荧光婴儿利什曼原虫对人中性粒细胞的感染和活化。

R E Davis, C J Thalhofer, M E Wilson
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引用次数: 5

摘要

嗜中性粒细胞(pmn)被利什曼属原生动物寄生虫大量招募到宿主感染部位。虽然pmn能够吞噬利什曼原虫寄生虫,并且是抗微生物化合物(包括活性氧)的有效生产者,但它们无法控制感染的建立。先前的研究记录了在允许吞噬的条件下,与利什曼原虫孵养的分离PMN中ROS的产生,但由于没有测量单个细胞的反应,因此无法辨别在内化寄生虫的细胞中PMN的激活和ROS的产生是否受到抑制或无效。为了解决这些相互作用,我们设计了一种荧光的,表达mccherry的利什曼原虫(mCherry-Li)。通过用mccherry - li体外感染分离的人pmn,我们观察到寄生虫与pmn有时间和剂量依赖性的直接关联。我们还检测了PMN ROS的产生(使用荧光化合物DHR123)和PMN的激活(作为表面CD62L表达缺失的证据)。尽管许多锂离子相关(mCherry+) pmn对寄生虫的相互作用和摄取有ROS产生和/或激活的反应,但有一部分pmn没有表现出任何反应。此外,很大一部分mCherry -“旁观者”pmn同时表现出ROS的产生和激活。pmn对利什曼原虫暴露的异质反应使我们假设,首先,一些pmn在吞噬利什曼原虫时表现出活性降低,并可能支持其维持。其次,旁观者pmn的反应可能导致局部炎症环境对寄生虫清除无效。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Infection and Activation of Human Neutrophils with Fluorescent <i>Leishmania infantum</i>.

Infection and Activation of Human Neutrophils with Fluorescent <i>Leishmania infantum</i>.

Infection and Activation of Human Neutrophils with Fluorescent Leishmania infantum.

Neutrophils (PMNs) are recruited in high numbers to sites of host infection by the protozoan parasites of the genus Leishmania. Although PMNs are capable of phagocytizing Leishmania parasites and are potent producers of anti-microbial compounds including reactive oxygen species (ROS), they are unable to control the establishment of infection. Prior studies document production of ROS in isolated PMNs incubated with Leishmania under conditions allowing phagocytosis, but without a measure of single cells' responses it cannot be discerned whether PMN activation and ROS production is suppressed or ineffective in the cells that internalize the parasite. To address these interactions, we engineered a strain of fluorescent, mCherry-expressing Leishmania infantum (mCherry-Li). By infecting isolated human PMNs in vitro with mCherry-Li, we observed ready association of the parasites with PMNs in a time- and dose-dependent fashion. We also examined production of PMN ROS (using the fluorescent compound DHR123) and PMN activation (as evidence by loss of surface CD62L expression). Whereas many Li-associated (mCherry+) PMNs responded to parasite interactions and uptake with ROS production and/or activation, a proportion exhibited neither response. Furthermore, a large proportion of mCherry - "bystander" PMNs displayed both ROS production and activation. The heterogeneous response of PMNs to Leishmania exposure leads us to hypothesize, first, that some PMNs exhibit decreased activation upon phagocytosis of Leishmania, and could support their maintenance. Second, responses of bystander PMNs may contribute to a local inflammatory environment that is ineffective at parasite clearance.

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