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首页> 外文期刊>Cancer research: The official organ of the American Association for Cancer Research, Inc >Differential mechanisms of acquired resistance to insulin-like growth factor-i receptor antibody therapy or to a small-molecule inhibitor, BMS-754807, in a human rhabdomyosarcoma model.
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Differential mechanisms of acquired resistance to insulin-like growth factor-i receptor antibody therapy or to a small-molecule inhibitor, BMS-754807, in a human rhabdomyosarcoma model.

机译:在人横纹肌肉瘤模型中获得的对胰岛素样生长因子-i受体抗体治疗或小分子抑制剂BMS-754807的耐药性的差异机制。

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Agents targeting insulin-like growth factor-I receptor (IGF-IR), including antibodies and small-molecule inhibitors, are currently in clinical development for the treatment of cancers including sarcoma. However, development of resistance is a common phenomenon resulting in failures of anticancer therapies. In light of this problem, we developed two resistant models from the rhabdomyosarcoma cell line Rh41: Rh41-807R, with acquired resistance to BMS-754807, a small-molecule dual-kinase inhibitor targeting IGF-IR and insulin receptor (IR), and Rh41-MAB391R, with resistance to MAB391, an IGF-IR-blocking antibody. In addition, tumor xenograft models were established from Rh41 and Rh41-807R cell lines. Gene expression and DNA copy number analyses of these models revealed shared as well as unique acquired resistance mechanisms for the two types of IGF-IR inhibitors. Each resistant model used different signaling pathways as a mechanism for proliferation. Platelet-derived growth factor receptor alpha (PDGFRalpha) was amplified, overexpressed, and constitutively activated in Rh41-807R cells and tumors. Knockdown of PDGFRalpha by small interfering RNA in Rh41-807R resensitized the cells to BMS-754807. Synergistic activities were observed when BMS-754807 was combined with PDGFRalpha inhibitors in the Rh41-807R model in vitro. In contrast, AXL expression was highly elevated in Rh41-MAB391R but downregulated in Rh41-807R. Notably, BMS-754807 was active in Rh41-MAB391R cells and able to overcome resistance to MAB391, but MAB391 was not active in Rh41-807R cells, suggesting potentially broader clinical activity of BMS-754807. This is the first study to define and compare acquired resistance mechanisms for IGF-IR-targeted therapies. It provides insights into the differential acquired resistance mechanisms for IGF-IR/IR small-molecule inhibitor versus anti-IGF-IR antibody.
机译:目前,针对胰岛素样生长因子-I受体(IGF-IR)的药物,包括抗体和小分子抑制剂,正在临床开发中,用于治疗包括肉瘤在内的癌症。但是,耐药性的发展是导致抗癌治疗失败的普遍现象。针对这一问题,我们开发了横纹肌肉瘤细胞系Rh41的两种耐药模型:Rh41-807R,对BMS-754807,一种靶向IGF-IR和胰岛素受体(IR)的小分子双激酶抑制剂具有耐药性,并且Rh41-MAB391R,对IGF-IR阻断抗体MAB391具有抗性。另外,从Rh41和Rh41-807R细胞系建立了肿瘤异种移植模型。这些模型的基因表达和DNA拷贝数分析表明,两种类型的IGF-1R抑制剂具有共同的以及独特的获得性耐药机制。每个抗药性模型使用不同的信号传导途径作为增殖机制。在Rh41-807R细胞和肿瘤中,血小板衍生的生长因子受体α(PDGFRalpha)被扩增,过表达并被组成性激活。通过Rh41-807R中的小干扰RNA抑制PDGFRalpha,使细胞对BMS-754807再次敏感。当BMS-754807与PDGFRalpha抑制剂在Rh41-807R模型中体外组合时,观察到协同活性。相反,AXL表达在Rh41-MAB391R中高度升高,但在Rh41-807R中下调。值得注意的是,BMS-754807在Rh41-MAB391R细胞中具有活性,并且能够克服对MAB391的抗性,但MAB391在Rh41-807R细胞中不具有活性,表明BMS-754807的潜在临床活性更广泛。这是首次定义和比较针对IGF-IR靶向疗法的获得性耐药机制的研究。它提供了有关IGF-IR / IR小分子抑制剂与抗IGF-IR抗体的差异获得性耐药机制的见解。

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