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The Drosophila Dead end Arf-like3 GTPase controls vesicle trafficking during tracheal fusion cell morphogenesis

机译:果蝇死端Arf样3 GTP酶控制气管融合细胞形态发生过程中的囊泡运输。

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摘要

The Drosophila larval tracheal system consists of a highly branched tubular organ that becomes interconnected by migration-fusion events during embryonic development. Fusion cells at the tip of each branch guide migration, adhere, and then undergo extensive remodeling as the tracheal lumen extends between the two branches. The Drosophila dead end gene is expressed in fusion cells, and encodes an Arf-like3 GTPase. Analyses of dead end RNAi and mutant embryos reveals that the lumen fails to connect between the two branches. Expression of a constitutively active form of Dead end in S2 cells reveal that it influences the state of actin polymerization, and is present on particles that traffic along actin/microtubule-containing processes. Imaging experiments in vivo reveal that Dead end-containing vesicles are associated with recycling endosomes and the exocyst, and control exocyst localization in fusion cells. These results indicate that the Dead end GTPase plays an important role in trafficking membrane components involved in tracheal fusion cell morphogenesis and lumenal development.
机译:果蝇幼虫气管系统由高度分支的管状器官组成,该器官在胚胎发育过程中通过迁移-融合事件相互连接。在每个分支末端的融合细胞引导迁移,粘附,然后随着气管腔在两个分支之间延伸而进行广泛的重塑。果蝇的死端基因在融合细胞中表达,并编码一个Arf-like3 GTPase。死端RNAi和突变体胚胎的分析表明,内腔无法连接两个分支之间。死端的组成型活性形式在S2细胞中的表达表明它会影响肌动蛋白的聚合状态,并存在于沿肌动蛋白/微管过程中运输的颗粒上。体内成像实验表明,含有死端的囊泡与再循环内体和囊泡有关,并控制囊泡在融合细胞中的定位。这些结果表明,死端GTP酶在运输涉及气管融合细胞形态发生和管腔发育的膜成分中起重要作用。

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