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载脂蛋白E受体2的一种分泌型可溶性形式作为一种显性负性受体发挥作用,并抑制Reelin信号传导。

A secreted soluble form of ApoE receptor 2 acts as a dominant-negative receptor and inhibits Reelin signaling.

作者信息

Koch Stefanie, Strasser Vera, Hauser Christoph, Fasching Daniela, Brandes Christian, Bajari Tarek M, Schneider Wolfgang J, Nimpf Johannes

机构信息

The Institute of Medical Biochemistry, Department of Molecular Genetics, BioCenter and University of Vienna, Vienna, Austria.

出版信息

EMBO J. 2002 Nov 15;21(22):5996-6004. doi: 10.1093/emboj/cdf599.

Abstract

Specialized neurons throughout the developing central nervous system secrete Reelin, which binds to ApoE receptor 2 (ApoER2) and very low density lipoprotein receptor (VLDLR), triggering a signal cascade that guides neurons to their correct position. Binding of Reelin to ApoER2 and VLDLR induces phosphorylation of Dab1, which binds to the intracellular domains of both receptors. Due to differential splicing, several isoforms of ApoER2 differing in their ligand-binding and intracellular domains exist. One isoform harbors four binding repeats plus an adjacent short 13 amino acid insertion containing a furin cleavage site. It is not known whether furin processing of this ApoER2 variant actually takes place and, if so, whether the produced fragment is secreted. Here we demonstrate that cleavage of this ApoER2 variant does indeed take place, and that the resulting receptor fragment consisting of the entire ligand-binding domain is secreted as soluble polypeptide. This receptor fragment inhibits Reelin signaling in primary neurons, indicating that it can act in a dominant-negative fashion in the regulation of Reelin signaling during embryonic brain development.

摘要

在整个发育中的中枢神经系统中,特化神经元分泌Reelin,它与载脂蛋白E受体2(ApoER2)和极低密度脂蛋白受体(VLDLR)结合,触发一个信号级联反应,引导神经元到达其正确位置。Reelin与ApoER2和VLDLR的结合诱导Dab1磷酸化,Dab1与这两种受体的细胞内结构域结合。由于可变剪接,存在几种在配体结合和细胞内结构域方面不同的ApoER2亚型。一种亚型含有四个结合重复序列以及一个相邻的包含弗林蛋白酶切割位点的13个氨基酸的短插入序列。尚不清楚这种ApoER2变体的弗林蛋白酶加工是否实际发生,如果发生,产生的片段是否会被分泌。在这里,我们证明这种ApoER2变体确实会发生切割,并且由整个配体结合结构域组成的所得受体片段作为可溶性多肽被分泌。这种受体片段在原代神经元中抑制Reelin信号传导,表明它在胚胎脑发育过程中对Reelin信号传导的调节中可以以显性负性方式起作用。

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引用本文的文献

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ApoER2: Functional Tuning Through Splicing.载脂蛋白E受体2:通过剪接进行功能调节
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