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Combined p53/Bax mutation results in extremely poor prognosis in gastric carcinoma with low microsatellite instability.

机译:结合的p53 / Bax突变导致具有低微卫星不稳定性的胃癌预后极差。

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摘要

Gastric cancer is highly refractory to DNA-damaging therapies. We therefore studied both gene mutation and protein expression of p53 and Bax in a cohort of 116 patients with gastric cancer who underwent R0-resection with a curative intent. Bax mutation was independent from severe microsatellite instability (MSI), that is, global mismatch repair deficiency as determined by analysis of BAT-25/BAT-26 microsatellite markers. Thus, Bax-frameshift mutation is a feature of tumors with low MSI. In contrast and as expected, no p53 mutations were observed in the microsatellite instable tumors. p53 Mutation or p53 overexpression did not have an impact on disease prognosis. p53-Inactivation was, however, associated with an extremely poor prognosis in the subgroup of patients with Bax-mutated tumors. Thus, we show for the first time that the combined mutation of p53 and Bax, two key regulators of the mitochondrial apoptosis pathway, results in an extremely aggressive tumor biology and poor clinical prognosis.Cell Death and Differentiation (2003) 10, 461-467. doi:10.1038/sj.cdd.4401193
机译:胃癌对DNA损伤疗法非常难治。因此,我们在116例行根治性切除术的胃癌患者中研究了p53和Bax的基因突变和蛋白表达。 Bax突变独立于严重的微卫星不稳定性(MSI),即通过分析BAT-25 / BAT-26微卫星标记确定的总体失配修复缺陷。因此,Bax移码突变是MSI低的肿瘤的特征。相比之下,正如预期的那样,在微卫星不稳定肿瘤中未观察到p53突变。 p53突变或p53过表达对疾病的预后没有影响。然而,在Bax突变的肿瘤患者亚组中,p53失活与预后极差有关。因此,我们首次证明了线粒体凋亡途径的两个关键调节因子p53和Bax的联合突变,导致肿瘤生物学异常活跃,临床预后也很差。细胞死亡与分化(2003)10,461-467 。 doi:10.1038 / sj.cdd.4401193

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