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神经元支架蛋白Shank3介导受体酪氨酸激酶Ret在上皮细胞中的信号传导和生物学功能。

The neuronal scaffold protein Shank3 mediates signaling and biological function of the receptor tyrosine kinase Ret in epithelial cells.

作者信息

Schuetz Gunnar, Rosário Marta, Grimm Jan, Boeckers Tobias M, Gundelfinger Eckart D, Birchmeier Walter

机构信息

MaxDelbrück-Center for Molecular Medicine, Berlin, Germany.

出版信息

J Cell Biol. 2004 Dec 6;167(5):945-52. doi: 10.1083/jcb.200404108. Epub 2004 Nov 29.

Abstract

Shank proteins, initially also described as ProSAP proteins, are scaffolding adaptors that have been previously shown to integrate neurotransmitter receptors into the cortical cytoskeleton at postsynaptic densities. We show here that Shank proteins are also crucial in receptor tyrosine kinase signaling. The PDZ domain-containing Shank3 protein was found to represent a novel interaction partner of the receptor tyrosine kinase Ret, which binds specifically to a PDZ-binding motif present in the Ret9 but not in the Ret51 isoform. Furthermore, we show that Ret9 but not Ret51 induces epithelial cells to form branched tubular structures in three-dimensional cultures in a Shank3-dependent manner. Ret9 but not Ret51 has been previously shown to be required for kidney development. Shank3 protein mediates sustained Erk-MAPK and PI3K signaling, which is crucial for tubule formation, through recruitment of the adaptor protein Grb2. These results demonstrate that the Shank3 adaptor protein can mediate cellular signaling, and provide a molecular mechanism for the biological divergence between the Ret9 and Ret51 isoform.

摘要

支架蛋白最初也被描述为ProSAP蛋白,是一种支架衔接蛋白,此前已证明其能将神经递质受体整合到突触后致密区的皮质细胞骨架中。我们在此表明,支架蛋白在受体酪氨酸激酶信号传导中也至关重要。发现含PDZ结构域的支架蛋白3是受体酪氨酸激酶Ret的一种新型相互作用伙伴,它特异性结合Ret9而非Ret51异构体中存在的PDZ结合基序。此外,我们表明,Ret9而非Ret51以支架蛋白3依赖的方式诱导上皮细胞在三维培养中形成分支管状结构。此前已证明,肾脏发育需要Ret9而非Ret51。支架蛋白3通过募集衔接蛋白Grb2介导持续的Erk-MAPK和PI3K信号传导,这对肾小管形成至关重要。这些结果表明,支架蛋白3衔接蛋白可介导细胞信号传导,并为Ret9和Ret51异构体之间的生物学差异提供了分子机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9efa/2172453/f2596d25ee4b/200404108f1.jpg

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