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首页> 外文期刊>Virchows Archiv: an international journal of pathology >A combined histologic and molecular approach identifies three groups of gastric cancer with different prognosis.
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A combined histologic and molecular approach identifies three groups of gastric cancer with different prognosis.

机译:组织学和分子学相结合的方法确定了三组预后不同的胃癌。

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The limited prognostic value of currently used histologic classifications of gastric cancer and their failure to account for the complexity of the disease as revealed by more recent investigations prompted a combined reinvestigation of histologic, molecular, and clinicopathologic patterns in 294 extensively sampled, invasive gastric cancers representing all main histotypes and stages of the disease and followed for a median of 150 months. Among histologic parameters tested, only cellular atypia, angio-lympho- or neuroinvasion, Ki67 proliferation index, expansile/infiltrative type growth, and T8 cell-rich high lymphoid intra-/peritumor response (HLR) proved to be stage-independent predictors of patient survival. Among molecular tests, p53 gene exon 7 (loop 3) and 8 (loop-sheet-helix motif and S-10 band), but not p53 protein overexpression, TP53 LOH or 18qLOH, were found to worsen prognosis. Microsatellite DNA instability was a favorable prognostic factor when coupled with HLR. Patient survival analysis of the main histotypes and their subtypes confirmed the favorable prognosis of HLR, well-differentiated tubular, muconodular, and low grade diffuse desmoplastic cancers, and highlighted the worse prognosis of anaplastic and infiltrative-lymphoinvasive mucinous cancers compared to ordinary cohesive and diffuse cancers. Distinct roles of individual morphologic and molecular factors in tumor progression of the different histotypes have been recognized. The combination of survival-predictive histotypes and individual histologic or molecular parameters allowed us to develop a classification of all gastric cancers into three grades of increasing malignancy which proved to be of high prognostic value.
机译:最近的研究表明,当前使用的胃癌组织学分类法的预后价值有限,且未能解释疾病的复杂性,这促使对294例广泛采样的浸润性胃癌组织学,分子和临床病理类型进行了联合再调查疾病的所有主要组织类型和阶段,平均随访150个月。在所测试的组织学参数中,只有细胞异型性,血管淋巴或神经浸润,Ki67增殖指数,扩张/浸润型生长和富含T8细胞的高淋巴样内/周围反应(HLR)被证明是患者的阶段独立预测因子生存。在分子测试中,发现p53基因外显子7(环3)和8(环片螺旋基序和S-10条带),但p53蛋白过表达,TP53 LOH或18qLOH没有恶化。与HLR结合使用时,微卫星DNA不稳定性是一个有利的预后因素。对主要组织类型及其亚型的患者生存分析证实了HLR,高分化肾小管,黏膜小管和低度弥漫性增生性癌症的良好预后,并强调了变性和浸润性淋巴浸润性黏液性癌的预后较普通的粘着性和弥散性黏性癌差癌症。个体形态和分子因素在不同组织型肿瘤进展中的不同作用已得到公认。生存预测的组织学类型与个体的组织学或分子参数的结合使我们能够将所有胃癌的分类分为恶性程度增加的三个等级,这被证明具有较高的预后价值。

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