Sequential recruitment of Rab GTPases during early stages of phagocytosis.

Cellular logistics Pub Date : 2016-01-29 eCollection Date: 2016-01-01 DOI:10.1080/21592799.2016.1140615
Jeremy C Yeo, Adam A Wall, Lin Luo, Jennifer L Stow
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引用次数: 22

Abstract

The phagocytosis and destruction of pathogens and dead cells by macrophages is important for innate immunity and tissue maintenance. Multiple Rab family GTPases engage effector molecules to coordinate the early stages of phagocytosis, which include rapid changes in actin polymerization, membrane phospholipids, trafficking and the activation of receptors. Defining the spatiotemporal, sequential recruitment of these Rabs is critical for insights into how phagocytosis is initiated and coordinated. Here, we screened GFP-tagged Rabs expressed in fixed and live cells to identify and stratify those recruited to early phagocytic membranes at stages defined by phospholipid transitions. We propose a sequence of Rabs 35, 13, 8a, 8b, 27a, 10, and 31 that precedes and accompanies phagocytic cup closure, followed after closure by recruitment of endosomal Rabs 5a, 5b, 5c, 14, and 11. Reducing the expression of individual Rabs by siRNA knockdown, notably Rabs 35 and 13, disrupts phagocytosis prior to phagocytic cup closure, confirming a known role for Rab35 and revealing anew the involvement of Rab13. The results enhance our understanding of innate immune responses in macrophages by revealing the sequence of Rabs that initiates phagocytosis.

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吞噬作用早期Rab gtpase的序贯募集。
巨噬细胞吞噬和破坏病原体和死细胞对先天免疫和组织维持至关重要。多种Rab家族gtpase参与效应分子协调吞噬的早期阶段,包括肌动蛋白聚合、膜磷脂、运输和受体激活的快速变化。定义这些Rabs的时空序列募集对于了解吞噬是如何启动和协调的至关重要。在这里,我们筛选了在固定细胞和活细胞中表达的gfp标记的Rabs,以识别和分层那些在磷脂转变定义的阶段招募到早期吞噬膜的Rabs。我们提出Rabs 35、13、8a、8b、27a、10和31序列在吞噬杯闭合之前和伴随,在吞噬杯闭合之后,内体Rabs 5a、5b、5c、14和11被募集。通过敲低siRNA降低单个Rabs的表达,特别是Rabs 35和Rabs 13,在吞噬杯关闭之前破坏吞噬作用,证实了Rab35的已知作用,并重新揭示了Rab13的参与。该结果通过揭示启动吞噬的Rabs序列,增强了我们对巨噬细胞先天免疫反应的理解。
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