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Colorectal carcinogenesis: Insights into the cell death and signal transduction pathways: A review

机译:结直肠癌变:洞察细胞死亡和信号转导途径:综述

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摘要

Colorectal carcinogenesis (CRC) imposes a major health burden in developing countries. It is the third major cause of cancer deaths. Despite several treatment strategies, novel drugs are warranted to reduce the severity of this disease. Adenomatous polyps in the colon are the major culprits in CRC and found in 45% of cancers, especially in patients 60 years of age. Inflammatory polyps are currently gaining attention in CRC, and a growing body of evidence denotes the role of inflammation in CRC. Several experimental models are being employed to investigate CRC in animals, which include the APCmin/+ mouse model, Azoxymethane, Dimethyl hydrazine, and a combination of Dextran sodium sulphate and dimethyl hydrazine. During CRC progression, several signal transduction pathways are activated. Among the major signal transduction pathways are p53, Transforming growth factor beta, Wnt/β-catenin, Delta Notch, Hippo signalling, nuclear factor erythroid 2-related factor 2 and Kelch-like ECH-associated protein 1 pathways. These signalling pathways collaborate with cell death mechanisms, which include apoptosis, necroptosis and autophagy, to determine cell fate. Extensive research has been carried out in our laboratory to investigate these signal transduction and cell death mechanistic pathways in CRC. This review summarizes CRC pathogenesis and the related cell death and signal transduction pathways.
机译:结肠直肠癌变(CRC)在发展中国家构成了主要的健康负担。它是癌症死亡的第三大原因。尽管采取了几种治疗策略,但仍需使用新药来减轻这种疾病的严重程度。结肠腺瘤性息肉是CRC的主要元凶,在45%的癌症中特别是60岁的患者中发现。炎症性息肉目前在CRC中得到关注,越来越多的证据表明炎症在CRC中的作用。几种实验模型被用于研究动物的CRC,包括APC min / + 小鼠模型,Azoxymethane,二甲基肼以及右旋糖酐硫酸钠和二甲基肼的组合。在CRC进展过程中,一些信号转导途径被激活。在主要的信号转导途径中,有p53,转化生长因子β,Wnt /β-catenin,Delta Notch,Hippo信号传导,核因子类红细胞2相关因子2和Kelch样ECH相关蛋白1途径。这些信号通路与细胞死亡机制(包括凋亡,坏死病和自噬)协同作用,以确定细胞命运。在我们的实验室中进行了广泛的研究,以研究CRC中的这些信号转导和细胞死亡机制。这篇综述总结了CRC的发病机理以及相关的细胞死亡和信号转导途径。

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