极化运输需要 AP-1 介导的 KIF13A 和 KIF13B 在跨高尔基体的招募。

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC
ACS Applied Electronic Materials Pub Date : 2024-05-01 Epub Date: 2024-03-06 DOI:10.1091/mbc.E23-10-0401
Andrew C Montgomery, Christina S Mendoza, Alex Garbouchian, Geraldine B Quinones, Marvin Bentley
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引用次数: 0

摘要

神经元是一种极化细胞,需要准确的膜转运来维持树突和轴突膜上不同的蛋白质补体。Kinesin-3 家族成员 KIF13A 和 KIF13B 被认为介导了树突选择性运输,但它们被招募到极化囊泡的机制以及每种 KIF13 在特定运输作用上的差异尚未明确。我们对培养的海马神经元进行了活细胞成像,发现 KIF13A 是一种专门的树突选择性驱动蛋白。KIF13B 具有两种不同的运输模式,即树突选择性运输和轴突选择性运输。两种 KIF13 都通过与异构四聚体适配蛋白复合物 AP-1 的相互作用维持在跨高尔基网络中。干扰KIF13与AP-1的结合会导致树突和轴突选择性转运的中断。我们认为,AP-1 是将极化货物分选到囊泡和招募驱动蛋白以实现极化运输之间的分子联系。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Polarized transport requires AP-1-mediated recruitment of KIF13A and KIF13B at the trans-Golgi.

Neurons are polarized cells that require accurate membrane trafficking to maintain distinct protein complements at dendritic and axonal membranes. The Kinesin-3 family members KIF13A and KIF13B are thought to mediate dendrite-selective transport, but the mechanism by which they are recruited to polarized vesicles and the differences in the specific trafficking role of each KIF13 have not been defined. We performed live-cell imaging in cultured hippocampal neurons and found that KIF13A is a dedicated dendrite-selective kinesin. KIF13B confers two different transport modes, dendrite- and axon-selective transport. Both KIF13s are maintained at the trans-Golgi network by interactions with the heterotetrameric adaptor protein complex AP-1. Interference with KIF13 binding to AP-1 resulted in disruptions to both dendrite- and axon-selective trafficking. We propose that AP-1 is the molecular link between the sorting of polarized cargoes into vesicles and the recruitment of kinesins that confer polarized transport.

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CiteScore
7.20
自引率
4.30%
发文量
567
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