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首页> 外文期刊>Canadian family physician: Medecin de famille canadien >Approach to diagnosing celiac disease in patients with low bone mineral density or fragility fractures:Multidisciplinary task force report [Approche au diagnostic de la maladie coeliaque chez les patients ayant une faible densité minérale osseuse ou des fractures de fragilité]
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Approach to diagnosing celiac disease in patients with low bone mineral density or fragility fractures:Multidisciplinary task force report [Approche au diagnostic de la maladie coeliaque chez les patients ayant une faible densité minérale osseuse ou des fractures de fragilité]

机译:低骨矿物质密度或脆性骨折患者的乳糜泻的诊断方法:多学科工作组报告[低骨矿物质密度或脆性骨折的患者乳糜泻的诊断方法]

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Objective To provide clinicians with an update on the diagnosis of celiac disease (CD) and to make recommendations on the indications to screen for CD in patients presenting with low bone mineral density (BMD) or fragility fractures. Quality of evidence A multidisciplinary task force developed clinically relevant questions related to the diagnosis of CD as the basis for a literature search of the MEDLINE, EMBASE, and CENTRAL databases (January 2000 to January 2009) using the key words celiac disease, osteoporosis, osteopenia, low bone mass, and fracture. The existing literature consists of level I and II studies. Main message The estimated prevalence of asymptomatic CD is 2% to 3% in individuals with low BMD. Routine screening for CD is not justified in patients with low BMD. However, targeted screening for CD is recommended for patients who have T-scores of -1.0 or less at the spine or hip, or a history of fragility fractures in association with any CD-related symptoms or conditions; family history of CD; or low urinary calcium levels, vitamin D insufficiency, and raised parathyroid hormone levels despite adequate intake of calcium and vitamin D. Celiac disease testing should be performed while the subject is consuming a gluten-containing diet; initial screening should be performed with human recombinant immunoglobulin (Ig) A tissue transglutaminase or other IgA tissue transglutaminase assays, in association with IgA endomysial antibody immunofluorescence. Duodenal biopsy is necessary to confirm the diagnosis of CD. Human leukocyte antigen typing might assist in confirming or ruling out the diagnosis of CD in cases where serology and histology are discordant. Definitive diagnosis is based on clinical, serologic, and histologic features, combined with a positive response to a gluten-free diet. Conclusion Current evidence does not support routine screening for CD in all patients with low BMD. A targeted case-finding approach is appropriate for patients who are at higher risk of CD.g.
机译:目的为临床医生提供乳糜泻(CD)诊断的最新信息,并为筛查患有低骨密度(BMD)或易碎性骨折的患者筛查CD的适应症提供建议。证据质量一支跨学科的工作组开发了与CD诊断有关的临床相关问题,以此为基础对MEDLINE,EMBASE和CENTRAL数据库(2000年1月至2009年1月)进行文献检索,关键词是乳糜泻,骨质疏松,骨质减少,骨量低和骨折。现有文献包括一级和二级研究。主要信息在低BMD人群中,无症状CD的估计患病率为2%至3%。 BMD低的患者不能常规筛查CD。但是,对于在脊柱或髋部的T分数小于或等于1.0的患者,或者与任何与CD相关的症状或状况相关的脆性骨折史的患者,建议进行CD的靶向筛查。 CD家族史;尽管钙和维生素D摄入量充足,但尿钙水平低,维生素D功能不足和甲状旁腺激素水平升高。应在受试者食用含麸质饮食的同时进行乳糜泻测试;初步筛选应使用人重组免疫球蛋白(Ig)组织转谷氨酰胺酶或其他IgA组织转谷氨酰胺酶试验,并结合IgA肌内膜抗体免疫荧光进行。十二指肠活检对于确定CD的诊断是必要的。在血清学和组织学不一致的情况下,人白细胞抗原分型可能有助于确认或排除CD的诊断。明确的诊断基于临床,血清学和组织学特征,以及对无麸质饮食的积极反应。结论目前的证据并不支持对所有低BMD患者进行CD常规筛查。有针对性的病例发现方法适用于CD风险较高的患者。

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