Pielage Jan, Fetter Richard D, Davis Graeme W
Department of Biochemistry and Biophysics, University of California, San Francisco, San Francisco, CA 94143, USA.
J Cell Biol. 2006 Nov 6;175(3):491-503. doi: 10.1083/jcb.200607036.
Synaptic connections are established with characteristic, cell type-specific size and spacing. In this study, we document a role for the postsynaptic Spectrin skeleton in this process. We use transgenic double-stranded RNA to selectively eliminate alpha-Spectrin, beta-Spectrin, or Ankyrin. In the absence of postsynaptic alpha- or beta-Spectrin, active zone size is increased and spacing is perturbed. In addition, subsynaptic muscle membranes are significantly altered. However, despite these changes, the subdivision of the synapse into active zone and periactive zone domains remains intact, both pre- and postsynaptically. Functionally, altered active zone dimensions correlate with an increase in quantal size without a change in presynaptic vesicle size. Mechanistically, beta-Spectrin is required for the localization of alpha-Spectrin and Ankyrin to the postsynaptic membrane. Although Ankyrin is not required for the localization of the Spectrin skeleton to the neuromuscular junction, it contributes to Spectrin-mediated synapse development. We propose a model in which a postsynaptic Spectrin-actin lattice acts as an organizing scaffold upon which pre- and postsynaptic development are arranged.
突触连接以特定的、细胞类型特异性的大小和间距建立。在本研究中,我们记录了突触后血影蛋白骨架在此过程中的作用。我们使用转基因双链RNA选择性地消除α-血影蛋白、β-血影蛋白或锚蛋白。在没有突触后α-或β-血影蛋白的情况下,活性区大小增加且间距受到干扰。此外,突触下肌膜发生显著改变。然而,尽管有这些变化,突触在突触前和突触后分为活性区和活性周围区的划分仍然完整。在功能上,活性区尺寸的改变与量子大小的增加相关,而突触前囊泡大小没有变化。从机制上讲,β-血影蛋白是α-血影蛋白和锚蛋白定位于突触后膜所必需的。虽然锚蛋白对于血影蛋白骨架定位于神经肌肉接头不是必需的,但它有助于血影蛋白介导的突触发育。我们提出了一个模型,其中突触后血影蛋白-肌动蛋白晶格作为一个组织支架,在此基础上安排突触前和突触后的发育。
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