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IgA 抗组织转谷氨酰胺酶:为乳糜泻筛查奠定基础。

IgA anti-tissue transglutaminase: setting the stage for coeliac disease screening.

作者信息

Schuppan D, Hahn E G

机构信息

Medical Department I, University of Erlangen-Nuernberg, Erlangen, Germany.

出版信息

Eur J Gastroenterol Hepatol. 2001 Jun;13(6):635-7. doi: 10.1097/00042737-200106000-00004.

Abstract

Coeliac disease is triggered in genetically predisposed individuals by the ingestion of wheat and related cereals. Affected persons raise an intestinal mucosal T-cell response against the gluten fraction of these cereals. Furthermore, they produce characteristic circulating IgA antibodies to a self-antigen present in the extracellular matrix that can be detected on tissue sections. The positive predictive value of these endomysial, reticular or umbilical cord antibodies for coeliac disease comes close to 100%. Recently, the enzyme tissue transglutaminase was identified as the main, if not sole, endomysial autoantigen in coeliac disease. Enzyme-linked immunosorbent assay tests with tissue transglutaminase from guinea pig or the recombinant human enzyme have been established that allow a standardized and quantitative determination of IgA anti-tissue transglutaminase titres. While the published assay variants report high positive and negative predictive values for coeliac disease, they were applied to preselected patients from mostly single centres. Therefore, validation and in part cross-validation of a standardized assay based on guinea pig tissue transglutaminase in 38 European and non-European centres is timely. With a sensitivity of 90% and specificity of 96% relative to local diagnostic standards the assay performed well. Considering further improvement by the use of recombinant human tissue transglutaminase as the antigen and central re-evaluation of the local standards for confirmation of coeliac disease, this enzyme-linked immunosorbent assay promises to become the primary tool for non-invasive diagnosis, therapy control and screening of coeliac disease. However, with an estimated prevalence of 1:100-1:200 of mostly atypical and subclinical coeliacs in Western populations, we are confronted with the question of how far mass screening is ethically feasible and cost effective.

摘要

乳糜泻在具有遗传易感性的个体中由摄入小麦及相关谷物引发。患者会针对这些谷物的麸质部分产生肠道黏膜T细胞反应。此外,他们会产生针对细胞外基质中一种自身抗原的特征性循环IgA抗体,这种抗体可在组织切片上检测到。这些肌内膜、网状或脐带抗体对乳糜泻的阳性预测值接近100%。最近,酶组织转谷氨酰胺酶被确定为乳糜泻中主要的(即便不是唯一的)肌内膜自身抗原。已经建立了使用豚鼠组织转谷氨酰胺酶或重组人酶的酶联免疫吸附测定试验,可对IgA抗组织转谷氨酰胺酶滴度进行标准化和定量测定。虽然已发表的测定变体报告了对乳糜泻的高阳性和阴性预测值,但它们大多应用于来自单一中心的预先选择的患者。因此,在38个欧洲和非欧洲中心对基于豚鼠组织转谷氨酰胺酶的标准化测定进行验证以及部分交叉验证是适时的。相对于当地诊断标准,该测定的敏感性为90%,特异性为96%,表现良好。考虑到使用重组人组织转谷氨酰胺酶作为抗原进一步改进以及对乳糜泻确诊的当地标准进行集中重新评估,这种酶联免疫吸附测定有望成为乳糜泻非侵入性诊断、治疗监测和筛查的主要工具。然而,据估计,西方人群中大多数非典型和亚临床乳糜泻患者的患病率为1:100 - 1:200,我们面临着大规模筛查在伦理上可行及成本效益方面能走多远的问题。

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