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抗击结核病:寻找卡介苗的替代品

Fighting Tuberculosis: In Search of a BCG Replacement.

作者信息

Nadolinskaia Nonna I, Kotliarova Maria S, Goncharenko Anna V

机构信息

Bach Institute of Biochemistry, Fundamentals of Biotechnology Federal Research Center, Russian Academy of Sciences, 119071 Moscow, Russia.

出版信息

Microorganisms. 2022 Dec 23;11(1):51. doi: 10.3390/microorganisms11010051.

Abstract

Tuberculosis is one of the most threatening infectious diseases and represents an important and significant reason for mortality in high-burden regions. The only licensed vaccine, BCG, is hardly capable of establishing long-term tuberculosis protection and is highly variable in its effectiveness. Even after 100 years of BCG use and research, we still cannot unequivocally answer the question of which immune correlates of protection are crucial to prevent (Mtb) infection or the progression of the disease. The development of a new vaccine against tuberculosis arises a nontrivial scientific challenge caused by several specific features of the intracellular lifestyle of Mtb and the ability of the pathogen to manipulate host immunity. The purpose of this review is to discuss promising strategies and the possibilities of creating a new vaccine that could replace BCG and provide greater protection. The considered approaches include supplementing mycobacterial strains with immunodominant antigens and genetic engineering aimed at altering the interaction between the bacterium and the host cell, such as the exit from the phagosome. Improved new vaccine strains based on BCG and Mtb undergoing clinical evaluation are also overviewed.

摘要

结核病是最具威胁性的传染病之一,也是高负担地区重要的死亡原因。唯一获得许可的疫苗卡介苗几乎无法提供长期的结核病防护,其有效性也存在很大差异。即使在卡介苗使用和研究了100年后,我们仍然无法明确回答哪种保护性免疫相关因素对于预防结核分枝杆菌(Mtb)感染或疾病进展至关重要。由于Mtb细胞内生活方式的几个特定特征以及病原体操纵宿主免疫的能力,开发一种新的抗结核疫苗面临着重大的科学挑战。本综述的目的是讨论有前景的策略以及研发一种能够替代卡介苗并提供更强保护的新疫苗的可能性。所考虑的方法包括用免疫显性抗原补充分枝杆菌菌株以及进行基因工程改造以改变细菌与宿主细胞之间的相互作用,如从吞噬体中逸出。还概述了基于卡介苗和正在进行临床评估的结核分枝杆菌的改良新疫苗菌株。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9be2/9863999/a9021192d9a0/microorganisms-11-00051-g001.jpg

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