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口蹄疫疫苗的研发及诱导持久免疫力面临的挑战:趋势与当前观点

Foot and Mouth Disease Vaccine Development and Challenges in Inducing Long-Lasting Immunity: Trends and Current Perspectives.

作者信息

Kenubih Ambaye

机构信息

University of Gondar, College of Veterinary Medicine and Animal Sciences, Para-Clinical Studies, Gondar, Ethiopia.

出版信息

Vet Med (Auckl). 2021 Sep 1;12:205-215. doi: 10.2147/VMRR.S319761. eCollection 2021.

Abstract

Foot and mouth disease (FMD) is an extremely contagious viral disease of livestock caused by foot and mouse disease virus genus: , which causes a serious economic impact on both individual farmers and the national economy. Many attempts to advance a vaccine for FMD have failed to induce sterile immunity. The classical methods of vaccine production were due to selective accumulation of mutations around antigenic and binding sites. Reversion of the agent by positive selection and quasi-species swarm, use of this method is inapplicable for use in non-endemic areas. Chemical attenuation using binary ethyleneimine (BEI) protected the capsid integrity and produced a pronounced immunity against the challenge strain. Viral antigens which have been chemically synthesized or expressed in viruses, plasmid, or plants were tried in the vaccination of animals. DNA vaccines expressing either structural or nonstructural protein antigens have been tried to immunize animals. Using interleukins as a genetic adjuvant for DNA vaccines have a promising effect. While the challenges of inducing sterile immunity lies on non-structural (NS) proteins of FMDV which are responsible for apoptosis of dendritic cells and have negative effects on lympho-proliferative responses which lead to transient immunosuppression. Furthermore, destruction of host protein trafficking by nonstructural proteins suppressed CD T-cell proliferation. In this review, it tried to address multiple approaches for vaccine development trials and bottle necks of producing sterile immunity.

摘要

口蹄疫(FMD)是由口蹄疫病毒属引起的一种极具传染性的家畜病毒性疾病,对个体养殖户和国民经济都造成了严重的经济影响。许多研发口蹄疫疫苗的尝试都未能诱导出无菌免疫力。传统的疫苗生产方法是由于抗原和结合位点周围的突变选择性积累。通过正向选择和准种群体使病原体发生回复突变,这种方法不适用于非流行地区。使用双乙烯亚胺(BEI)进行化学减毒可保护衣壳完整性,并对攻击毒株产生显著的免疫力。已尝试将化学合成或在病毒、质粒或植物中表达的病毒抗原用于动物疫苗接种。已尝试使用表达结构或非结构蛋白抗原的DNA疫苗对动物进行免疫。将白细胞介素用作DNA疫苗的遗传佐剂具有良好的效果。然而,诱导无菌免疫力面临的挑战在于口蹄疫病毒的非结构(NS)蛋白,这些蛋白会导致树突状细胞凋亡,并对淋巴细胞增殖反应产生负面影响,从而导致短暂的免疫抑制。此外,非结构蛋白对宿主蛋白转运的破坏会抑制CD4+ T细胞增殖。在这篇综述中,试图探讨疫苗研发试验的多种方法以及产生无菌免疫力的瓶颈。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3126/8420785/704a8d725325/VMRR-12-205-g0001.jpg

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