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口蹄疫病毒结构蛋白中的细胞培养适应性氨基酸取代:受体嗜性改变的关键机制

Cell Culture Adaptive Amino Acid Substitutions in FMDV Structural Proteins: A Key Mechanism for Altered Receptor Tropism.

作者信息

Mushtaq Hassan, Shah Syed Salman, Zarlashat Yusra, Iqbal Mazhar, Abbas Wasim

机构信息

Health Biotechnology Division, National Institute for Biotechnology and Genetic Engineering-C (NIBGE), Faisalabad 38000, Pakistan.

Pakistan Institute of Engineering and Applied Sciences (PIEAS), Islamabad 45650, Pakistan.

出版信息

Viruses. 2024 Mar 27;16(4):512. doi: 10.3390/v16040512.

Abstract

The foot-and-mouth disease virus is a highly contagious and economically devastating virus of cloven-hooved animals, including cattle, buffalo, sheep, and goats, causing reduced animal productivity and posing international trade restrictions. For decades, chemically inactivated vaccines have been serving as the most effective strategy for the management of foot-and-mouth disease. Inactivated vaccines are commercially produced in cell culture systems, which require successful propagation and adaptation of field isolates, demanding a high cost and laborious time. Cell culture adaptation is chiefly indebted to amino acid substitutions in surface-exposed capsid proteins, altering the necessity of RGD-dependent receptors to heparan sulfate macromolecules for virus binding. Several amino acid substations in VP1, VP2, and VP3 capsid proteins of FMDV, both at structural and functional levels, have been characterized previously. This literature review combines frequently reported amino acid substitutions in virus capsid proteins, their critical roles in virus adaptation, and functional characterization of the substitutions. Furthermore, this data can facilitate molecular virologists to develop new vaccine strains against the foot-and-mouth disease virus, revolutionizing vaccinology via reverse genetic engineering and synthetic biology.

摘要

口蹄疫病毒是一种对偶蹄动物具有高度传染性且在经济上具有毁灭性的病毒,这些偶蹄动物包括牛、水牛、绵羊和山羊,它会导致动物生产力下降并造成国际贸易限制。几十年来,化学灭活疫苗一直是控制口蹄疫最有效的策略。灭活疫苗在细胞培养系统中进行商业化生产,这需要成功繁殖和适应田间分离株,成本高昂且耗时费力。细胞培养适应性主要归因于表面暴露的衣壳蛋白中的氨基酸替换,这改变了病毒结合时RGD依赖性受体对硫酸乙酰肝素大分子的需求。先前已经在结构和功能水平上对口蹄疫病毒VP1、VP2和VP3衣壳蛋白中的几个氨基酸替换进行了表征。这篇文献综述结合了病毒衣壳蛋白中频繁报道的氨基酸替换、它们在病毒适应中的关键作用以及这些替换的功能表征。此外,这些数据可以帮助分子病毒学家开发针对口蹄疫病毒的新疫苗株,通过反向基因工程和合成生物学彻底改变疫苗学。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8e0f/11054764/017cd1318db0/viruses-16-00512-g001.jpg

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