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Spatial control of Draper receptor signaling initiates apoptotic cell engulfment

机译:Draper受体信号传导的空间控制引发凋亡细胞吞噬

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摘要

The engulfment of apoptotic cells is essential for tissue homeostasis and recovering from damage. Engulfment is mediated by receptors that recognize ligands exposed on apoptotic cells such as phosphatidylserine (PS). In this study, we convert Drosophila melanogaster S2 cells into proficient phagocytes by transfecting the Draper engulfment receptor and replacing apoptotic cells with PS-coated beads. Similar to the T cell receptor (TCR), PS-ligated Draper forms dynamic microclusters that recruit cytosolic effector proteins and exclude a bulky transmembrane phosphatase, consistent with a kinetic segregation-based triggering mechanism. However, in contrast with the TCR, localized signaling at Draper microclusters results in time-dependent depletion of actin filaments, which facilitates engulfment. The Draper–PS extracellular module can be replaced with FRB and FKBP, respectively, resulting in a rapamycin-inducible engulfment system that can be programmed toward defined targets. Collectively, our results reveal mechanistic similarities and differences between the receptors involved in apoptotic corpse clearance and mammalian immunity and demonstrate that engulfment can be reprogrammed toward nonnative targets.
机译:凋亡细胞的吞噬对于组织稳态和从损伤中恢复是必不可少的。吞噬由识别暴露在凋亡细胞上的配体(例如磷脂酰丝氨酸(PS))的受体介导。在这项研究中,我们通过转染Draper吞噬受体并用PS包被的珠粒替代凋亡细胞,将果蝇S2细胞转化为吞噬细胞。与T细胞受体(TCR)相似,与PS连接的Draper形成动态微簇,可募集细胞溶质效应蛋白并排除庞大的跨膜磷酸酶,这与基于动力学分离的触发机制一致。但是,与TCR相比,Draper微簇上的局部信号传导导致肌动蛋白丝的时间依赖性消耗,这有利于吞噬。 Draper-PS细胞外模块可以分别用FRB和FKBP代替,从而形成雷帕霉素诱导的吞噬系统,可以将其编程为确定的靶标。总的来说,我们的结果揭示了参与凋亡小体清除和哺乳动物免疫力的受体之间的机制相似性和差异性,并证明吞噬可以重新编程为非天然靶标。

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