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III 型中间丝周围蛋白在体外抑制 II 型螺旋神经节神经元的神经突生成。

Type III intermediate filament peripherin inhibits neuritogenesis in type II spiral ganglion neurons in vitro.

机构信息

Department of Physiology, The University of Auckland, Private Bag 92019, Auckland, New Zealand.

出版信息

Neurosci Lett. 2010 Jul 5;478(2):51-5. doi: 10.1016/j.neulet.2010.01.063. Epub 2010 Feb 2.

Abstract

Peripherin, a type III intermediate filament protein, forms part of the cytoskeleton in a subset of neurons, most of which have peripheral fibre projections. Studies suggest a role for peripherin in axon outgrowth and regeneration, but evidence for this in sensory and brain tissues is limited. The exclusive expression of peripherin in a sub-population of primary auditory neurons, the type II spiral ganglion neurons (SGN) prompted our investigation of the effect of peripherin gene deletion (pphKO) on these neurons. We used confocal immunofluorescence to examine the establishment of the innervation of the cochlear outer hair cells by the type II SGN neurites in vivo and in vitro, in wildtype (WT) and pphKO mice, in the first postnatal week. The distribution of the type II SGN nerve fibres was normal in pphKO cochleae. However, using P1 spiral ganglion explants under culture conditions where the majority of neurites were derived from type II SGN, pphKO resulted in increased numbers of neurites/explant compared to WT controls. Type II SGN neurites from pphKO explants extended approximately double the distance of WT neurites, and had reduced complexity based on greater distance between turning points. Addition of brain-derived neurotrophic factor (BDNF) to the culture media increased neurite number in WT and KO explants approximately 30-fold, but did not affect neurite length or distance between turning. These results indicate that peripherin may interact with other cytoskeletal elements to regulate outgrowth of the peripheral neurites of type II SGN, distinguishing these neurons from the type I SGN innervating the inner hair cells.

摘要

周围蛋白是一种 III 型中间丝蛋白,构成了一部分具有外周纤维投射的神经元细胞骨架的一部分。研究表明,周围蛋白在轴突生长和再生中起作用,但在感觉和脑组织中,这方面的证据有限。周围蛋白仅在一小部分初级听觉神经元中表达,即 II 型螺旋神经节神经元(SGN),这促使我们研究周围蛋白基因缺失(pphKO)对这些神经元的影响。我们使用共聚焦免疫荧光技术,在体内和体外研究了 WT 和 pphKO 小鼠出生后第一周,II 型 SGN 神经突对耳蜗外毛细胞的支配建立情况。在 pphKO 耳蜗中,II 型 SGN 神经纤维的分布正常。然而,在培养条件下使用 P1 螺旋神经节外植体,其中大多数神经突来源于 II 型 SGN,与 WT 对照组相比,pphKO 导致神经突/外植体数量增加。与 WT 神经突相比,来自 pphKO 外植体的 II 型 SGN 神经突的延伸距离约为两倍,并且由于转折点之间的距离增加,复杂性降低。向培养物中添加脑源性神经营养因子(BDNF)可使 WT 和 KO 外植体的神经突数量增加约 30 倍,但不会影响神经突长度或转折点之间的距离。这些结果表明,周围蛋白可能与其他细胞骨架元件相互作用,以调节 II 型 SGN 外周神经突的生长,从而将这些神经元与支配内毛细胞的 I 型 SGN 区分开来。

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