首页> 美国卫生研究院文献>Cell Regulation >A chimeric serine/threonine kinase receptor system reveals the potential of multiple type II receptors to cooperate with transforming growth factor-beta type I receptor.
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A chimeric serine/threonine kinase receptor system reveals the potential of multiple type II receptors to cooperate with transforming growth factor-beta type I receptor.

机译:嵌合的丝氨酸/苏氨酸激酶受体系统揭示了多种II型受体与转化生长因子βI型受体协同作用的潜力。

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摘要

Receptor-type serine/threonine kinases (RSKs) have been organized into two distinct classes known as types I and II on the basis of sequence similarity. However, experiments have shown ligand specificities in the two classes and as a result type I and type II receptors can often bind to a common ligand. The transforming growth factor-beta- (TGF-beta) specific receptors represent such a case, where both type I and II receptors (T beta RI and T beta RII) are observed. Of additional interest is the observation that heteromeric associations of type I and II receptors can also enable signaling. To further elucidate the function of various RSKs, the extracellular domains of both alpha and beta chains from human granulocyte-macrophage colony-stimulating factor receptors were linked to transmembrane cytoplasmic domains of RSKs. Chimeric receptors of human granulocyte-macrophage receptor (hGMR) alpha with T beta RI and hGMR beta with T beta RII were expressed in murine pre-B cell-derived Ba/F3 cells. These chimeras formed heteromeric complexes, transmitted TGF-beta signals, and were down-modulated in response to human granulocyte-macrophage colony-stimulating factor. However, experiments utilizing these chimeric receptors in different combinations revealed that only heteromeric associations of transmembrane cytoplasmic domains mediated signaling and down-modulation. Chimeric receptors with transmembrane cytoplasmic domains of activin receptor type II and bone morphogenetic protein receptor type II also provided signals in conjunction with chimeric T beta RI. As a result, these type II receptors may share a common potential to signal via T beta RI. hGMR-RSK chimeric receptors may be useful tools for the identification and characterization of the divergent signals mediated by individual RSKs.
机译:受体类型的丝氨酸/苏氨酸激酶(RSK)已根据序列相似性分为两类,分别称为I型和II型。但是,实验表明这两种配体都具有特异性,因此I型和II型受体通常可以结合到一个普通的配体上。转化生长因子-β-(TGF-β)特异性受体代表了这种情况,其中同时观察到I型和II型受体(T beta RI和T beta RII)。另一个有趣的发现是,I型和II型受体的异源结合也可以实现信号传导。为了进一步阐明各种RSK的功能,将来自人类粒细胞-巨噬细胞集落刺激因子受体的α和β链的胞外域与RSK的跨膜胞质域相连。人粒细胞巨噬细胞受体(hGMR)alpha与T beta RI的嵌合受体和hGMR beta与T beta RII的嵌合受体在鼠pre-B细胞衍生的Ba / F3细胞中表达。这些嵌合体形成异源复合物,传递TGF-β信号,并响应人类粒细胞-巨噬细胞集落刺激因子而被下调。然而,以不同组合利用这些嵌合受体的实验表明,跨膜细胞质结构域的仅异源缔合介导信号传导和下调。具有激活蛋白II型跨膜细胞质结构域和II型骨形态发生蛋白受体的跨膜细胞质结构域的嵌合受体也提供与嵌合TβRI结合的信号。结果,这些II型受体可能具有共同的潜力,可以通过T beta RI发出信号。 hGMR-RSK嵌合受体可能是有用的工具,用于鉴定和表征由单个RSK介导的发散信号。

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