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Chemokines induce axon outgrowth downstream of Hepatocyte Growth Factor and TCF/β-catenin signaling

机译:趋化因子诱导肝细胞生长因子下游的轴突生长和TCF /β-catenin信号传导

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摘要

Axon morphogenesis is a complex process regulated by a variety of secreted molecules, including morphogens and growth factors, resulting in the establishment of the neuronal circuitry. Our previous work demonstrated that growth factors [Neurotrophins (NT) and Hepatocyte Growth Factor (HGF)] signal through β-catenin during axon morphogenesis. HGF signaling promotes axon outgrowth and branching by inducing β-catenin phosphorylation at Y142 and transcriptional regulation of T-Cell Factor (TCF) target genes. Here, we asked which genes are regulated by HGF signaling during axon morphogenesis. An array screening indicated that HGF signaling elevates the expression of chemokines of the CC and CXC families. In line with this, CCL7, CCL20, and CXCL2 significantly increase axon outgrowth in hippocampal neurons. Experiments using blocking antibodies and chemokine receptor antagonists demonstrate that chemokines act downstream of HGF signaling during axon morphogenesis. In addition, qPCR data demonstrates that CXCL2 and CCL5 expression is stimulated by HGF through Met/b-catenin/TCF pathway. These results identify CC family members and CXCL2 chemokines as novel regulators of axon morphogenesis downstream of HGF signaling.
机译:轴突形态发生是一个复杂的过程,受多种分泌分子(包括形态发生子和生长因子)调控,从而导致神经元回路的建立。我们以前的工作表明,在轴突形态发生过程中,生长因子[神经营养因子(NT)和肝细胞生长因子(HGF)]通过β-catenin发出信号。 HGF信号传导通过诱导Y142处的β-catenin磷酸化和T细胞因子(TCF)靶基因的转录调控来促进轴突生长和分支。在这里,我们问轴突形态发生过程中哪些基因受HGF信号传导调控。阵列筛选表明,HGF信号传导提高了CC和CXC家族趋化因子的表达。与此相一致,CCL7,CCL20和CXCL2显着增加海马神经元的轴突生长。使用封闭抗体和趋化因子受体拮抗剂的实验表明,趋化因子在轴突形态发生过程中在HGF信号传导的下游起作用。此外,qPCR数据表明HGF通过Met / b-catenin / TCF途径刺激CXCL2和CCL5表达。这些结果确定CC家庭成员和CXCL2趋化因子是HGF信号下游的轴突形态发生的新型调节剂。

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