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首页> 外文期刊>American Journal of Cancer Research >Genomics and splicing events of type II endometrial cancers in the black population: racial disparity, socioeconomic and geographical differences
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Genomics and splicing events of type II endometrial cancers in the black population: racial disparity, socioeconomic and geographical differences

机译:黑人群中II型子宫内膜癌的基因组学和剪接事件:种族差异,社会经济和地理差异

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Endometrial cancer, also known as uterine cancer, is the most common gynaecological malignancy with burgeoning incidence and mortality rates globally. Racial disparity, socioeconomic and geographical differences are important determinants of endometrial cancer incidence and mortality. Endometrial cancer is mainly categorised as type I and type II. Although less prevalent, type II is the most aggressive form of the disease and typically diagnosed at a late stage, contributing to higher mortality. Black women are at higher risk of developing aggressive, type II disease. Type I tumours are related to higher levels of circulating estrogen with lower-grade tumours that have a good prognosis and frequently related to PTEN mutations. In comparison, type II tumours are estrogen-independent, typically have poor prognosis and associated with the p53, HER2, PPP2R1A, FBXW7 and PIK3R1 mutations. The risk of developing type II malignancy is higher in women with Lynch syndrome as a result of mutations in the MMR gene family. Genetic modifications contribute to aberrant alternative splicing events that are related to tumour development, progression and resistance to therapy. Alternative splicing events are rapidly emerging as potential biomarkers and therapeutic targets. Type II endometrial cancer lacks targeted therapy and biomarkers for novel therapeutic strategies. Recent advances have illustrated a number of molecular targets that are currently explored for the treatment of advanced, late-stage endometrial cancer. The aim of this review is to outline 1) the epidemiology of type II endometrial cancer in black women, 2) discuss the correlated risk factors that contribute to the development of type II endometrial cancer and 3) the associated molecular mechanisms and genetic factors underlying the disease, and 4) aberrant splicing events and biomarkers with therapeutic potential as novel drug targets.
机译:子宫内膜癌,也称为子宫癌,是最常见的妇科恶性肿瘤,并在全球蓬勃发展的发病率和死亡率。种族差异,社会经济和地理差异是子宫内膜癌症发病率和死亡率的重要决定因素。子宫内膜癌主要分为I型和II型。虽然较少普遍,II型是最具侵略性的疾病形式,通常在晚期诊断术,促进了更高的死亡率。黑人女性患有II型疾病的侵略性风险较高。 I型肿瘤与具有良好预后和PTEN突变的较低级肿瘤的循环雌激素的血液雌激素有关。相比之下,II型肿瘤是雌激素无关的,通常具有差的预后和与P53,HER2,PPP2R1A,FBXW7和PIK3R1突变相关。由于MMR基因家族中的突变,妇女患有II型恶性肿瘤的恶性肿瘤的风险较高。遗传修饰有助于异常替代的剪接事件,与肿瘤发育,进展和对治疗抗性有关。替代剪接事件迅速涌现为潜在的生物标志物和治疗目标。 II型子宫内膜癌缺乏针对新的治疗策略的靶向治疗和生物标志物。最近的进展已经说明了目前用于治疗先进的晚期子宫内膜癌的许多分子靶标。本综述的目的是概述1)黑人女性II型子宫内膜癌的流行病学,2)讨论有助于II型子宫内膜癌和3)相关的分子机制和遗传因素的相关危险因素疾病和4)异常剪接事件和具有治疗潜力作为新药靶标的生物标志物。

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