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转录调控 F-肌动蛋白成核因子 Spire 构建的树突状结构。

Dendrite architecture organized by transcriptional control of the F-actin nucleator Spire.

机构信息

McGill Centre for Research in Neuroscience, McGill University Health Centre, 1650 Cedar Avenue, Montreal, QC H3G 1A4, Canada.

出版信息

Development. 2014 Feb;141(3):650-60. doi: 10.1242/dev.099655.

Abstract

The architectures of dendritic trees are crucial for the wiring and function of neuronal circuits because they determine coverage of receptive territories, as well as the nature and strength of sensory or synaptic inputs. Here, we describe a cell-intrinsic pathway sculpting dendritic arborization (da) neurons in Drosophila that requires Longitudinals Lacking (Lola), a BTB/POZ transcription factor, and its control of the F-actin cytoskeleton through Spire (Spir), an actin nucleation protein. Loss of Lola from da neurons reduced the overall length of dendritic arbors, increased the expression of Spir, and produced inappropriate F-actin-rich dendrites at positions too near the cell soma. Selective removal of Lola from only class IV da neurons decreased the evasive responses of larvae to nociception. The increased Spir expression contributed to the abnormal F-actin-rich dendrites and the decreased nocifensive responses because both were suppressed by reduced dose of Spir. Thus, an important role of Lola is to limit expression of Spir to appropriate levels within da neurons. We found Spir to be expressed in dendritic arbors and to be important for their development. Removal of Spir from class IV da neurons reduced F-actin levels and total branch number, shifted the position of greatest branch density away from the cell soma, and compromised nocifensive behavior. We conclude that the Lola-Spir pathway is crucial for the spatial arrangement of branches within dendritic trees and for neural circuit function because it provides balanced control of the F-actin cytoskeleton.

摘要

树突的结构对于神经元回路的连接和功能至关重要,因为它们决定了感受域的覆盖范围,以及感觉或突触输入的性质和强度。在这里,我们描述了一个内在的细胞途径,该途径可塑造果蝇中的树突分支(da)神经元,该途径需要 Longitudinals Lacking(Lola),一种 BTB/POZ 转录因子,以及其通过 Spire(Spir)控制 F-肌动蛋白细胞骨架的作用,Spire 是一种肌动蛋白成核蛋白。da 神经元中 Lola 的缺失减少了树突分支的总长度,增加了 Spir 的表达,并在离细胞体太近的位置产生了不适当的富含 F-肌动蛋白的树突。仅从第四类 da 神经元中选择性去除 Lola 减少了幼虫对伤害感受的逃避反应。增加的 Spir 表达导致异常的富含 F-肌动蛋白的树突和降低的伤害感受反应,因为两者都被减少的 Spir 剂量所抑制。因此,Lola 的一个重要作用是将 Spir 的表达限制在 da 神经元内的适当水平。我们发现 Spir 在树突中表达,并对其发育很重要。从第四类 da 神经元中去除 Spir 会降低 F-肌动蛋白水平和总分支数量,使最大分支密度的位置远离细胞体,并损害伤害感受行为。我们得出结论,Lola-Spir 途径对于树突内分支的空间排列以及神经回路功能至关重要,因为它提供了 F-肌动蛋白细胞骨架的平衡控制。

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