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儿童乳糜泻:走向更优的血清学大规模筛查策略。

Childhood coeliac disease: towards an improved serological mass screening strategy.

机构信息

Department of Paediatric Gastroenterology, Leiden University Medical Center, Leiden, The Netherlands.

出版信息

Aliment Pharmacol Ther. 2010 Apr;31(7):760-6. doi: 10.1111/j.1365-2036.2009.04226.x. Epub 2009 Dec 25.

DOI:10.1111/j.1365-2036.2009.04226.x
PMID:20047580
Abstract

BACKGROUND

In 1997-1998, 6127 asymptomatic children aged 2-4 years were screened for coeliac disease (CD) by anti-endomysium (EmA) testing in the Netherlands. After 6 (+/-2) months, biopsies were performed in 57 seropositive children; 31(54%) had villous atrophy, but 26 (46%), all HLA-DQ2/DQ8 positive, had normal histology.

AIMS

To reduce the number of unnecessary biopsies after serological mass screening for CD in asymptomatic young children by optimizing screening procedures.

METHODS

Comparing different tests and optimizing their cut-off point: screening samples were tested for EmA, tissue-transglutaminase (tTGA), antigliadin and deamidated-gliadin-peptides (anti-DGP) antibodies. Determining serological persistence over time: persistence of EmA and tTGA was determined by testing serological samples obtained at biopsy.

RESULTS

Tissue-transglutaminase and anti-DGP correlated with EmA. Optimization of standard cut-off points not only reduced unnecessary biopsies by 50-96% but also reduced sensitivity. EmA persisted in all CD children, but in only 50% of the non-CD children. tTGA persisted in 83% of CD, but in only 15% of non-CD children.

CONCLUSIONS

Coeliac disease antibodies may be present transiently in genetically predisposed children. To avoid unnecessary biopsies, serological mass screening procedures may be improved by repeating EmA and/or tTGA in initially seropositive young children after 6 months, before proceeding to biopsy. This may reduce the number of unnecessary biopsies that are performed.

摘要

背景

1997-1998 年,荷兰对 6127 名无症状 2-4 岁儿童进行了抗内膜(EmA)检测,以筛查乳糜泻(CD)。6(±2)个月后,对 57 名血清阳性儿童进行了活检;31 名(54%)有绒毛萎缩,但 26 名(46%)均为 HLA-DQ2/DQ8 阳性,组织学正常。

目的

通过优化筛查程序,减少无症状幼儿进行 CD 血清学大规模筛查后不必要的活检数量。

方法

比较不同的检测方法并优化其临界值:筛查样本检测 EmA、组织转谷氨酰胺酶(tTGA)、抗麦胶蛋白和脱酰胺麦胶蛋白肽(抗-DGP)抗体。确定血清学随时间的持续性:通过检测活检时获得的血清学样本来确定 EmA 和 tTGA 的持续性。

结果

tTGA 和抗-DGP 与 EmA 相关。标准临界值的优化不仅将不必要的活检减少了 50-96%,而且降低了敏感性。EmA 在所有 CD 患儿中持续存在,但在非 CD 患儿中仅持续存在 50%。tTGA 在 83%的 CD 患儿中持续存在,但在非 CD 患儿中仅持续存在 15%。

结论

在遗传易感儿童中,乳糜泻抗体可能短暂存在。为避免不必要的活检,可在最初血清阳性的幼儿 6 个月后重复进行 EmA 和/或 tTGA,然后再进行活检,以改进血清学大规模筛查程序。这可能会减少不必要的活检数量。

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