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绒毛萎缩的内镜标志物对于检测消化不良症状患者的乳糜泻并无用处。

Endoscopic markers of villous atrophy are not useful for the detection of celiac disease in patients with dyspeptic symptoms.

作者信息

Lecleire S, Di Fiore F, Antonietti M, Savoye G, Lemoine F, Le Pessot F, Lerebours E, Ducrotté P

机构信息

Department of Gastroenterology and Nutrition, ADEN-EA3234/IFRMP23 Research Group, Rouen University Hospital Charles-Nicolle, Rouen, France.

出版信息

Endoscopy. 2006 Jul;38(7):696-701. doi: 10.1055/s-2006-925373. Epub 2006 Jun 6.

Abstract

BACKGROUND AND STUDY AIMS

Celiac disease can manifest with nonspecific symptoms, including functional gastrointestinal disorders such as dyspepsia. The aim of our study was to assess the usefulness of duodenal endoscopic markers of villous atrophy for the selection of dyspeptic patients for histological assessment.

PATIENTS AND METHODS

Esophagogastroduodenoscopy was performed in dyspeptic patients, in patients considered to be at risk of having celiac disease, and in healthy controls. At least three duodenal biopsies were performed for histological assessment of villous atrophy in all patients and controls. We looked for the following four duodenal endoscopic markers of celiac disease: reduction in the number of folds, scalloping of folds, mosaic-pattern mucosa, and nodular mucosa.

RESULTS

A total of 175 people were enrolled (75 patients with dyspepsia; 75 patients who were "at risk" of having celiac disease; and 25 healthy volunteers, or "controls"). Of the dyspeptic patients, four had endoscopic markers of celiac disease with no histologically confirmed villous atrophy, while one patient without endoscopic markers was found to have Marsh type I villous atrophy. Of the patients at risk of having celiac disease, 16 had at least one endoscopic marker and 10/16 were found to have histological villous atrophy. In this group, the sensitivity and specificity of the endoscopic markers were 100 % and 90.8 % respectively. "At-risk" patients with two or more endoscopic markers all had histologically confirmed villous atrophy. Neither endoscopic markers nor villous atrophy were found in any of the control patients.

CONCLUSIONS

Additional endoscopic markers are valuable for diagnosis in patients with clinical symptoms suggestive of celiac disease. In contrast, endoscopic markers of villous atrophy are not useful for selecting a subgroup of dyspeptic patients for screening for celiac disease by duodenal histological assessment. These patients should be screened using other protocols.

摘要

背景与研究目的

乳糜泻可表现为非特异性症状,包括功能性胃肠疾病如消化不良。我们研究的目的是评估十二指肠内镜下绒毛萎缩标志物对于选择消化不良患者进行组织学评估的实用性。

患者与方法

对消化不良患者、被认为有乳糜泻风险的患者以及健康对照者进行食管胃十二指肠镜检查。对所有患者和对照者至少进行三次十二指肠活检以评估绒毛萎缩的组织学情况。我们寻找以下四种乳糜泻的十二指肠内镜标志物:皱襞数量减少、皱襞扇贝样改变、马赛克样黏膜和结节状黏膜。

结果

共纳入175人(75例消化不良患者;75例有乳糜泻“风险”的患者;25名健康志愿者,即“对照者”)。在消化不良患者中,4例有乳糜泻的内镜标志物但组织学未证实有绒毛萎缩,而1例无内镜标志物的患者被发现有马什I型绒毛萎缩。在有乳糜泻风险的患者中,16例有至少一种内镜标志物,其中10/16被发现有组织学绒毛萎缩。在该组中,内镜标志物的敏感性和特异性分别为100%和90.8%。有两种或更多内镜标志物的“有风险”患者均有组织学证实的绒毛萎缩。在任何对照患者中均未发现内镜标志物或绒毛萎缩。

结论

额外的内镜标志物对于有乳糜泻临床症状的患者诊断有价值。相比之下,绒毛萎缩的内镜标志物对于选择消化不良患者亚组进行十二指肠组织学评估以筛查乳糜泻并无用处。这些患者应采用其他方案进行筛查。

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