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A fresh look at the function of Rabaptin5 on endosomes

机译:重新审视Rabaptin5对内体的功能

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摘要

Rab GTPases act as organizers of protein networks defining identities and functions of organelles of the endocytic and secretory pathways. Various modes of coordination between different Rabs drive the timely maturation and conversion of membranes. Endosomal Rab5 has been known as the prime example for self-activation via a feedback loop recruiting Rabaptln5, which is complexed with the Rab5 exchange factor RabexS, and couples to Rab4-GTP. Among other effectors, RabS also recruits the Mon1/SAND1-Ccz1 complex that both activates Rab7 and dissociates RabexS for Rab5-to-Rab7 conversion of early-to-late endosomes. A detailed deletion analysis now revealed 2 separate binding sites each for Rab4-GTP and Rab5-GTP and indicates a feedforward mechanism of Rab5activation. Rabaptin5/Rabex5 is recruited to endosomal membranes positive for Rab4-GTP and ubiquitinated cargo (binding to the ubiquitin binding site of Rabex5). This mechanism also suggests additional criteria for Rab5 inactivation concomitant with increasing Rab7-GTP levels. The disappearance of ubiquitinated cargo upon ESCRT-mediated formation of intraluminal vesicles and inactivation of Rab4 may also contribute to loss of Rab5 activation. Rabaptin5/Rabex5 thus may integrate several cues of maturation to perform Rab conversion. Furthermore Rab5 binding to RabaptinS appears to prevent uncontrolled progression to late endosomes.
机译:Rab GTPases充当蛋白质网络的组织者,定义了内吞和分泌途径细胞器的身份和功能。不同的Rabs之间的各种协调模式驱动膜的及时成熟和转化。内体Rab5是通过反馈回路募集Rabaptln5(与Rab5交换因子RabexS复合并与Rab4-GTP结合)的反馈回路而被称为自我激活的主要实例。在其他效应子中,RabS还募集了Mon1 / SAND1-Ccz1复合物,该复合物既激活Rab7,又使RabexS解离,以实现早期到晚期内体的Rab5-to-Rab7转化。现在进行了详细的缺失分析,揭示了Rab4-GTP和Rab5-GTP各自具有2个独立的结合位点,并表明了Rab5激活的前馈机制。 Rabaptin5 / Rabex5被募集到对Rab4-GTP和泛素化的货物呈阳性(结合到Rabex5的泛素结合位点)呈阳性的内体膜。该机制还提出了与Rab7-GTP水平升高相伴的Rab5灭活的附加标准。 ESCRT介导的腔内囊泡形成后,泛素化货物的消失和Rab4的失活也可能导致Rab5的丧失。 Rabaptin5 / Rabex5可能因此整合了几种成熟的线索以执行Rab转换。此外,Rab5与RabaptinS的结合似乎可以防止不受控制地发展为晚期内体。

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