcCDA)。如透射电镜研究所示,EcCDA存在于兔脑炎微孢子虫生命周期早期的质膜上。在孢子母细胞阶段,该酶尤其积聚在壁旁体中,壁旁体是质膜向壁开放的卷曲结构。在昆虫寄生虫蝗虫蚁孢子虫(原蝗虫微孢子虫)中鉴定出EcCDA同源物,表明这种酶在微孢子虫中广泛分布。这种新的微孢子虫表面蛋白的表征为理解孢子壁形成和孢子抗性创造了新的视角。

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