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Insulin/IGF signaling and discoidin domain receptors: An emerging functional connection

机译:胰岛素/ IGF信号和盘状蛋白域受体:新兴功能连接

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摘要

The insulin/insulin-like growth factor system (IIGFs) plays a fundamental role in the regulation of prenatal and postnatal growth, metabolism and homeostasis. As a consequence, dysregulation of this axis is associated with growth disturbance, type 2 diabetes, chronic inflammation and tumor progression. A functional crosstalk between IIGFs and discoidin domain receptors (DDRs) has been recently discovered. DDRs are non-integrin collagen receptors that canonically undergo slow and long-lasting autophosphorylation after binding to fibrillar collagen. While both DDR1 and DDR2 functionally interact with IIGFs, the crosstalk with DDR1 is so far better characterized. Notably, the IIGFs-DDR1 crosstalk presents a feed-forward mechanism, which does not require collagen binding, thus identifying novel non-canonical action of DDR1. Further studies are needed to fully explore the role of this IIGFs-DDRs functional loop as potential target in the treatment of inflammatory and neoplastic disorders.
机译:胰岛素/胰岛素样生长因子体系(IIGF)在调节产前和产后生长,代谢和稳态的调节中起着重要作用。 结果,该轴的失调与生长紊乱有关,2型糖尿病,慢性炎症和肿瘤进展相关。 最近发现了IIGF和Discoidin域受体(DDR)之间的功能性串扰。 DDR是非整联蛋白受体,其在与纤维胶原结合后经常经历缓慢和长期的自磷酸化。 虽然DDR1和DDR2都与IIGF功能相互作用,但到目前为止,带有DDR1的串扰是更好的表征。 值得注意的是,IIGFS-DDR1串扰提出了一种前馈机制,其不需要胶原蛋白结合,从而鉴定DDR1的新型非规范作用。 需要进一步的研究来充分探讨这种IIGFS-DDR官能循环作为治疗炎症和肿瘤障碍的潜在目标的作用。

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