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还原剂和氧化剂对Qβ噬菌体感染性及其衣壳整体结构的影响。

Impact of reducing and oxidizing agents on the infectivity of Qβ phage and the overall structure of its capsid.

作者信息

Loison Pauline, Majou Didier, Gelhaye Eric, Boudaud Nicolas, Gantzer Christophe

机构信息

LCPME (Laboratory of Physical Chemistry and Microbiology for the Environment), Joint Research Unit - UMR 7564, CNRS/Université de Lorraine, Nancy 54000, France CNRS, LCPME, UMR 7564, Institut Jean Barriol (IJB), Nancy 54000, France Food Safety Department, ACTALIA, Saint Lô 50000, France.

ACTIA, 16 rue Claude Bernard, 75231 Paris Cedex 05, France.

出版信息

FEMS Microbiol Ecol. 2016 Nov;92(11). doi: 10.1093/femsec/fiw153. Epub 2016 Jul 10.

Abstract

Qβ phages infect Escherichia coli in the human gut by recognizing F-pili as receptors. Infection therefore occurs under reducing conditions induced by physiological agents (e.g. glutathione) or the intestinal bacterial flora. After excretion in the environment, phage particles are exposed to oxidizing conditions and sometimes disinfection. If inactivation does not occur, the phage may infect new hosts in the human gut through the oral route. During such a life cycle, we demonstrated that, outside the human gut, cysteines of the major protein capsid of Qβ phage form disulfide bonds. Disinfection with NaClO does not allow overoxidation to occur. Such oxidation induces inactivation rather by irreversible damage to the minor proteins. In the presence of glutathione, most disulfide bonds are reduced, which slightly increases the capacity of the phage to infect E. coli in vitro Such reduction is reversible and barely alters infectivity of the phage. Reduction of all disulfide bonds by dithiothreitol leads to complete capsid destabilization. These data provide new insights into how the phages are impacted by oxidizing-reducing conditions outside their host cell and raises the possibility of the intervention of the redox during life cycle of the phage.

摘要

Qβ噬菌体通过将F菌毛识别为受体来感染人类肠道中的大肠杆菌。因此,感染发生在由生理因子(如谷胱甘肽)或肠道细菌菌群诱导的还原条件下。在环境中排泄后,噬菌体颗粒会暴露于氧化条件下,有时还会受到消毒处理。如果没有发生灭活,噬菌体可能会通过口腔途径感染人类肠道中的新宿主。在这样的生命周期中,我们证明,在人类肠道外,Qβ噬菌体主要衣壳蛋白的半胱氨酸会形成二硫键。用次氯酸钠消毒不会导致过度氧化。这种氧化反而通过对次要蛋白质的不可逆损伤诱导灭活。在谷胱甘肽存在的情况下,大多数二硫键会被还原,这会略微增加噬菌体在体外感染大肠杆菌的能力。这种还原是可逆的,并且几乎不会改变噬菌体的感染性。用二硫苏糖醇还原所有二硫键会导致衣壳完全不稳定。这些数据为噬菌体如何受到宿主细胞外氧化还原条件的影响提供了新的见解,并提出了在噬菌体生命周期中氧化还原干预的可能性。

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