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鼠α-防御素cryptdin-4 的杀菌活性主要影响非共生菌。

Bactericidal activity of mouse α-defensin cryptdin-4 predominantly affects noncommensal bacteria.

机构信息

Innate Immunity Laboratory, Graduate School of Life Science, Hokkaido University, Sapporo, Japan.

出版信息

J Innate Immun. 2011;3(3):315-26. doi: 10.1159/000322037. Epub 2010 Nov 22.

Abstract

Mouse Paneth cell α-defensins, termed cryptdins, are secreted into the intestinal lumen, have microbicidal activity, and contribute to intestinal innate immunity. Among them, cryptdin-4 (Crp4) has the most potent microbicidal activity. In the intestinal lumen, commensal bacteria colonize and elicit beneficial effects in the host. However, the effects of Crp4 against commensal bacteria are poorly understood. Thus, we investigated the bactericidal activities of Crp4 against commensal bacteria compared to noncommensal bacteria. Oxidized Crp4 showed only minimal or no bactericidal activity against 8 out of 12 commensal bacterial species, including Bifidobacterium bifidum and Lactobacillus casei. We further addressed a role of the conserved disulfide bonds of Crp4 by analyzing reduced Crp4 (r-Crp4). r-Crp4 demonstrated significantly greater bactericidal activities against 7 of 12 commensal bacteria than did oxidized Crp4. Oxidized Crp4 and r-Crp4 elicited equivalently potent bactericidal activities against 11 of the 11 noncommensal bacteria tested, such as Salmonella enterica serovar Typhimurium,and against 5 of 12 commensal bacteria. Furthermore, when r-Crp4 was exposed to a processing enzyme of cryptdins, i.e. MMP-7, r-Crp4 was degraded and the bactericidal activities disappeared. These findings suggest that Crp4 has selective bactericidal activities against intestinal microbiota and that the activities are dependent on the disulfide bonds.

摘要

鼠潘氏细胞α-防御素,称为隐穴素,分泌到肠腔中,具有杀菌活性,并有助于肠道先天免疫。其中,隐穴素-4(Crp4)具有最强的杀菌活性。在肠腔中,共生菌定植并在宿主中产生有益的影响。然而,Crp4 对共生菌的作用知之甚少。因此,我们研究了 Crp4 对共生菌与非共生菌的杀菌活性。氧化 Crp4 对 12 种共生菌中的 8 种,包括双歧杆菌和干酪乳杆菌,仅表现出最小或没有杀菌活性。我们进一步通过分析还原 Crp4(r-Crp4)来研究 Crp4 保守二硫键的作用。r-Crp4 对 7 种共生菌的杀菌活性明显大于氧化 Crp4。氧化 Crp4 和 r-Crp4 对 11 种非共生菌(如肠炎沙门氏菌血清型 Typhimurium)和 12 种共生菌中的 5 种的杀菌活性相同。此外,当 r-Crp4 暴露于隐穴素的加工酶,即 MMP-7 时,r-Crp4 被降解,杀菌活性消失。这些发现表明 Crp4 对肠道微生物群具有选择性杀菌活性,并且该活性依赖于二硫键。

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