首页> 外文期刊>European journal of gastroenterology and hepatology >Non-endoscopic diagnosis of atrophic gastritis with a blood test. Correlation between gastric histology and serum levels of gastrin-17 and pepsinogen I: a multicentre study.
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Non-endoscopic diagnosis of atrophic gastritis with a blood test. Correlation between gastric histology and serum levels of gastrin-17 and pepsinogen I: a multicentre study.

机译:血液检查非内镜诊断萎缩性胃炎。胃组织学与血清胃泌素17和胃蛋白酶原I水平的相关性:一项多中心研究。

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BACKGROUND AND AIMS: Serum levels of gastrin-17 (S-G-17) and pepsinogen I (S-PGI) are biomarkers of gastric antral and corpus mucosa, respectively. In a prospective multicentre investigation, we determined whether these tests, together with the assay of Helicobacter pylori antibodies, are a non-endoscopic tool for the diagnosis of atrophic gastritis. MATERIALS AND METHODS: The series comprised 404 consecutive adult outpatients undergoing diagnostic upper-gastrointestinal endoscopy for various dyspeptic symptoms in five outpatient clinics. Gastric biopsies from the antrum and corpus (at least two biopsies from both sites) were available from all patients, and they were evaluated according to the guidelines of the updated Sydney system. S-PGI and S-G-17 were assayed with ELISA methods using monoclonal antibodies to pepsinogen I and amidated gastrin-17. In addition to the fasting level (S-G-17(fast)), a postprandial S-G-17 (S-G-17(prand)) level was measured 20 min after ingestion of a protein-rich drink. H. pylori antibodies were determined using a polyclonal EIA method. RESULTS: S-G-17(prand) (and S-G-17(fast)) and S-PGI levels decreased with increasing grade of atrophy of the antrum or corpus, respectively. S-G-17(prand) levels were significantly lower in patients with advanced (moderate or severe) atrophic antral H. pylori gastritis than in those with non-atrophic H. pylori gastritis. All patients with a resected antrum demonstrated S-G-17(prand) levels that were almost undetectable. Of the nine patients with an H. pylori-positive moderate or severe atrophic antral gastritis, six had S-G-17(prand) levels below 5 pmol/l. Similarly, S-PGI levels were significantly lower in patients with advanced corpus atrophy than in those without. Of the 45 patients with moderate or severe corpus atrophy in endoscopic biopsies, 35 patients had S-PGI levels < 25 microg/l. By using the cut-off levels for S-G-17(prand) and S-PGI with the best discrimination, the sensitivity and specificity of the blood test panel in delineation of patients with advanced atrophic gastritis (either in the antrum or the corpus, or both) were 83% and 95%, respectively. The predictive values of the positive and negative test results were 75% and 97%, respectively. In the diagnosis of atrophic gastritis, the application of S-G-17(fast) showed a slightly lower sensitivity and specificity than the application of S-G-17(prand) as a biomarker for antral atrophy. CONCLUSIONS: The diagnosis of atrophic gastritis obtained with the blood test panel of S-G-17, S-PGI and H. pylori antibodies is in good agreement with the endoscopic and biopsy findings. The panel is a tool for non-endoscopic diagnosis and screening of atrophic gastritis.
机译:背景与目的:胃泌素17(S-G-17)和胃蛋白酶原I(S-PGI)的血清水平分别是胃窦和胃粘膜的生物标志物。在一项前瞻性多中心调查中,我们确定了这些检测方法与幽门螺杆菌抗体检测方法是否一起用于诊断萎缩性胃炎。材料与方法:该系列包括404位连续的成人门诊病人,他们在5家门诊诊所接受了上消化道内镜诊断,发现有各种消化不良症状。所有患者均可获得胃窦和胃体的胃活检(两个部位至少有两个活检),并根据更新的悉尼系统的指南进行评估。使用针对胃蛋白酶原I和酰胺化胃泌素17的单克隆抗体,采用ELISA方法测定S-PGI和S-G-17。除了禁食水平(S-G-17(禁食)),在摄入富含蛋白质的饮料20分钟后还测量了餐后S-G-17(S-G-17(禁食))水平。使用多克隆EIA方法确定幽门螺杆菌抗体。结果:S-G-17(prand)(和S-G-17(fast))和S-PGI水平分别随着胃窦或体萎缩程度的增加而降低。晚期(中度或重度)萎缩性胃幽门螺杆菌胃炎患者的S-G-17(prand)水平显着低于非萎缩性幽门螺杆菌胃炎患者的S-G-17水平。所有胃腔切除的患者均表现出几乎无法检测到的S-G-17(prand)水平。在9例幽门螺杆菌阳性的中度或重度萎缩性胃窦炎患者中,有6例的S-G-17(prand)水平低于5 pmol / l。同样,晚期advanced体萎缩患者的S-PGI水平显着低于无without体萎缩的患者。在内窥镜活检中45例中度或重度体萎缩患者中,有35例S-PGI水平<25 microg / l。通过使用SG-17(品级)和S-PGI的临界值进行最佳区分,血液检测组对晚期萎缩性胃炎(胃窦或or体或两者)分别为83%和95%。阳性和阴性测试结果的预测值分别为75%和97%。在萎缩性胃炎的诊断中,应用S-G-17(快速)显示的敏感性和特异性略低于使用S-G-17(prand)作为肛门萎缩的生物标志物。结论:通过S-G-17,S-PGI和幽门螺杆菌抗体血液检测小组获得的萎缩性胃炎的诊断与内窥镜检查和活检结果相吻合。该面板是非内窥镜诊断和萎缩性胃炎筛查的工具。

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