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Phenotypic Diversity and Emerging New Tools to Study Macrophage Activation in Bacterial Infectious Diseases

机译:表型多样性和新兴工具研究细菌感染性疾病中的巨噬细胞活化

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摘要

Macrophage polarization is a concept that has been useful to describe the different features of macrophage activation related to specific functions. Macrophage polarization is responsible for a dichotomic approach (killing vs. repair) of the host response to bacteria; M1-type conditions are protective, whereas M2-type conditions are associated with bacterial persistence. The use of the polarization concept to classify the features of macrophage activation in infected patients using transcriptional and/or molecular data and to provide biomarkers for diagnosis and prognosis has most often been unsuccessful. The confrontation of polarization with different clinical situations in which monocytes/macrophages encounter bacteria obliged us to reappraise this concept. With the exception of M2-type infectious diseases, such as leprosy and Whipple’s disease, most acute (sepsis) or chronic (Q fever, tuberculosis) infectious diseases do not exhibit polarized monocytes/macrophages. This is also the case for commensals that shape the immune response and for probiotics that alter the immune response independent of macrophage polarization. We propose that the type of myeloid cells (monocytes vs. macrophages) and the kinetics of the immune response (early vs. late responses) are critical variables for understanding macrophage activation in human infectious diseases. Explorating the role of these new markers will provide important tools to better understand complex macrophage physiology.
机译:巨噬细胞极化是一个概念,用于描述与特定功能相关的巨噬细胞激活的不同特征。巨噬细胞极化负责宿主对细菌反应的二分法(杀死与修复)。 M1型条件是保护性的,而M2型条件与细菌的持久性有关。使用极化概念来利用转录和/或分子数据对感染患者中巨噬细胞活化的特征进行分类并提供用于诊断和预后的生物标记物的尝试通常是不成功的。在单核细胞/巨噬细胞遇到细菌的不同临床情况下,极化的对抗迫使我们重新评估了这一概念。除了麻风和Whipple病等M2型传染病外,大多数急性(败血症)或慢性(Q发热,结核病)传染病均未表现出极化的单核细胞/巨噬细胞。塑造免疫应答的奖杯和独立于巨噬细胞极化改变免疫应答的益生菌也是如此。我们认为,髓样细胞的类型(单核细胞与巨噬细胞)和免疫应答的动力学(早期应答与晚期应答)是理解人类传染病中巨噬细胞活化的关键变量。探索这些新标记的作用将提供重要的工具,以更好地了解复杂的巨噬细胞生理。

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