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Signal transduction by the Fat cytoplasmic domain

机译:脂肪胞质域的信号转导

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The large atypical cadherin Fat is a receptor for both Hippo and planar cell polarity (PCP) pathways. Here we investigate the molecular basis for signal transduction downstream of Fat by creating targeted alterations within a genomic construct that contains the entire fat locus, and by monitoring and manipulating the membrane localization of the Fat pathway component Dachs. We establish that the human Fat homolog FAT4 lacks the ability to transduce Hippo signaling in Drosophila, but can transduce Drosophila PCP signaling. Targeted deletion of conserved motifs identifies a four amino acid C-terminal motif that is essential for aspects of Fat-mediated PCP, and other internal motifs that contribute to Fat-Hippo signaling. Fat-Hippo signaling requires the Drosophila Casein kinase 1?? encoded by discs overgrown (Dco), and we characterize candidate Dco phosphorylation sites in the Fat intracellular domain (ICD), the mutation of which impairs Fat-Hippo signaling. Through characterization of Dachs localization and directed membrane targeting of Dachs, we show that localization of Dachs influences both the Hippo and PCP pathways. Our results identify a conservation of Fat-PCP signaling mechanisms, establish distinct functions for different regions of the Fat ICD, support the correlation of Fat ICD phosphorylation with Fat-Hippo signaling, and confirm the importance of Dachs membrane localization to downstream signaling pathways. ? 2013.
机译:大的非典型钙粘蛋白脂肪是河马和平面细胞极性(PCP)途径的受体。在这里,我们通过在包含整个脂肪基因座的基因组构建体中创建针对性的改变,以及通过监视和操纵脂肪途径成分Dachs的膜定位,来研究脂肪下游信号转导的分子基础。我们建立了人类脂肪同系物FAT4缺乏在果蝇中转导河马信号转导的能力,但可以转导果蝇PCP信号转导。保守基序的有针对性的删除确定了四个氨基酸的C末端基序,这是对于脂肪介导的PCP方面至关重要的,以及其他有助于脂肪河马信号转导的内部基序。脂肪-河马信号需要果蝇酪蛋白激酶1?由过度生长的光盘(Dco)编码,并且我们表征了脂肪细胞内结构域(ICD)中的候选Dco磷酸化位点,其突变会损害Fat-Hippo信号传导。通过Dachs定位和Dachs的定向膜靶向的表征,我们表明Dachs的定位影响河马和PCP途径。我们的结果确定了Fat-PCP信号传导机制的保守性,为Fat ICD的不同区域建立了不同的功能,支持Fat ICD磷酸化与Fat-Hippo信号传导的相关性,并确认了Dachs膜定位对下游信号传导途径的重要性。 ? 2013。

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