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通过反向疫苗学方法鉴定的布鲁氏菌 16M 外膜蛋白疫苗候选物的免疫原性和侵袭性。

Immunogenic and invasive properties of Brucella melitensis 16M outer membrane protein vaccine candidates identified via a reverse vaccinology approach.

机构信息

Department of Veterinary Pathobiology, Texas A&M University, College Station, Texas, United States of America.

出版信息

PLoS One. 2013;8(3):e59751. doi: 10.1371/journal.pone.0059751. Epub 2013 Mar 22.

Abstract

Brucella is the etiologic agent of brucellosis, one of the most common and widely distributed zoonotic diseases. Its highly infectious nature, the insidious, systemic, chronic, debilitating aspects of the disease and the lack of an approved vaccine for human use in the United States are features that make Brucella a viable threat to public health. One of the main impediments to vaccine development is identification of suitable antigens. In order to identify antigens that could potentially be used in a vaccine formulation, we describe a multi-step antigen selection approach. We initially used an algorithm (Vaxign) to predict ORF encoding outer membrane proteins with antigenic determinants. Differential gene expression during acute infection and published evidence for a role in virulence were used as criteria for down-selection of the candidate antigens that resulted from in silico prediction. This approach resulted in the identification of nine Brucella melitensis outer membrane proteins, 5 of which were recombinantly expressed and used for validation. Omp22 and Hia had the highest in silico scores for adhesin probability and also conferred invasive capacity to E. coli overexpressing recombinant proteins. With the exception of FlgK in the goat, all proteins reacted to pooled sera from exposed goats, mice, and humans. BtuB, Hia and FlgK stimulated a mixed Th1-Th2 response in splenocytes from immunized mice while BtuB and Hia elicited NO release from splenocytes of S19 immunized mice. The results support the applicability of the current approach to the identification of antigens with immunogenic and invasive properties. Studies to assess immunogenicity and protective efficacy of individual proteins in the mouse are currently underway.

摘要

布鲁氏菌是布鲁氏菌病的病原体,这是一种最常见和广泛分布的人畜共患病。其高度传染性、疾病的隐匿性、系统性、慢性和衰弱性以及在美国缺乏批准用于人类的疫苗等特点,使其成为对公共卫生的一个可行威胁。疫苗开发的主要障碍之一是确定合适的抗原。为了确定潜在可用于疫苗配方的抗原,我们描述了一种多步骤的抗原选择方法。我们最初使用一种算法(Vaxign)预测具有抗原决定簇的外膜蛋白的 ORF 编码。急性感染期间的差异基因表达和发表的关于在毒力中作用的证据被用作从计算机预测中选择候选抗原的标准。这种方法导致鉴定了 9 种绵羊布鲁氏菌外膜蛋白,其中 5 种被重组表达并用于验证。Omp22 和 Hia 在黏附素概率方面的计算机得分最高,并且还赋予了过表达重组蛋白的大肠杆菌侵袭能力。除了山羊中的 FlgK 外,所有蛋白质都与来自暴露的山羊、小鼠和人类的混合血清发生反应。BtuB、Hia 和 FlgK 刺激免疫小鼠的脾细胞产生混合 Th1-Th2 反应,而 BtuB 和 Hia 诱导 S19 免疫小鼠的脾细胞释放 NO。结果支持当前方法在鉴定具有免疫原性和侵袭性的抗原方面的适用性。目前正在进行评估单个蛋白质在小鼠中的免疫原性和保护效力的研究。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2919/3606113/5684eb90d483/pone.0059751.g001.jpg

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