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基于一种针对由……引起的感染的新型候选疫苗的计算机辅助疫苗设计。

In-Silico Vaccine Design Based on a Novel Vaccine Candidate Against Infections Caused by .

作者信息

Khalid Kashaf, Irum Sidra, Ullah Sidra Rahmat, Andleeb Saadia

机构信息

Department of Industrial Biotechnology, Atta-ur-Rahman School of Applied Biosciences (ASAB), National University of Sciences and Technology (NUST), Islamabad, 44000 Pakistan.

出版信息

Int J Pept Res Ther. 2022;28(1):16. doi: 10.1007/s10989-021-10316-7. Epub 2021 Dec 2.

Abstract

UNLABELLED

is notorious for causing serious infections of the skin, lungs, soft tissues, bloodstream, and urinary tract. Despite the overwhelming information available so far, there has still been no approved vaccine in the market to prevent these infections. Therefore, this study focuses on developing a rational vaccine design using the technique of epitope mapping to curb the infections caused by . . An outer membrane protein with immunogenic potential as well as all the properties of a good vaccine candidate was selected and used to calculate epitopes for selection on the basis of a low percentile rank, high binding scores, good immunological properties, and non-allergenicity. Thus, a 240 amino-acid vaccine sequence was obtained by manually joining all the epitopes in sequence-wise manner with the appropriate linkers, namely AAY, GPGPG, and EAAAK. Additionally, a 50S ribosomal protein L7/L12, agonist to the human innate immune receptors was attached to the N-terminus to increase the overall immune response towards the vaccine. As a result, enhanced overall protein stability, expression, immunostimulatory capabilities, and solubility of the designed construct were observed. Molecular dynamic simulations revealed the compactness and stability of the polypeptide construct. Moreover, molecular docking exhibited strong binding of the designed vaccine with TLR-4 and TLR-9. In-silico immune simulations indicated an immense increment in T-cell and B-cell populations. Bioinformatic tools also significantly assisted with optimizing codons which allowed for successful cloning of constructs into desired host vectors. Using in-silico tools to design a vaccine against . demonstrated that this construct could pave the way for successfully combating infections caused by multidrug-resistant bacteria.

SUPPLEMENTARY INFORMATION

The online version contains supplementary material available at 10.1007/s10989-021-10316-7.

摘要

未标记

因引发皮肤、肺部、软组织、血液和泌尿系统的严重感染而声名狼藉。尽管目前已有大量信息,但市场上仍没有获批的疫苗来预防这些感染。因此,本研究聚焦于利用表位作图技术开发一种合理的疫苗设计,以抑制由……引起的感染。选择了一种具有免疫原性潜力且具备良好疫苗候选物所有特性的外膜蛋白,并基于低百分位数排名、高结合分数、良好的免疫特性和无致敏性来计算表位以进行选择。通过使用合适的连接子(即AAY、GPGPG和EAAAK)以序列方式手动连接所有表位,从而获得了一个240个氨基酸的疫苗序列。此外,将一种对人类先天免疫受体具有激动作用的50S核糖体蛋白L7/L12连接到N端,以增强对该疫苗的整体免疫反应。结果,观察到所设计构建体的整体蛋白质稳定性、表达、免疫刺激能力和溶解性均有所增强。分子动力学模拟揭示了多肽构建体的紧凑性和稳定性。此外,分子对接显示所设计的疫苗与TLR-4和TLR-9具有强结合。计算机模拟免疫表明T细胞和B细胞群体大幅增加。生物信息学工具也显著有助于优化密码子,从而成功地将构建体克隆到所需的宿主载体中。使用计算机工具设计针对……的疫苗表明,该构建体可为成功对抗多重耐药细菌引起的感染铺平道路。

补充信息

在线版本包含可在10.1007/s10989-021-10316-7获取的补充材料。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7e66/8636788/da913947eefe/10989_2021_10316_Fig1_HTML.jpg

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