klotho基因、Fgf21和Fgfr1在肿瘤发生中的作用

Wójcik-Krowiranda Katarzyna
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摘要

Klotho于1997年被发现是一种抗衰老基因,当它过表达时,可能会延长寿命,但当它被破坏时,它可能是导致早衰综合征的一个因素。本文介绍了Klotho家族的αKlotho和βKlotho基因在恶性肿瘤中的结构和作用。βKlotho基因的表达谱与αKlotho的表达谱显著不同。本文分析了Klotho在乳腺癌症、癌症和癌症子宫内膜癌中的表达。现有数据表明βKlotho参与子宫内膜的肿瘤转化。更晚期的疾病与βKlotho基因的负表达有关。成纤维细胞生长因子(FGFs)是一大类蛋白质,在细胞发育和代谢中具有不同的功能。FGF信号传导也与癌症发生有关。报道了某些FGF亚家族与子宫内膜癌症临床资料的关系。FGF亚家族和作为共受体的Klotho亚家族蛋白之间的相互作用受到强调。FGF/FGFR通路的信号传导障碍已在妇科得到证实。可以推测FGF21表达的增加可能是癌症的抑制因子。FGF21因子与βKlotho蛋白一样,通过FGFR1受体实现其生物学作用。FGFR1基因的高表达抑制了肿瘤的进一步生长。FGFR1具有在肿瘤发生过程中发挥抑制和启动子作用的潜力。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The Role of The ?klotho Gene, Fgf21 and Fgfr1 in Cancerogenesis
Klotho was discovered in 1997 as an anti-aging gene that, when overexpressed, may extend the life span, but when it is disrupted, it may be a factor responsible for premature aging syndrome. The structure and the role of αKlotho and βKlotho genes from Klotho family in malignant tumors is described. The expression profile of the βKlotho gene is significantly different from the expression of the αKlotho gene. Analysis of Klotho expression in breast cancer, cervical cancer as well as endometrial cancer are discussed. The available data indicate the involvement of βKlotho in the neoplastic transformation of the endometrium. More advanced disease is related to negative expression of βKlotho gene. Fibroblast growth factors (FGFs) are a large family of proteins characterized by different functions in the cell development and metabolism. The FGF signaling is also associated with cancerogenesis. The relation between some FGF subfamilies and endometrial cancer clinical data is reported. The interaction between FGF subfamilies and the Klotho subfamily proteins acting as a co-receptor is stressed. Disorders in signaling of the FGF / FGFR pathway have been confirmed in gynecology. It can be assumed that increased expression of FGF21 might be a suppressor factor in endometrial cancer. The FGF21 factor, like the βKlotho protein, achieves its biological effect via the FGFR1 receptor. High expression of the FGFR1 gene inhibits further tumor growth. FGFR1 has the potential to perform both a suppressor and promoter role in the oncogenesis process.
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