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开曼共济失调蛋白 caytaxin 通过与驱动蛋白轻链结合,沿神经突由驱动蛋白运输。

Cayman ataxia protein caytaxin is transported by kinesin along neurites through binding to kinesin light chains.

机构信息

Nara Institute of Science and Technology, 8916-5 Takayama, Ikoma, Nara 630-0192, Japan.

出版信息

J Cell Sci. 2009 Nov 15;122(Pt 22):4177-85. doi: 10.1242/jcs.048579. Epub 2009 Oct 27.

DOI:10.1242/jcs.048579
PMID:19861499
Abstract

Deficiency of caytaxin results in hereditary ataxia or dystonia in humans, mice and rats. Our yeast two-hybrid screen identified kinesin light chains (KLCs) as caytaxin-binding proteins. The tetratricopeptide-repeat region of KLC1 recognizes the ELEWED sequence (amino acids 115-120) of caytaxin. This motif is conserved among BNIP-2 family members and other KLC-interacting kinesin cargo proteins such as calsyntenins. Caytaxin associates with kinesin heavy chains (KHCs) indirectly by binding to KLCs, suggesting that caytaxin binds to the tetrameric kinesin molecule. In cultured hippocampal neurons, we found that caytaxin is distributed in both axons and dendrites in punctate patterns, and it colocalizes with microtubules and KHC. GFP-caytaxin expressed in hippocampal neurons is transported at a speed ( approximately 1 mum/second) compatible with kinesin movement. Inhibition of kinesin-1 by dominant-negative KHC decreases the accumulation of caytaxin in the growth cone. Caytaxin puncta do not coincide with vesicles containing known kinesin cargos such as APP or JIP-1. A part of caytaxin, however, colocalizes with mitochondria and suppression of caytaxin expression by RNAi redistributes mitochondria away from the distal ends of neurites. These data indicate that caytaxin binds to kinesin-1 and functions as an adaptor that mediates intracellular transport of specific cargos, one of which is the mitochondrion.

摘要

Caytaxin 缺失会导致人类、小鼠和大鼠遗传性共济失调或肌张力障碍。我们的酵母双杂交筛选鉴定出线粒体动力相关蛋白轻链(KLC)为 caytaxin 的结合蛋白。KLC1 的四肽重复区识别 caytaxin 的 ELEWED 序列(氨基酸 115-120)。该基序在 BNIP-2 家族成员和其他与 KLC 相互作用的驱动蛋白货物蛋白(如 calsyntenin)中保守。Caytaxin 通过与 KLC 结合间接与驱动蛋白重链(KHC)结合,表明 caytaxin 结合到四聚体驱动蛋白分子上。在培养的海马神经元中,我们发现 caytaxin 以点状模式分布在轴突和树突中,并且与微管和 KHC 共定位。在海马神经元中表达的 GFP-caytaxin 以与驱动蛋白运动相兼容的速度(约 1 µm/秒)运输。通过显性负性 KHC 抑制驱动蛋白-1 会减少 caytaxin 在生长锥中的积累。Caytaxin 斑点与包含已知驱动蛋白货物(如 APP 或 JIP-1)的囊泡不重合。然而,caytaxin 的一部分与线粒体共定位,并且 RNAi 抑制 caytaxin 的表达会将线粒体从神经突的远端重新分布。这些数据表明 caytaxin 与驱动蛋白-1 结合并作为衔接子起作用,介导特定货物的细胞内运输,其中之一是线粒体。

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