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2
Shigella type III secretion effectors: how, where, when, for what purposes?志贺氏菌III型分泌效应蛋白:如何、何处、何时以及为何目的?
Curr Opin Microbiol. 2009 Feb;12(1):110-6. doi: 10.1016/j.mib.2008.12.002. Epub 2009 Jan 20.
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Vaccine. 2008 Jun 19;26(26):3291-6. doi: 10.1016/j.vaccine.2008.03.079. Epub 2008 Apr 16.
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Vaccine. 2008 Feb 13;26(7):978-87. doi: 10.1016/j.vaccine.2007.11.024. Epub 2007 Dec 3.
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Hum Vaccin. 2007 Nov-Dec;3(6):268-75. doi: 10.4161/hv.4746. Epub 2007 Jul 15.
6
Clinical trials of Shigella vaccines: two steps forward and one step back on a long, hard road.志贺氏菌疫苗的临床试验:在漫长而艰难的道路上前进两步,后退一步。
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Shigella's ways of manipulating the host intestinal innate and adaptive immune system: a tool box for survival?志贺氏菌操纵宿主肠道先天性和适应性免疫系统的方式:生存的工具箱?
Immunol Cell Biol. 2007 Feb-Mar;85(2):119-29. doi: 10.1038/sj.icb7100025. Epub 2007 Jan 9.
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Live-attenuated Shigella vaccines.减毒活志贺氏菌疫苗
Expert Rev Vaccines. 2006 Oct;5(5):669-86. doi: 10.1586/14760584.5.5.669.
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Recombinant Shiga toxin B-subunit-keyhole limpet hemocyanin conjugate vaccine protects mice from Shigatoxemia.重组志贺毒素B亚基-钥孔血蓝蛋白结合疫苗可保护小鼠免受志贺毒素血症的侵害。
Infect Immun. 2005 Oct;73(10):6523-9. doi: 10.1128/IAI.73.10.6523-6529.2005.
10
Immunogenicity of multivalent Shigella-ETEC candidate vaccine strains in a guinea pig model.多价志贺氏菌-产肠毒素大肠杆菌候选疫苗株在豚鼠模型中的免疫原性
Vaccine. 2006 May 1;24(18):3727-34. doi: 10.1016/j.vaccine.2005.07.013. Epub 2005 Jul 22.

表达志贺毒素 B 亚单位的减毒活痢疾志贺菌 1 型疫苗株。

Live attenuated Shigella dysenteriae type 1 vaccine strains overexpressing shiga toxin B subunit.

机构信息

University of Maryland School of Medicine, Baltimore, MD, USA.

出版信息

Infect Immun. 2011 Dec;79(12):4912-22. doi: 10.1128/IAI.05814-11. Epub 2011 Oct 3.

DOI:10.1128/IAI.05814-11
PMID:21969003
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3232646/
Abstract

Shigella dysenteriae serotype 1 (S. dysenteriae 1) is unique among the Shigella species and serotypes in the expression of Shiga toxin which contributes to more severe disease sequelae and the ability to cause explosive outbreaks and pandemics. S. dysenteriae 1 shares characteristics with other Shigella species, including the capability of causing clinical illness with a very low inoculum (10 to 100 CFU) and resistance to multiple antibiotics, underscoring the need for efficacious vaccines and therapeutics. Following the demonstration of the successful attenuating capacity of deletion mutations in the guaBA operon in S. flexneri 2a vaccine strains in clinical studies, we developed a series of S. dysenteriae 1 vaccine candidates containing the fundamental attenuating mutation in guaBA. All strains are devoid of Shiga toxin activity by specific deletion of the gene encoding the StxA subunit, which encodes enzymatic activity. The StxB subunit was overexpressed in several derivatives by either plasmid-based constructs or chromosomal manipulation to include a strong promoter. All strains are attenuated for growth in vitro in the HeLa cell assay and for plaque formation and were safe in the Serény test and immunogenic in the guinea pigs. Each strain induced robust serum and mucosal anti-S. dysenteriae 1 lipopolysaccharide (LPS) responses and protected against wild-type challenge. Two strains engineered to overexpress StxB induced high titers of Shiga toxin neutralizing antibodies. These candidates demonstrate the potential for a live attenuated vaccine to protect against disease caused by S. dysenteriae 1 and potentially to protect against the toxic effects of other Shiga toxin 1-expressing pathogens.

摘要

志贺氏痢疾杆菌血清型 1(S. dysenteriae 1)在表达志贺毒素方面与其他志贺氏菌血清型不同,这导致了更严重的疾病后遗症,并且具有引起爆发和大流行的能力。S. dysenteriae 1 与其他志贺氏菌具有共同特征,包括能够用非常低的接种量(10 到 100 CFU)引起临床疾病以及对多种抗生素的耐药性,这突出表明需要有效的疫苗和治疗方法。在证明了 S. flexneri 2a 疫苗株中 guaBA 操纵子缺失突变的成功减毒能力后,我们开发了一系列含有 guaBA 基本减毒突变的 S. dysenteriae 1 疫苗候选物。所有菌株通过特异性缺失编码 StxA 亚单位的基因而丧失了志贺毒素活性,StxA 亚单位编码酶活性。通过质粒构建或染色体操作在几个衍生菌株中过表达 StxB 亚单位,以包含强启动子。所有菌株在 HeLa 细胞测定中体外生长、形成噬菌斑以及 Serény 试验中的安全性和豚鼠中的免疫原性均减弱。每种菌株均诱导了针对 S. dysenteriae 1 脂多糖(LPS)的强烈血清和粘膜抗血清反应,并能抵抗野生型挑战。两种过表达 StxB 的工程菌株诱导了高滴度的志贺毒素中和抗体。这些候选物证明了活减毒疫苗有潜力预防由 S. dysenteriae 1 引起的疾病,并可能预防其他表达 Shiga 毒素 1 的病原体的毒性作用。