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重组卡介苗以增强其免疫调节活性。

Recombinant BCG to Enhance Its Immunomodulatory Activities.

作者信息

Kowalewicz-Kulbat Magdalena, Locht Camille

机构信息

Department of Immunology and Infectious Biology, Institute of Microbiology, Biotechnology and Immunology, Faculty of Biology and Environmental Protection, University of Lodz, 90-237 Lodz, Poland.

CHU Lille, Institut Pasteur de Lille, U1019-UMR9017-CIIL-Center for Infection and Immunity of Lille, University Lille, CNRS, Inserm, F-59000 Lille, France.

出版信息

Vaccines (Basel). 2022 May 23;10(5):827. doi: 10.3390/vaccines10050827.

Abstract

The bacillus Calmette-Guérin (BCG) is an attenuated derivative that has been widely used as a live vaccine against tuberculosis for a century. In addition to its use as a tuberculosis vaccine, BCG has also been found to have utility in the prevention or treatment of unrelated diseases, including cancer. However, the protective and therapeutic efficacy of BCG against tuberculosis and other diseases is not perfect. For three decades, it has been possible to genetically modify BCG in an attempt to improve its efficacy. Various immune-modulatory molecules have been produced in recombinant BCG strains and tested for protection against tuberculosis or treatment of several cancers or inflammatory diseases. These molecules include cytokines, bacterial toxins or toxin fragments, as well as other protein and non-protein immune-modulatory molecules. The deletion of genes responsible for the immune-suppressive properties of BCG has also been explored for their effect on BCG-induced innate and adaptive immune responses. Most studies limited their investigations to the description of T cell immune responses that were modified by the genetic modifications of BCG. Some studies also reported improved protection by recombinant BCG against tuberculosis or enhanced therapeutic efficacy against various cancer forms or allergies. However, so far, these investigations have been limited to mouse models, and the prophylactic or therapeutic potential of recombinant BCG strains has not yet been illustrated in other species, including humans, with the exception of a genetically modified BCG strain that is now in late-stage clinical development as a vaccine against tuberculosis. In this review, we provide an overview of the different molecular engineering strategies adopted over the last three decades in order to enhance the immune-modulatory potential of BCG.

摘要

卡介苗(BCG)是一种减毒衍生物,一个世纪以来一直被广泛用作抗结核病的活疫苗。除了用作结核病疫苗外,还发现卡介苗在预防或治疗包括癌症在内的其他不相关疾病方面也有作用。然而,卡介苗对结核病和其他疾病的保护及治疗效果并不理想。三十年来,人们一直可以对卡介苗进行基因改造以提高其疗效。各种免疫调节分子已在重组卡介苗菌株中产生,并测试其对结核病的保护作用或对几种癌症或炎症性疾病的治疗效果。这些分子包括细胞因子、细菌毒素或毒素片段,以及其他蛋白质和非蛋白质免疫调节分子。人们还探索了删除负责卡介苗免疫抑制特性的基因对卡介苗诱导的先天和适应性免疫反应的影响。大多数研究将其调查局限于描述经卡介苗基因改造而改变的T细胞免疫反应。一些研究还报告了重组卡介苗对结核病的保护作用有所改善,或对各种癌症形式或过敏症的治疗效果增强。然而,到目前为止,这些研究仅限于小鼠模型,除了一种作为抗结核病疫苗目前正处于临床开发后期的基因改造卡介苗菌株外,重组卡介苗菌株在包括人类在内的其他物种中的预防或治疗潜力尚未得到证实。在这篇综述中,我们概述了过去三十年来为增强卡介苗的免疫调节潜力而采用的不同分子工程策略。

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