激活巨噬细胞杀死立克次体和利什曼原虫:细胞内杀微生物活性的分离和肿瘤和蠕虫目标的细胞外破坏。

C A Nacy, C N Oster, S L James, M S Meltzer
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引用次数: 37

摘要

单核吞噬细胞在骨髓干细胞向常驻组织巨噬细胞分化的过程中发生了巨大的变化。在整个分化过程中,细胞失去或获得了许多形态、代谢和功能能力,因此一个组织中成熟的、常驻的巨噬细胞往往与另一个组织中的常驻细胞几乎没有相似之处。在单核吞噬细胞分化的内在连续体上叠加的是内源性和外源性刺激诱导的巨噬细胞反应性变化:单核吞噬细胞对特定刺激的反应能力也可能随着细胞分化而改变。这种细胞分化和对微环境反应的动态相互作用,以及由此导致的单核吞噬细胞在许多功能特征上的异质性,在我们在本报告中描述的活化巨噬细胞的效应活性中清楚地说明了这一点。尽管对立克次体、利什曼原虫、血吸虫和肿瘤细胞等多种靶标有效的瞬时非特异性细胞毒性反应的诱导和表达有共同的调节事件,但这些效应功能可以被执行效应活性的细胞和调节这些活性的信号分离。在反应性群体中,不同靶点对LK诱导的特定杀伤机制的不同敏感性只会增加这些体外分析的复杂性。活化巨噬细胞的效应功能细节对每个靶标都是独特的。
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Activation of macrophages to kill rickettsiae and Leishmania: dissociation of intracellular microbicidal activities and extracellular destruction of neoplastic and helminth targets.

Mononuclear phagocytes undergo dramatic changes during differentiation from bone marrow stem cells to resident tissue macrophages. Throughout differentiation, cells lose or acquire numerous morphologic, metabolic and functional capacities such that mature, resident macrophages of one tissue often bear little resemblance to resident cells of another. Superimposed on the intrinsic continuum of mononuclear phagocyte differentiation are the reactive changes in macrophages induced by endogenous and exogenous stimuli: the ability of mononuclear phagocytes to respond to a particular stimulus may also change with cell differentiation. This dynamic interaction of cell differentiation and response to a micro-environment, and the resulting heterogeneity among mononuclear phagocytes for many functional characteristics, is clearly illustrated by the effector activities of activated macrophages that we describe in this report. Despite the common regulatory events for induction and expression of transient nonspecific cytotoxic reactions effective against such diverse targets as rickettsiae, leishmania, schistosomula, and neoplastic cells, these effector functions can be dissociated by the cells that perform the effector activity, and the signals that regulate these activities. The differential susceptibility of the various targets to particular killing mechanisms induced by LK in responsive populations only adds to the complexity of these in vitro analyses. The details of effector functions of activated macrophages are unique for each target.

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