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Is Fibroblast Growth Factor Receptor 4 a Suitable Target of Cancer Therapy?

机译:成纤维细胞生长因子受体4是否适合作为癌症治疗的靶标?

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摘要

Fibroblast growth factors (FGF) and their tyrosine kinase receptors (FGFR) support cell proliferation, survival and migration during embryonic development, organogenesis and tissue maintenance and their deregulation is frequently observed in cancer development and progression. Consequently, increasing efforts are focusing on the development of strategies to target FGF/FGFR signaling for cancer therapy.Among the FGFRs the family member FGFR4 is least well understood and differs from FGFRs1-3 in several aspects. Importantly, FGFR4 deletion does not lead to an embryonic lethal phenotype suggesting the possibility that its inhibition in cancer therapy might not cause grave adverse effects. In addition, the FGFR4 kinase domain differs sufficiently from those of FGFRs1-3 to permit development of highly specific inhibitors. The oncogenic impact of FGFR4, however, is not undisputed, as the FGFR4-mediated hormonal effects of several FGF ligands may also constitute a tissue-protective tumor suppressor activity especially in the liver.Therefore it is the purpose of this review to summarize all relevant aspects of FGFR4 physiology and pathophysiology and discuss the options of targeting this receptor for cancer therapy.
机译:成纤维细胞生长因子(FGF)及其酪氨酸激酶受体(FGFR)在胚胎发育,器官发生和组织维持过程中支持细胞增殖,存活和迁移,在癌症发生和发展中经常观察到它们的失调。因此,越来越多的努力集中在针对癌症治疗的靶向FGF / FGFR信号转导的策略的开发上。在FGFR中,家族成员FGFR4被最不了解,并且在几个方面与FGFRs1-3不同。重要的是,FGFR4缺失不会导致胚胎致死表型,提示其在癌症治疗中的抑制作用可能不会引起严重的不良反应。此外,FGFR4激酶结构域与FGFRs1-3的结构域有足够不同,可以开发出高度特异性的抑制剂。然而,FGFR4的致癌作用并非无可争议,因为FGFR4介导的几种FGF配体的激素作用也可能构成组织保护性肿瘤抑制活性,尤其是在肝脏中。因此,本综述的目的是总结所有相关内容FGFR4生理学和病理生理学的各个方面,并讨论了针对该受体靶向癌症治疗的选择。

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