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首页> 外文期刊>Modern Pathology >Allelic Loss and Tumor Pathology in Head and Neck Squamous Cell Carcinoma
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Allelic Loss and Tumor Pathology in Head and Neck Squamous Cell Carcinoma

机译:头颈部鳞状细胞癌的等位基因缺失和肿瘤病理学

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Allelic loss is a common occurrence in head and neck tumors and has been shown to be an independent predictor of prognosis; however, the relationship between allelic loss and tumor pathology is not well-known. We studied 139 patients who were newly diagnosed with squamous cell cancer of the head and neck to determine whether tumor pathology was correlated with allelic loss at one or more of eight different regions on chromosomes 3p, 5q, 8p, 9p, 10p, 18q, and 21q. At each chromosomal region, loss of heterozygosity at any one of three or four highly polymorphic microsatellite markers that spanned the region in question was considered evidence for allelic loss. A pathologist scored all tumors for seven tumor pathology and host interface parameters. Mean allelic loss across all eight regions was associated with mitotic index (P = .034) and inflammatory response (P = .005). For allelic loss at specific chromosomal regions, the most statistically significant trends were between overall tumor grade and 3p14.2-p13 (P = .014), mitotic index and 3p24.3-p14.3 (P = .026), 9p24.2-p21 (P = .004) and 18q12.3-q23 (P = .009), inflammatory response and 3p14.2-p13 (P = .008) and 9p24.2-p21 (P = .001), desmoplastic response and 9p24.2-p21 (P = .009), and pattern of invasion and 21q21-q22.2 (P = .015). Our results suggest that genes involved in tumor suppression and oncogenesis can potentially be classified based on specific pathologic events in head and neck squamous cell carcinogenesis that they modify.
机译:等位基因丢失是常见于头颈部肿瘤的疾病,已被证明是预后的独立预测因子。然而,等位基因缺失与肿瘤病理之间的关系尚不为人所知。我们研究了139例新诊断为头颈部鳞状细胞癌的患者,以确定肿瘤病理与3p,5q,8p,9p,10p,18q和8号染色体上八个不同区域中的一个或多个是否与等位基因丢失相关。 21q。在每个染色体区域,跨越所讨论区域的三个或四个高度多态性微卫星标记中任何一个的杂合性丧失均被视为等位基因缺失的证据。病理学家对所有肿瘤评分了七个肿瘤病理学和宿主界面参数。所有八个区域的平均等位基因缺失与有丝分裂指数(P = .034)和炎症反应(P = .005)相关。对于特定染色体区域的等位基因缺失,统计学上最显着的趋势是总体肿瘤分级与3p14.2-p13(P = .014),有丝分裂指数与3p24.3-p14.3(P = .026),9p24之间。 2-p21(P = .004)和18q12.3-q23(P = .009),炎症反应和3p14.2-p13(P = .008)和9p24.2-p21(P = .001),增生响应和9p24.2-p21(P = .009),入侵模式和21q21-q22.2(P = .015)。我们的结果表明,涉及肿瘤抑制和肿瘤发生的基因可能会根据其修饰的头颈部鳞状细胞癌发生中的特定病理事件进行分类。

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