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首页> 外文期刊>Ecological restoration >Generating mucosal and systemic immune response following vaccination of vibrio cholerae adhesion molecule against shigella flexneri infection
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Generating mucosal and systemic immune response following vaccination of vibrio cholerae adhesion molecule against shigella flexneri infection

机译:在对志贺氏菌感染的影响后产生粘膜和全身免疫应答

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摘要

Introduction: Previous studies have shown 37.8 kDa pili subunit protein of Vibrio cholerae and 49.8 kDa pili subunit protein of Shigella flexneri can act as an adhesion molecule to initiate infection. These molecules also have the ability to agglutinate blood. The present study assessed mucosal and systemic immunity following vaccination using 37.8 kDa V. cholerae and protection against S. flexneri. Subjects and Methods: Haemagglutination test was performed after purification of V. cholerae protein, followed by an anti-haemagglutination test. The intestinal weight and colony count were used to validate the protective effect on balb/c mice which were divided into the naive group, Shigella-positive control group, Vibrio-positive control group, V. cholerae infected-Vibrio-vaccinated group and S. flexneri-infected-Vibrio-vaccinated group. Th17, Treg, interleukin (IL) IL-17A, beta-defensin and secretory-immunoglobulin A (s-IgA) were also measured to determine the systemic and mucosal immunity after vaccination. Results: The haemagglutination and anti-haemagglutination tests showed that the 37.8 kDa protein could inhibit 49.8 kDa of the S. flexneri pili subunit. Decreased intestinal weight and colony count of vaccinated group compared to naive group also support cross reaction findings. Vaccination also generates higher level of Th17, Treg, IL-17A, beta-defensin and s-IgA significantly. Conclusions: 37.8 kDa subunit pili can act as a homologous vaccine candidate to prevent V. cholerae and S. flexneri infection.
机译:介绍:以前的研究显示了37.8kda pili亚基蛋白的慢性霍乱和49.8kda pili亚单位蛋白的shigella flexeri可以用作引发感染的粘附分子。这些分子还具有凝集血液的能力。本研究评估了使用37.8kDa V.霍乱和对抗S. Flexners的疫苗接种后的粘膜和全身免疫。受试者和方法:在富含V.霍乱蛋白的纯化后进行血凝试验,然后进行抗血凝试验。肠道重量和菌落计数用于验证对BALB / C小鼠的保护作用,分为幼稚基团,志贺氏菌阳性对照组,振动阳性对照组V.Cholerae感染弧菌疫苗基团和S. Flexeri感染弧菌接种疫苗。还测量Th17,Treg,白细胞介素(IL)IL-17A,β-防御素和分泌免疫球蛋白A(S-IgA)以确定疫苗接种后的全身和粘膜免疫。结果:血凝和抗血凝试验显示,37.8kDa蛋白可以抑制49.8kda的S.Flexeri pili亚基。与幼稚基团相比,接种疫苗的肠道重量和菌落计数降低也支持交叉反应结果。接种疫苗也显着产生更高水平的TH17,Treg,IL-17a,β-防御素和S-IgA。结论:37.8 kda亚基pili可以作为一种同源疫苗候选者,以防止霍乱和柔屈的感染。

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