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炭疽芽孢杆菌孢子在原代小鼠巨噬细胞中对特定萌发剂的反应受pXO1质粒上编码的一种蛋白质调控。

The response to a specific germinant by Bacillus anthracis spores in primary mouse macrophages is modulated by a protein encoded on the pXO1 plasmid.

作者信息

Aronson Arthur I, Hu Haijing

机构信息

Department of Biological Sciences, Purdue University, W. Lafayette, IN 47907, USA.

出版信息

Arch Microbiol. 2008 Nov;190(5):539-46. doi: 10.1007/s00203-008-0403-5. Epub 2008 Jul 25.

Abstract

A Bacillus anthracis Sterne pXO1 plasmid-encoded protein designated Cot43 was found in coat extracts of purified spores. Cot43 is a tetratricopeptide repeat domain protein related to those which function as phosphatases in the sporulation phosphorelay and as regulators of competence and pathogenic factors. The synthesis of Cot43 began in the late exponential phase downstream from a sigmaA promoter (as mapped by RACE) and it was present at least until the formation of phase white endospores. There was specificity in the association of Cot43 with B. anthracis spores since Bacillus cereus producing Cot43 from a cloned gene had very little of this protein in spore coat extracts. In addition, Cot43 was synthesized by B. anthracis cells to the same extent in glucose-yeast extract and nutrient sporulation media, but was essentially absent from spores formed in the former. L-histidine is an important germinant for B. anthracis spores in macrophages, Spores produced by a mutant with a disruption of cot43 germinated in response to L-histidine both in vitro and within primary mouse macrophages earlier and more extensively than Sterne strain spores. The germination delay due to the presence of Cot43 would enhance spore survival and thus increase the chances for a successful infection.

摘要

在纯化孢子的外壳提取物中发现了一种由炭疽芽孢杆菌斯特恩株pXO1质粒编码的名为Cot43的蛋白质。Cot43是一种四肽重复结构域蛋白,与那些在孢子形成磷信号转导中起磷酸酶作用以及作为感受态和致病因子调节剂的蛋白相关。Cot43的合成始于指数后期阶段,位于sigmaA启动子下游(通过RACE定位),并且至少在白色期内生孢子形成时仍然存在。Cot43与炭疽芽孢杆菌孢子的结合具有特异性,因为从克隆基因产生Cot43的蜡样芽孢杆菌在孢子外壳提取物中几乎没有这种蛋白质。此外,炭疽芽孢杆菌细胞在葡萄糖 - 酵母提取物和营养孢子形成培养基中合成Cot43的程度相同,但在前一种培养基中形成的孢子中基本上不存在。L - 组氨酸是炭疽芽孢杆菌孢子在巨噬细胞中的重要萌发剂,由cot43基因破坏的突变体产生的孢子在体外和原代小鼠巨噬细胞内对L - 组氨酸的萌发反应比斯特恩株孢子更早且更广泛。由于Cot43的存在导致的萌发延迟会提高孢子的存活率,从而增加成功感染的机会。

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