Suneil A Raju, Katerina E Ingham, Olivia Green, Calvin M Johnson, Mohamed G Shiha, Nicoletta Nandi, Nick Trott, Hugo A Penny, Marios Hadjivassiliou, Graeme Wild, David S Sanders
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引用次数: 0
Abstract
Background and aims: In coeliac disease, the clinical role of the urinary gluten immunogenic peptide is unclear. It has been suggested it can be a non-invasive marker of villous atrophy. Therefore, we present the largest cross-sectional clinical data in patients with coeliac disease to establish the diagnostic accuracy of the urinary gluten immunogenic peptide in identifying villous atrophy.
Methods: Patients providing urinary gluten immunogenic peptide were identified between September 2018 and August 2023 at the National Health Service (NHS) England National Centre for Non-Responsive and Refractory CD. In our retrospective study, the results of the urinary gluten immunogenic peptide test collected within 7 days, self-reported adherence to a gluten free diet reported within 3 months, serology collected within 7 days (immunoglobulin A - tissue transglutaminase and endomysial antibody) and histology at the time of endoscopy were compared in individuals with coeliac disease who were either asymptomatic and undergoing remission biopsies (group 1), non-responsive coeliac disease (group 2) and refractory coeliac disease on immunosuppressive therapy (group 3). Associations between dichotomous variables were calculated using chi-squared test.
Results: In group 1 the sensitivity, specificity, positive predictive value (PPV) and negative predictive value (NPV) for detecting villous atrophy were 42.9%, 83.3.%, 64.3% and 67.6% respectively. In group 2 the sensitivity, specificity, PPV and NPV for detecting villous atrophy were 36.2%, 79.0%, 39.5% and 76.6% respectively. In group 3 the sensitivity, specificity, PPV and NPV for detecting villous atrophy were 56.3%, 70.6%, 73.0% and 53.3%. More patients on immunosuppression had a positive urinary gluten immunogenic peptide than those not on immunosuppression (43.3% vs 24.1%, p<0.001).
Conclusions: The urinary gluten immunogenic peptide does not have a role in identifying villous atrophy. Therefore, to assess for villous atrophy an upper gastrointestinal endoscopy is still required.
背景和目的:尿谷蛋白免疫原肽在乳糜泻中的临床作用尚不清楚。有人认为它可以作为绒毛萎缩的非侵入性标志。因此,我们在乳糜泻患者中提供了最大的横断面临床数据,以确定尿谷蛋白免疫原性肽在识别绒毛萎缩方面的诊断准确性。方法:在2018年9月至2023年8月期间,在英国国家无反应性和难治性乳糜泻国家中心确定了提供尿谷蛋白免疫原性肽的患者。在我们的回顾性研究中,在7天内收集尿谷蛋白免疫原性肽测试结果,在3个月内报告自我报告坚持无谷蛋白饮食,比较无症状且接受缓解性活组织检查的乳糜泻患者(1组)、无反应性乳糜泻患者(2组)和接受免疫抑制治疗的难治性乳糜泻患者(3组)7天内采集的血清学(免疫球蛋白A组织转谷氨酰胺酶和肌内膜抗体)和内镜检查时的组织学。使用卡方检验计算二分变量之间的相关性。结果:1组检测绒毛萎缩的敏感性、特异性、阳性预测值(PPV)和阴性预测值(NPV)分别为42.9%、83.3%;%, 64.3%, 67.6%。2组检测绒毛萎缩的敏感性为36.2%,特异性为79.0%,PPV和NPV分别为39.5%和76.6%。3组检测绒毛萎缩的灵敏度、特异度、PPV和NPV分别为56.3%、70.6%、73.0%和53.3%。免疫抑制组尿谷蛋白免疫原肽阳性的比例高于非免疫抑制组(43.3% vs 24.1%)。结论:尿谷蛋白免疫原肽对绒毛萎缩没有鉴别作用。因此,评估绒毛萎缩仍然需要上消化道内窥镜检查。
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