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Three-Dimensional In Vitro Models of Granuloma to Study Bacteria-Host Interactions, Drug-Susceptibility, and Resuscitation of Dormant Mycobacteria

机译:肉芽肿的三维体外模型研究细菌-宿主相互作用,药物敏感性和休眠分枝杆菌的复苏

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Mycobacterium tuberculosis, Mycobacterium leprae, Mycobacterium bovis, and Mycobacterium avium subsp. paratuberculosis can survive within host macrophages in a dormant state, encased within an organized aggregate of immune host cells called granuloma. Granulomas consist of uninfected macrophages, foamy macrophages, epithelioid cells, and T lymphocytes accumulated around infected macrophages. Within granulomas, activated macrophages can fuse to form multinucleated giant cells, also called giant Langhans cells. A rim of T lymphocytes surrounds the core, and a tight coat of fibroblast closes the structure. Several in vivo models have been used to study granulomas structure and function, but recently developed in vitro models of granuloma show potential for closer observation of the early stages of host's responses to live mycobacteria. This paper reviews culture conditions that resulted in three-dimensional granulomas, formed by the adhesion of cell populations in peripheral blood mononuclear cells infected with mycobacteria. The similarities of these models to granulomas encountered in clinical specimens include cellular composition, granulomas' cytokine production, and cell surface antigens. A reliable in vitro dormancy model may serve as a useful platform to test whether drug candidates can kill dormant mycobacteria. Novel drugs that target dormancy-specific pathways may shorten the current long, difficult treatments necessary to cure mycobacterial diseases.
机译:结核分枝杆菌,麻风分枝杆菌,牛分枝杆菌和鸟分枝杆菌亚种。副结核病可以在休眠状态的宿主巨噬细胞内存活,并被包裹在称为肉芽肿的免疫宿主细胞的有组织聚集体内。肉芽肿由未感染的巨噬细胞,泡沫巨噬细胞,上皮样细胞和在感染的巨噬细胞周围积累的T淋巴细胞组成。在肉芽肿内,活化的巨噬细胞可以融合形成多核巨细胞,也称为巨朗汉斯细胞。 T淋巴细胞的边缘围绕着核心,紧密的成纤维细胞涂层封闭了结构。几种体内模型已被用于研究肉芽肿的结构和功能,但最近开发的肉芽肿体外模型显示了更密切观察宿主对活分枝杆菌反应早期阶段的潜力。本文综述了导致三维肉芽肿的培养条件,这些肉芽肿是由感染分枝杆菌的外周血单个核细胞中细胞群的粘附形成的。这些模型与临床标本中遇到的肉芽肿的相似之处包括细胞组成,肉芽肿的细胞因子产生和细胞表面抗原。一个可靠的体外休眠模型可以作为测试候选药物是否可以杀死休眠分枝杆菌的有用平台。针对休眠特定途径的新型药物可能会缩短目前治疗分枝杆菌疾病所需的漫长而困难的治疗方法。

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