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首页> 外文期刊>The journal of obstetrics and gynaecology research >Carcinogenic mechanisms of endometrial cancer: Involvement of genetics and epigenetics
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Carcinogenic mechanisms of endometrial cancer: Involvement of genetics and epigenetics

机译:子宫内膜癌的致癌机制:遗传学和表观遗传学的参与

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摘要

Endometrial cancer is increasing worldwide and the number of patients with this disease is likely to continue to grow, including younger patients. Many endometrial cancers show estrogen-dependent proliferation, but the carcinogenic mechanisms are unknown or not completely explained beyond mutations of single oncogenes and tumor suppressor genes. Possible carcinogenic mechanisms include imbalance between endometrial proliferation by unopposed estrogen and the mismatch repair (MMR) system; hypermethylation of the MMR gene hMLH1; mutation of PTEN, beta-catenin and K-ras genes in type I endometrial cancer and of HER-2eu and p53 genes in type II endometrial cancer; hypermethylation of SPRY2, RASSF1A, RSK4, CHFR and CDH1; and methylation of tumor suppressor microRNAs, including miR-124, miR-126, miR-137, miR-491, miR-129-2 and miR-152. Thus, it is likely that the carcinogenic mechanisms of endometrial cancer involve both genetic and epigenetic changes. Mutations and methylation of MMR genes induce various oncogenic changes that cause carcinogenesis, and both MMR mutation in germ cells and methylation patterns may be inherited over generations and cause familial tumorigenesis. Determination of the detailed carcinogenic mechanisms will be useful for prevention and diagnosis of endometrial cancer, risk assessment, and development of new treatment strategies targeting MMR genes.
机译:子宫内膜癌在世界范围内正在增加,患有这种疾病的患者人数可能会继续增长,包括年轻患者。许多子宫内膜癌表现出雌激素依赖性增殖,但是除了单个癌基因和抑癌基因的突变外,致癌机制尚不清楚或无法完全解释。可能的致癌机制包括雌激素抵抗子宫内膜增生与失配修复(MMR)系统之间的不平衡; MMR基因hMLH1的甲基化过高; I型子宫内膜癌的PTEN,β-catenin和K-ras基因突变,II型子宫内膜癌的HER-2 / neu和p53基因突变; SPRY2,RASSF1A,RSK4,CHFR和CDH1的超甲基化;抑癌微RNA,包括miR-124,miR-126,miR-137,miR-491,miR-129-2和miR-152的甲基化和甲基化。因此,子宫内膜癌的致癌机制可能涉及遗传和表观遗传学变化。 MMR基因的突变和甲基化会诱发各种致癌性变化,从而导致癌变,并且生殖细胞中的MMR突变和甲基化模式都可能世代相传并导致家族性肿瘤发生。确定详细的致癌机制将有助于子宫内膜癌的预防和诊断,风险评估以及针对MMR基因的新治疗策略的开发。

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