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百日咳毒素中S2和S3亚基的基因交换。

Genetic exchange of the S2 and S3 subunits in pertussis toxin.

作者信息

Raze Dominique, Veithen Alex, Sato Hiroko, Antoine Rudy, Menozzi Franco D, Locht Camille

机构信息

INSERM U629, Institut Pasteur de Lille, 1 rue du Professeur Calmette, 59019 Lille Cedex, France.

出版信息

Mol Microbiol. 2006 Jun;60(5):1241-50. doi: 10.1111/j.1365-2958.2006.05165.x.

Abstract

Bordetella pertussis, the causative agent of whooping cough, produces a complex hetero-oligomeric exotoxin, named pertussis toxin (PTX), which is responsible for several of the clinical manifestations associated with whooping cough. The toxin is composed of five dissimilar subunits, named S1 through S5 and arranged in a hexameric structure with a 1S1:1S2:1S3:2S4:1S5 stoichiometry. Although S2 and S3 share 70% amino acid identity, these two subunits were previously thought not to be able to substitute for each other in toxin assembly/secretion and the biological activities of PTX. Here, we show that toxin analogues containing two S3 subunits and lacking S2 (PTXdeltaS2), or containing two S2 subunits and lacking S3 (PTXdeltaS3), can be produced, assembled and secreted by B. pertussis strains, in which the S2-encoding cistron or the S3-coding cistrons have been inactivated by internal in-frame deletions that avoid downstream effects. In fact, PTXdeltaS3 was produced in higher amounts in the bacterial culture supernatants than natural PTX, whereas PTXdeltaS2 was produced in lower amounts than PTX. The action of the toxin analogues on the clustering of Chinese Hamster Ovary cells was also affected differentially by the S2-S3 substitution. These toxin analogues constitute thus interesting probes for the study of cellular functions, in particular immune cell functions, for which natural PTX has already shown its usefulness.

摘要

百日咳博德特氏菌是百日咳的病原体,可产生一种复杂的杂合寡聚外毒素,称为百日咳毒素(PTX),它与百日咳相关的几种临床表现有关。该毒素由五个不同的亚基组成,命名为S1至S5,以1S1:1S2:1S3:2S4:1S5的化学计量比排列成六聚体结构。尽管S2和S3有70%的氨基酸同一性,但以前认为这两个亚基在毒素组装/分泌和PTX的生物学活性方面不能相互替代。在此,我们表明,含有两个S3亚基且缺少S2的毒素类似物(PTXdeltaS2),或含有两个S2亚基且缺少S3的毒素类似物(PTXdeltaS3),可由百日咳博德特氏菌菌株产生、组装和分泌,其中编码S2的顺反子或编码S3的顺反子已通过内部读框缺失失活,以避免下游效应。事实上,PTXdeltaS3在细菌培养上清液中的产量高于天然PTX,而PTXdeltaS2的产量低于PTX。毒素类似物对中国仓鼠卵巢细胞聚集的作用也因S2-S3替代而受到不同影响。因此,这些毒素类似物构成了研究细胞功能,特别是免疫细胞功能的有趣探针,天然PTX已证明其在这方面的有用性。

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