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促红细胞生成素受体的延伸盒2亚结构域对Jak2激活并非必需,但对FDC-ER细胞中的有效有丝分裂至关重要。

The extended box 2 subdomain of erythropoietin receptor is nonessential for Jak2 activation yet critical for efficient mitogenesis in FDC-ER cells.

作者信息

He T C, Jiang N, Zhuang H, Quelle D E, Wojchowski D M

机构信息

Department of Biochemistry and Molecular Biology, Pennsylvania State University, University Park 16802.

出版信息

J Biol Chem. 1994 Jul 15;269(28):18291-4.

PMID:8034573
Abstract

The development of erythroid progenitor cells depends upon exposure to the glycoprotein hormone, erythropoietin (EPO). Binding of EPO to its transmembrane receptor leads to the rapid tyrosine phosphorylation of several cellular targets including Shc, Raf-1, Gap120, the cloned EPO receptor (EPOR), pp100/97, and a M(r) 130,000 EPO-activated receptor-associated Janus protein tyrosine kinase, Jak2. A membrane-proximal cytosolic region of the EPOR recently has been shown to be essential for the activation of Jak2 and sufficient for EPO-induced mitogenesis. This cytosolic region includes 8-12 amino acid box 1 and box 2 subdomains, which are conserved in certain class I receptors as well as a more distal 10-40 amino acid subdomain (extended box 2 subdomain, ExBx2), which likewise is implicated in mitogenic signaling. Through the expression of EPOR carboxyl-terminal truncation mutants in FDC-P1 cells, we presently show that an EPOR form truncated within the ExBx2 domain efficiently activates Jak2, yet is deficient in mitogenesis. Efficient expression of this mutant receptor at the cell surface and its ability to activate Jak2 indicate that poor mitogenic activity does not result from aberrant transport or folding. Rather, failure of this mutant to support proliferation above nominal rates underlines an apparent role for the EPOR ExBx2 subdomain in the activation of a distinct primary mitogenic effector.

摘要

红系祖细胞的发育依赖于对糖蛋白激素促红细胞生成素(EPO)的暴露。EPO与其跨膜受体结合会导致包括Shc、Raf-1、Gap120、克隆的EPO受体(EPOR)、pp100/97以及一种分子量为130,000的EPO激活的受体相关Janus蛋白酪氨酸激酶Jak2在内的多个细胞靶点快速酪氨酸磷酸化。最近发现,EPOR的膜近端胞质区域对于Jak2的激活至关重要,并且足以介导EPO诱导的有丝分裂。该胞质区域包括8 - 12个氨基酸的框1和框2亚结构域,这些亚结构域在某些I类受体中是保守的,以及一个更远端的10 - 40个氨基酸的亚结构域(扩展框2亚结构域,ExBx2),同样也参与有丝分裂信号传导。通过在FDC - P1细胞中表达EPOR羧基末端截短突变体,我们目前表明,在ExBx2结构域内截短的EPOR形式能够有效地激活Jak2,但在有丝分裂方面存在缺陷。这种突变受体在细胞表面的高效表达及其激活Jak2的能力表明,有丝分裂活性差并非由异常转运或折叠导致。相反,这种突变体无法以高于正常水平的速率支持细胞增殖,这突出了EPOR ExBx2亚结构域在激活一种独特的初级有丝分裂效应器方面的明显作用。

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