Decreased internalisation of erbB1 mutants in lung cancer is linked with a mechanism conferring sensitivity to gefitinib.

B S Hendriks, G J Griffiths, R Benson, D Kenyon, M Lazzara, J Swinton, S Beck, M Hickinson, J M Beusmans, D Lauffenburger, D de Graaf
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引用次数: 52

Abstract

A majority of gefitinib (IRESSA)-responsive tumours in non-small cell lung cancer have been found to carry mutations in ErbB1. Previously, it has been observed that internalisation-deficient ErbB1 receptors are strong drivers of oncogenesis. Using a computational model of ErbB1 trafficking and signalling, it is found that a deficiency in ErbB1 internalisation is sufficient to explain the observed signalling phenotype of these gefitinib-responsive ErbB1 mutants in lung cancer cell lines. Experimental tests confirm that gefitinib-sensitive cell lines with and without ErbB1 mutations exhibit markedly slower internalisation rates than gefitinib-insensitive cell lines. Moreover, the computational model demonstrates that reduced ErbB1 internalisation rates are mechanistically linked to upregulated AKT signalling. Experimentally it is confirmed that impaired internalisation of ErbB1 is associated with increased AKT activity, which can be blocked by gefitinib. On the basis of these experimental and computational results, it is surmised that gefitinib sensitivity is a marker of a reliance on AKT signalling for cell survival that may be brought about by impaired ErbB1 internalisation.

肺癌中erbB1突变体内化减少与赋予吉非替尼敏感性的机制有关。
非小细胞肺癌中大多数对吉非替尼(IRESSA)应答的肿瘤被发现携带ErbB1突变。以前,已经观察到内化缺陷ErbB1受体是肿瘤发生的强大驱动因素。利用ErbB1运输和信号传导的计算模型,研究人员发现,ErbB1内化缺陷足以解释肺癌细胞系中这些对吉非替尼反应的ErbB1突变体所观察到的信号表型。实验测试证实,有或没有ErbB1突变的吉非替尼敏感细胞系的内化率明显低于吉非替尼不敏感细胞系。此外,计算模型表明,ErbB1内在化率的降低与AKT信号的上调有机制联系。实验证实,ErbB1内化受损与AKT活性增加有关,而吉非替尼可阻断AKT活性。基于这些实验和计算结果,我们推测吉非替尼敏感性可能是ErbB1内化受损导致细胞存活依赖AKT信号的标志。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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