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Neuron. 2009 Dec 10;64(5):663-77. doi: 10.1016/j.neuron.2009.11.002.
2
A precise and rapid mapping protocol for correlative light and electron microscopy of small invertebrate organisms.一种用于小型无脊椎动物生物的光镜和电镜相关研究的精确、快速的图谱绘制方案。
Biol Cell. 2009 Dec 4;102(2):121-32. doi: 10.1042/BC20090096.
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Assembling the presynaptic active zone.组装突触前活性区。
Curr Opin Neurobiol. 2009 Jun;19(3):311-8. doi: 10.1016/j.conb.2009.03.003. Epub 2009 Apr 22.
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Clathrin adaptor AP-1 complex excludes multiple postsynaptic receptors from axons in C. elegans.网格蛋白衔接蛋白AP-1复合物在秀丽隐杆线虫中阻止多种突触后受体进入轴突。
Proc Natl Acad Sci U S A. 2009 Feb 3;106(5):1632-7. doi: 10.1073/pnas.0812078106. Epub 2009 Jan 21.
5
The JIP3 scaffold protein UNC-16 regulates RAB-5 dependent membrane trafficking at C. elegans synapses.支架蛋白JIP3的UNC-16调控秀丽隐杆线虫突触处RAB-5依赖的膜转运。
Dev Neurobiol. 2009;69(2-3):174-90. doi: 10.1002/dneu.20690.
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UNC-6/netrin and its receptor UNC-5 locally exclude presynaptic components from dendrites.UNC-6/网蛋白及其受体UNC-5在局部将突触前成分排除在树突之外。
Nature. 2008 Oct 2;455(7213):669-73. doi: 10.1038/nature07291.
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Molecular mechanisms of presynaptic differentiation.突触前分化的分子机制
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The transmembrane segment of Tom20 is recognized by Mim1 for docking to the mitochondrial TOM complex.Tom20的跨膜片段被Mim1识别,以便对接至线粒体TOM复合体。
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Polyunsaturated fatty acids influence synaptojanin localization to regulate synaptic vesicle recycling.多不饱和脂肪酸影响突触素定位以调节突触小泡循环。
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10
Ultrastructural localization of active zone and synaptic vesicle proteins in a preassembled multi-vesicle transport aggregate.活性区和突触小泡蛋白在预组装的多囊泡运输聚集体中的超微结构定位。
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Arf 样小 G 蛋白 ARL-8 通过抑制囊泡聚集促进突触前 cargo 的轴突运输。

An Arf-like small G protein, ARL-8, promotes the axonal transport of presynaptic cargoes by suppressing vesicle aggregation.

机构信息

Howard Hughes Medical Institute, Department of Biology, Stanford University, Stanford, CA 94305, USA.

出版信息

Neuron. 2010 Jun 10;66(5):710-23. doi: 10.1016/j.neuron.2010.04.033.

DOI:10.1016/j.neuron.2010.04.033
PMID:20547129
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3168544/
Abstract

Presynaptic assembly requires the packaging of requisite proteins into vesicular cargoes in the cell soma, their long-distance microtubule-dependent transport down the axon, and, finally, their reconstitution into functional complexes at prespecified sites. Despite the identification of several molecules that contribute to these events, the regulatory mechanisms defining such discrete states remain elusive. We report the characterization of an Arf-like small G protein, ARL-8, required during this process. arl-8 mutants prematurely accumulate presynaptic cargoes within the proximal axon of several neuronal classes, with a corresponding failure to assemble presynapses distally. This proximal accumulation requires the activity of several molecules known to catalyze presynaptic assembly. Dynamic imaging studies reveal that arl-8 mutant vesicles exhibit an increased tendency to form immotile aggregates during transport. Together, these results suggest that arl-8 promotes a trafficking identity for presynaptic cargoes, facilitating their efficient transport by repressing premature self-association.

摘要

突触前装配需要将必需的蛋白质包装到细胞体中的囊泡货物中,这些蛋白质需要沿着轴突进行远距离微管依赖性运输,最后,它们在特定的部位重新组装成功能性复合物。尽管已经鉴定出了几种有助于这些事件的分子,但定义这些离散状态的调节机制仍然难以捉摸。我们报告了一种 Arf 样小 G 蛋白 ARL-8 的特征,该蛋白在这个过程中是必需的。arl-8 突变体在几种神经元类别的近端轴突中过早地积累突触前货物,而在远端则无法组装突触前。这种近端积累需要几种已知能催化突触前装配的分子的活性。动态成像研究表明,arl-8 突变体囊泡在运输过程中表现出增加的形成非运动性聚集的趋势。总之,这些结果表明 arl-8 促进了突触前货物的运输特性,通过抑制过早的自组装来促进它们的有效运输。