• 主题
高级搜索  >
历史搜索 清空历史
首页> 外文OA文献 >HER2 oncogenic function escapes EGFR tyrosine kinase inhibitors via activation of alternative HER receptors in breast cancer cells.
【2h】

HER2 oncogenic function escapes EGFR tyrosine kinase inhibitors via activation of alternative HER receptors in breast cancer cells.

机译:HER2致癌功能通过激活乳腺癌细胞中替代性HER受体而逃脱EGFR酪氨酸激酶抑制剂。

代理获取
本网站仅为用户提供外文OA文献查询和代理获取服务,本网站没有原文。下单后我们将采用程序或人工为您竭诚获取高质量的原文,但由于OA文献来源多样且变更频繁,仍可能出现获取不到、文献不完整或与标题不符等情况,如果获取不到我们将提供退款服务。请知悉。
获取外文期刊封面目录资料
页面导航
  • 摘要
  • 著录项
  • 相似文献
  • 相关主题

摘要

BACKGROUND: The response rate to EGFR tyrosine kinase inhibitors (TKIs) may be poor and unpredictable in cancer patients with EGFR expression itself being an inadequate response indicator. There is limited understanding of the mechanisms underlying this resistance. Furthermore, although TKIs suppress the growth of HER2-overexpressing breast tumor cells, they do not fully inhibit HER2 oncogenic function at physiological doses. METHODOLOGY AND PRINCIPAL FINDINGS: Here we have provided a molecular mechanism of how HER2 oncogenic function escapes TKIs' inhibition via alternative HER receptor activation as a result of autocrine ligand release. Using both Förster Resonance Energy Transfer (FRET) which monitors in situ HER receptor phosphorylation as well as classical biochemical analysis, we have shown that the specific tyrosine kinase inhibitors (TKIs) of EGFR, AG1478 and Iressa (Gefitinib) decreased EGFR and HER3 phosphorylation through the inhibition of EGFR/HER3 dimerization. Consequent to this, we demonstrate that cleavage of HER4 and dimerization of HER4/HER2 occur together with reactivation of HER3 via HER2/HER3, leading to persistent HER2 phosphorylation in the now resistant, surviving cells. These drug treatment-induced processes were found to be mediated by the release of ligands including heregulin and betacellulin that activate HER3 and HER4 via HER2. Whereas an anti-betacellulin antibody in combination with Iressa increased the anti-proliferative effect in resistant cells, ligands such as heregulin and betacellulin rendered sensitive SKBR3 cells resistant to Iressa. CONCLUSIONS AND SIGNIFICANCE: These results demonstrate the role of drug-induced autocrine events leading to the activation of alternative HER receptors in maintaining HER2 phosphorylation and in mediating resistance to EGFR tyrosine kinase inhibitors (TKIs) in breast cancer cells, and hence specify treatment opportunities to overcome resistance in patients.
机译:背景:在EGFR表达本身不足以作为治疗指标的癌症患者中,对EGFR酪氨酸激酶抑制剂(TKIs)的反应率可能较差且无法预测。对这种抵抗的机制了解有限。此外,尽管TKIs抑制了HER2过表达的乳腺癌细胞的生长,但在生理剂量下它们并未完全抑制HER2致癌功能。方法学和主要发现:在这里,我们提供了分子机制,说明由于自分泌配体的释放,HER2致癌功能如何通过替代性的HER受体激活而逃脱了TKIs的抑制作用。使用监测原位HER受体磷酸化的Förster共振能量转移(FRET)以及经典的生化分析,我们已经表明,EGFR,AG1478和易瑞沙(Gefitinib)的特定酪氨酸激酶抑制剂(TKIs)通过以下方式降低了EGFR和HER3的磷酸化EGFR / HER3二聚化的抑制作用。因此,我们证明了HER4的切割和HER4 / HER2的二聚化与通过HER2 / HER3的HER3的重新激活一起发生,从而导致了现在抵抗力强的存活细胞中持久的HER2磷酸化。发现这些药物治疗诱导的过程是通过配体的释放介导的,所述配体包括调蛋白和β纤维素通过HER2激活HER3和HER4。抗βcellulin抗体与易瑞沙的组合增加了抗性细胞的抗增殖作用,而配体(如调蛋白和β纤维素)使敏感的SKBR3细胞对易瑞沙具有抗性。结论和意义:这些结果表明药物诱导的自分泌事件导致替代性HER受体活化在维持HER2磷酸化和介导乳腺癌细胞中对EGFR酪氨酸激酶抑制剂(TKIs)的耐药性中的作用,并因此指明了治疗机会克服患者的抵抗力。

著录项

相似文献

  • 外文文献
  • 中文文献
  • 专利
代理获取

客服邮箱:kefu@zhangqiaokeyan.com

京公网安备:11010802029741号 ICP备案号:京ICP备15016152号-6 六维联合信息科技 (北京) 有限公司©版权所有

  • 客服微信

  • 服务号