首页> 外文期刊>Annals of Surgery >The effect of long-term control of reflux by fundoplication on aberrant deoxyribonucleic acid methylation in patients with Barrett esophagus.
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The effect of long-term control of reflux by fundoplication on aberrant deoxyribonucleic acid methylation in patients with Barrett esophagus.

机译:胃底折叠术长期控制反流对巴雷特食管患者异常脱氧核糖核酸甲基化的影响。

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OBJECTIVE: We investigated the relationship between reflux and aberrant deoxyribonucleic acid (DNA) methylation, comparing methylation in the columnar epithelium following successful fundoplication to that in subjects with a failed fundoplication. SUMMARY BACKGROUND DATA: Gastroesophageal reflux is the main risk factor for Barrett esophagus and adenocarcinoma. In these diseases, there is a high level of DNA methylation. METHODS: We enrolled 41 patients with Barrett esophagus and a fundoplication at least 5 years earlier for a 24-hour pH study, endoscopy, and collection of biopsies. Biopsies were obtained from 17 Barrett esophagus subjects who had not undergone esophageal surgery. RESULTS: At the time of the study, 31 subjects were pH normal, 10 abnormal. Columnar biopsies were collected from 21 of the pH normal and 9 pH abnormal subjects, and all no surgery subjects. Complete regression of columnar mucosa was seen in 7 subjects with pH normal and 1 with pH abnormal. The length of Barrett esophagus did not differ between groups preoperatively, but was significantly less at the time of the study in the pH normal compared with pH abnormal or no surgery groups. Significantly, fewer genes were methylated in the pH normal than the pH abnormal or no surgery groups, which did not differ from each other. The number of methylated genes correlated with increased reflux, intestinal metaplasia, and increased columnar-lined esophagus length, but not acid-suppression medication. CONCLUSIONS: Fundoplication that reduces reflux to normal levels can lead to regression of the columnar mucosa. Reflux is associated with aberrant DNA methylation, and control of reflux reduces deleterious genomic changes associated with cancer.
机译:目的:我们研究了反胃和反式脱氧核糖核酸(DNA)甲基化之间的关系,比较了成功胃底折叠术和失败胃底折叠术患者的柱状上皮中的甲基化。摘要背景资料:胃食管反流是巴雷特食管和腺癌的主要危险因素。在这些疾病中,DNA甲基化水平很高。方法:我们招募了至少5年前41例Barrett食管和胃底折叠术的患者,进行了24小时的pH研究,内窥镜检查和活检。活检取自17例未经食道手术的Barrett食管患者。结果:在研究时,有31名受试者的pH值正常,有10名异常。从21名pH正常的受试者和9名pH异常的受试者以及所有非手术受试者中收集柱状活检样品。 pH值正常的7名受试者和pH值异常的1名受试者可见柱状粘膜完全消退。术前两组间Barrett食管的长度没有差异,但在pH正常时与正常或非手术组相比,在研究时显着减少。值得注意的是,在pH正常条件下,甲基化的基因要少于pH异常或无手术组的基因,两者之间没有差异。甲基化基因的数量与反流增加,肠上皮化生和柱状内衬食管长度增加相关,但与抑酸药物无关。结论:胃底折叠术可将反流降低至正常水平,可导致柱状粘膜消退。反流与DNA甲基化异常有关,控制反流可减少与癌症相关的有害基因组变化。

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