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UNC-4 antagonizes Wnt signaling to regulate synaptic choice in the C. elegans motor circuit

机译:UNC-4拮抗Wnt信号转导线虫运动回路中的突触选择。

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摘要

Coordinated movement depends on the creation of synapses between specific neurons in the motor circuit. In C. elegans, this important decision is regulated by the UNC-4 homeodomain protein. unc-4 mutants are unable to execute backward locomotion because VA motor neurons are mis-wired with inputs normally reserved for their VB sisters. We have proposed that UNC-4 functions in VAs to block expression of VB genes. This model is substantiated by the finding that ectopic expression of the VB gene ceh-12 (encoding a homolog of the homeodomain protein HB9) in unc-4 mutants results in the mis-wiring of posterior VA motor neurons with VB-like connections. Here, we show that VA expression of CEH-12 depends on a nearby source of the Wnt protein EGL-20. Our results indicate that UNC-4 prevents VAs from responding to a local EGL-20 cue by disabling a canonical Wnt signaling cascade involving the Frizzled receptors MIG-1 and MOM-5. CEH-12 expression in VA motor neurons is also opposed by a separate pathway that includes the Wnt ligand LIN-44. This work has revealed a transcriptional mechanism for modulating the sensitivity of specific neurons to diffusible Wnt ligands and thereby defines distinct patterns of synaptic connectivity. The existence of comparable Wnt gradients in the vertebrate spinal cord could reflect similar roles for Wnt signaling in vertebrate motor circuit assembly.
机译:协调运动取决于运动回路中特定神经元之间突触的产生。在秀丽隐杆线虫中,这一重要决定由UNC-4同源域蛋白调节。 unc-4突变体无法执行向后运动,因为VA运动神经元与通常为其VB姐妹保留的输入接线错误。我们已经提出,UNC-4在VA中发挥功能来阻止VB基因的表达。该模型通过发现unc-4突变体中VB基因ceh-12(编码同源结构域蛋白HB9的同源物)的异位表达导致与VB样连接的后VA运动神经元的错误接线而得到证实。在这里,我们显示CEH-12的VA表达取决于Wnt蛋白EGL-20的附近来源。我们的结果表明,UNC-4通过禁用涉及卷曲的受体MIG-1和MOM-5的经典Wnt信号级联反应,从而防止VA对局部EGL-20信号作出反应。 VA运动神经元中CEH-12的表达也受到包含Wnt配体LIN-44的单独途径的反对。这项工作揭示了一种转录机制,可调节特定神经元对可扩散Wnt配体的敏感性,从而定义突触连接的不同模式。脊椎动物脊髓中可比的Wnt梯度的存在可能反映出Wnt信号在脊椎动物运动回路装配中的相似作用。

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