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The atypical cadherin Celsr1 functions non-cell autonomously to block rostral migration of facial branchiomotor neurons in mice

机译:非典型钙粘蛋白CLE1功能非细胞自主地阻止面部枝孢子神经元在小鼠中的rostral迁移

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The caudal migration of facial branchiomotor (FBM) neurons from rhombomere (r) 4 to r6 in the hindbrain is an excellent model to study neuronal migration mechanisms. Although several Wnt/Planar Cell Polarity (PCP) components are required for FBM neuron migration, only Celsr1, an atypical cadherin, regulates the direction of migration in mice. In Celsr1 mutants, a subset of FBM neurons migrates rostrally instead of caudally. Interestingly, Celsr1 is not expressed in the migrating FBM neurons, but rather in the adjacent floor plate and adjoining ventricular zone. To evaluate the contribution of different expression domains to neuronal migration, we conditionally inactivated Celsr1 in specific cell types. Intriguingly, inactivation of Celsr1 in the ventricular zone of r3-r5, but not in the floor plate, leads to rostral migration of FBM neurons, greatly resembling the migration defect of Celsr1 mutants. Dye fill experiments indicate that the rostrally-migrated FBM neurons in Celsr1 mutants originate from the anterior margin of r4. These data suggest strongly that Celsr1 ensures that FBM neurons migrate caudally by suppressing molecular cues in the rostra( hindbrain that can attract FBM neurons. (C) 2016 Elsevier Inc. All rights reserved.
机译:在后脑中菱形(R)4至R6的面部枝核球(FBM)神经元的尾部迁移是研究神经元迁移机制的优秀模型。虽然FBM神经元迁移需要几种WNT /平面细胞极性(PCP)组分,但仅CLSR1,非典型钙粘蛋白,调节小鼠中迁移的方向。在CELSR1突变体中,FBM神经元的子集迁移主动而不是尾骨。有趣的是,CELSR1在迁移的FBM神经元中不表达,而是在相邻的底板和相邻的心室区域中表达。为了评估不同表达域对神经元迁移的贡献,我们有条件地在特定细胞类型中灭活的CLE1。有趣的是,R3-R5的心室区域中Celsr1的灭活,但不在地板上,导致FBM神经元的升振偏移,大大类似于Celsr1突变体的迁移缺陷。染料填充实验表明,CELSR1突变体中的升峰迁移的FBM神经元源自R4的前缘。这些数据强烈表明,CELSR1确保FBM神经元通过抑制ROSTRA中的分子提示(可以吸引FBM神经元的后脑的分子提示而均匀迁移。(C)2016 Elsevier Inc.保留所有权利。

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