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Understanding the biology of HER3 receptor as a therapeutic target in human cancer

机译:了解HER3受体的生物学特性作为人类癌症的治疗靶标

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HER3 belongs to the human epidermal growth factor receptor (HER) family which also includes HER1/EGFR/erbB1, HER2/erbB2, and HER4/erbB4. As a unique member of the HER family, HER3 lacks or has little intrinsic tyrosine kinase activity. It frequently co-expresses and forms heterodimers with other receptor tyrosine kinases (RTKs) in cancer cells to activate oncogenic signaling, especially the PI-3K/Akt pathway and Src kinase. Elevated expression of HER3 has been observed in a wide variety of human cancers and associates with a worse survival in cancer patients with solid tumors. Studies on the underlying mechanism implicate HER3 expression as a major cause of treatment failure in cancer therapy. Activation of HER3 signaling has also been shown to promote cancer metastasis. These data strongly support the notion that therapeutic inactivation of HER3 and/or its downstream signaling is required to overcome treatment resistance and improve the outcomes of cancer patients.
机译:HER3属于人类表皮生长因子受体(HER)家族,还包括HER1 / EGFR / erbB1,HER2 / erbB2和HER4 / erbB4。作为HER家族的独特成员,HER3缺乏或几乎没有内在的酪氨酸激酶活性。它经常与癌细胞中的其他受体酪氨酸激酶(RTK)共表达并形成异二聚体,从而激活致癌信号,尤其是PI-3K / Akt途径和Src激酶。在多种人类癌症中已观察到HER3的表达升高,并与实体瘤癌症患者的生存期较差有关。对潜在机制的研究表明,HER3表达是癌症治疗中治疗失败的主要原因。 HER3信号转导的激活也已显示可促进癌症转移。这些数据强烈支持以下观念:需要治疗性灭活HER3和/或其下游信号以克服治疗耐药性并改善癌症患者的预后。

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