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Loss of FHIT expression in gastric mucosa of patients with family histories of gastric cancer and Helicobacter pylori infection

机译:胃癌家族史和幽门螺杆菌感染患者胃黏膜FHIT表达的丧失

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AIM: To answer the question whether FHIT gene expression is affected by the family history of gastric carcinoma and the presence of Helicobacter pylori (H pylori) in the gastric mucosa of patients with dyspepsia.METHODS: FHIT gene expression in two different topographic sites of the gastric mucosa of twenty-one patients with dyspepsia and with or without familial gastric carcinoma, infected or not infected with H pylori, was evaluated by reverse transcription-PCR (RT-PCR) and IMAGE QUANT methods. A rapid urease test and histopathological examination were used to determine H pylori colonization.RESULTS: In the gastric mucosa of patients with family histories of gastric carcinoma, the amount of FHIT protein mRNA was reduced down to 32%, and for patients with H pylori colonization, to 24% in comparison to controls with dyspepsia and without cancer in the family. FHIT expression was independent of the topography of specimens (corpus vs antrum), and for the control patients it was less sensitive to infection with H pylori. A considerable statistical difference in FHIT levels was observed in the gastric mucosa from the corpus of patients with family histories of gastric carcinoma in respect to H pylori colonization (P = 0.06). Macroscopic evaluation of the gastric mucosa demonstrated that pathologic changes classified according to the Sydney system had no significant influence on FHIT expression within each tested group of patients.CONCLUSION: Loss of FHIT expression was observed in patients with dyspepsia and family histories of gastric carcinoma, especially those infected with H pylori. Such results may constitute an early indication of the development of gastric carcinoma, which is associated with family factors including heredity and H pylori infection. The loss of the FHIT gene may serve as a marker for early diagnosis and prevention of gastric carcinoma, especially in context of early monitoring of H pylori infection in individuals with a record of familial stomach cancer.
机译:目的:回答消化不良患者胃粘膜家族史和幽门螺杆菌(H. pylori)是否影响FHIT基因表达的方法。方法:在两个不同的地形部位FHIT基因表达通过逆转录PCR(RT-PCR)和IMAGE QUANT方法评估了21例消化不良且有或没有家族性胃癌的消化不良患者,无论是否感染了幽门螺杆菌。结果:在有胃癌家族史的患者的胃黏膜中,FHIT蛋白mRNA的含量降低到32%,而在幽门螺杆菌的患者中,FHIT蛋白的mRNA减少了32%。 ,与有消化不良且无癌症的对照组相比,达到24%。 FHIT的表达与标本的形态无关(语料库与胃窦),对于对照患者,它对幽门螺杆菌感染的敏感性较低。在幽门螺杆菌定植方面,在有胃癌家族史的患者的胃黏膜中观察到FHIT水平有统计学差异(P = 0.06)。胃粘膜的肉眼观察表明,按悉尼系统分类的病理改变对每个患者组中的FHIT表达均无显着影响。结论:消化不良和胃癌家族史患者尤其是FHIT表达下降那些感染了幽门螺杆菌的人。这些结果可能构成了胃癌发展的早期迹象,这与家族因素包括遗传和 H pylori 感染有关。 FHIT 基因的缺失可能是早期诊断和预防胃癌的标志物,尤其是在早期监测 H pylori 感染且有记录的个体的情况下。家族性胃癌。

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