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血清胃蛋白酶原和幽门螺杆菌抗体联合内镜胃黏膜皱襞肥大性胃炎诊断非萎缩性胃炎伴高度活动炎症胃腺癌的发生。

Development of gastric cancer in nonatrophic stomach with highly active inflammation identified by serum levels of pepsinogen and Helicobacter pylori antibody together with endoscopic rugal hyperplastic gastritis.

机构信息

Second Department of Internal Medicine, School of Medicine, Wakayama Medical University, Wakayama City, Wakayama, Japan.

出版信息

Int J Cancer. 2012 Dec 1;131(11):2632-42. doi: 10.1002/ijc.27514. Epub 2012 Mar 28.

Abstract

This study aimed to elucidate groups at high risk of developing cancer among patients with serologically identified Helicobacter pylori infection and nonatrophic stomach. Annual endoscopy was performed for a mean of 5.4 years in 496 asymptomatic middle-aged men who were H. pylori antibody-positive and pepsinogen (PG) test-negative. Subjects were stratified according to the activity of H. pylori-associated gastritis measured by serum levels of PG and H. pylori antibody, and/or by endoscopic findings of rugal hyperplastic gastritis (RHG), and cancer development was investigated. During the study period, seven cases of cancer developed in the cohort (incidence rate, 261/100,000 person-years), with 85.7% developing in the group showing a PGI/II ratio ≤ 3.0, reflecting active inflammation-based high PGII levels. Cancer incidence was significantly higher in this group (750/100,000 person-years) than in groups with less active gastritis. Furthermore, cancer incidence for this group was significantly higher in the subgroup with high H. pylori antibody titers than in the low-titer subgroup. Meanwhile, endoscopic findings revealed that 11.7% of subjects showed RHG reflecting localized highly active inflammation, and cancer risk was significantly higher in patients with RHG than in patients without. Combining the two serum tests and endoscopic examination for RHG allowed identification of subjects with more active gastritis and higher cancer risk. No cancer development was observed in these high-risk subjects after H. pylori eradication. Subjects with highly active gastritis identified by the two serological tests and endoscopic RHG constitute a group at high risk of cancer development with H. pylori-infected nonatrophic stomach.

摘要

本研究旨在阐明血清学诊断为幽门螺杆菌感染和非萎缩性胃的患者中发生癌症的高危人群。496 名无症状中年男性 H. pylori 抗体阳性和胃蛋白酶原(PG)试验阴性,平均每年进行内镜检查 5.4 年。根据血清 PG 和 H. pylori 抗体水平以及内镜下皱襞增生性胃炎(RHG)的发现来衡量 H. pylori 相关性胃炎的活动程度,对受试者进行分层,并研究癌症的发展情况。在研究期间,该队列中有 7 例癌症发生(发生率为 261/100,000 人年),其中 85.7%发生在 PGI/II 比值≤3.0 的组,反映出炎症活跃且 PGII 水平较高。该组的癌症发病率明显高于其他组(750/100,000 人年)。此外,该组中高 H. pylori 抗体滴度的癌症发病率明显高于低滴度亚组。同时,内镜检查发现 11.7%的受试者存在 RHG,反映出局部高度活跃的炎症,RHG 患者的癌症风险明显高于无 RHG 患者。将两项血清学检测和内镜 RHG 检查相结合,可以识别出更活跃的胃炎和更高的癌症风险。在这些高危人群中,根除 H. pylori 后未观察到癌症的发展。通过两项血清学检测和内镜 RHG 发现的高度活跃性胃炎患者构成了具有 H. pylori 感染的非萎缩性胃的高危癌症发展人群。

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