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通过反向疫苗学注释潜在疫苗靶点并设计针对[具体疾病或病原体]的多表位亚单位疫苗,以及通过基于主体的建模方法进行验证。 (原文中against后缺少具体对象)

Annotation of Potential Vaccine Targets and Design of a Multi-Epitope Subunit Vaccine against through Reverse Vaccinology and Validation through an Agent-Based Modeling Approach.

作者信息

Haq Azaz Ul, Khan Abbas, Khan Jafar, Irum Shamaila, Waheed Yasir, Ahmad Sajjad, Nizam-Uddin N, Albutti Aqel, Zaman Nasib, Hussain Zahid, Ali Syed Shujait, Waseem Muhammad, Kanwal Fariha, Wei Dong-Qing, Wang Qian

机构信息

Center for Biotechnology and Microbiology, Kanju Campus, University of Swat, Swat 19200, Pakistan.

Department of Bioinformatics and Biological Statistics, School of Life Sciences and Biotechnology, Shanghai Jiao Tong University, Shanghai 200240, China.

出版信息

Vaccines (Basel). 2021 Nov 15;9(11):1327. doi: 10.3390/vaccines9111327.

Abstract

is responsible for plague and major pandemics in Asia and Europe. This bacterium has shown resistance to an array of drugs commonly used for the treatment of plague. Therefore, effective therapeutics measurements, such as designing a vaccine that can effectively and safely prevent infection, are of high interest. To fast-track vaccine development against , herein, proteome-wide vaccine target annotation was performed, and structural vaccinology-assisted epitopes were predicted. Among the total 3909 proteins, only 5 (rstB, YPO2385, hmuR, flaA1a, and psaB) were shortlisted as essential vaccine targets. These targets were then subjected to multi-epitope vaccine design using different linkers. EAAK, AAY, and GPGPG as linkers were used to link CTL, HTL, and B-cell epitopes, and an adjuvant (beta defensin) was also added at the N-terminal of the MEVC. Physiochemical characterization, such as determination of the instability index, theoretical pI, half-life, aliphatic index, stability profiling, antigenicity, allergenicity, and hydropathy of the ensemble, showed that the vaccine is highly stable, antigenic, and non-allergenic and produces multiple interactions with immune receptors upon docking. In addition, molecular dynamics simulation confirmed the stable binding and good dynamic properties of the vaccine-TLR complex. Furthermore, in silico and immune simulation of the developed MEVC for showed that the vaccine triggered strong immune response after several doses at different intervals. Neutralization of the antigen was observed at the third day of injection. Conclusively, the vaccine designed here for produces an immune response; however, further immunological testing is needed to unveil its real efficacy.

摘要

负责亚洲和欧洲的鼠疫及重大疫情。这种细菌已对一系列常用于治疗鼠疫的药物产生耐药性。因此,开展有效的治疗措施,如设计一种能有效且安全预防感染的疫苗,备受关注。为加速针对该病菌的疫苗研发,在此进行了全蛋白质组疫苗靶点注释,并预测了结构疫苗学辅助的表位。在总共3909种蛋白质中,仅有5种(rstB、YPO2385、hmuR、flaA1a和psaB)被列为关键疫苗靶点。然后使用不同的连接子对这些靶点进行多表位疫苗设计。使用EAAK、AAY和GPGPG作为连接子来连接细胞毒性T淋巴细胞(CTL)、辅助性T淋巴细胞(HTL)和B细胞表位,并且还在多表位疫苗构建体(MEVC)的N端添加了一种佐剂(β防御素)。对该疫苗构建体进行理化特性表征,如测定不稳定性指数、理论等电点、半衰期、脂肪族指数、稳定性分析、抗原性、致敏性和亲水性,结果表明该疫苗高度稳定、具有抗原性且无致敏性,对接时与免疫受体产生多种相互作用。此外,分子动力学模拟证实了疫苗 - Toll样受体(TLR)复合物的稳定结合和良好的动力学特性。此外,对所开发的针对该病菌的MEVC进行计算机模拟和免疫模拟表明,该疫苗在不同间隔给予几剂后引发了强烈的免疫反应。在注射第三天观察到抗原被中和。总之,此处设计的针对该病菌的疫苗产生了免疫反应;然而,需要进一步的免疫学测试来揭示其实际疗效。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/17de/8625334/3914162e123d/vaccines-09-01327-g001.jpg

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