Enrico Schirru, Rossano Rossino, Daniela Diana, Rita D Jores, Davide Baldera, Sandro Muntoni, Claudia Spiga, Carlo Ripoli, Maria R Ricciardi, Francesco Cucca, Mauro Congia
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Seventy-six of 822 patients with CD were also affected by T1D (CD-T1D), and their HLA genotypes were analyzed for specific HLA associations with CD, T1D, and controls.</p><p><strong>Results: </strong>High-risk HLA-DQ genotypes, including HLA-DQ2.5/DQ8, -DQ2.5/DQ2.5, and -DQ2.5/DQ2.3, were strongly associated with CD-T1D with frequencies of 34.5%, 15.9%, and 18.8%, respectively. Conversely, certain HLA genotypes associated with CD seemed to confer protection against T1D development. Therefore, HLA genotyping allows for the identification of those patients with CD who might develop T1D. The frequency of patients with CD preceding T1D is higher in younger children than older ones, with implications for the early childhood approach to diabetes prevention.</p><p><strong>Discussion: </strong>CD is a condition for future T1D development, and specific HLA genotypes can predict this risk. 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引用次数: 0
摘要
背景和目的:乳糜泻(CD)和1型糖尿病(T1D)经常同时发生,并且在HLA II类区有共同的遗传成分。我们的目的是研究 HLA 基因分型在预测 CD 患者罹患 T1D 风险方面的作用,以及这两种疾病之间的时间关系:对 1886 名撒丁岛患者进行了 HLA II 区分型,其中包括 822 名 CD 患者、1064 名 T1D 患者和 627 名对照组患者。在822名CD患者中,有76人同时患有T1D(CD-T1D),对他们的HLA基因型进行了分析,以确定HLA与CD、T1D和对照组的特定关联:高风险 HLA-DQ 基因型,包括 HLA-DQ2.5/DQ8、-DQ2.5/DQ2.5 和 -DQ2.5/DQ2.3,与 CD-T1D 密切相关,频率分别为 34.5%、15.9% 和 18.8%。相反,某些与 CD 相关的 HLA 基因型似乎可防止 T1D 的发生。因此,通过 HLA 基因分型可以识别那些可能发展成 T1D 的 CD 患者。在 T1D 之前患有 CD 的患者中,年龄较小的儿童要多于年龄较大的儿童,这对儿童早期糖尿病预防方法具有重要意义:结论:乳糜泻是未来罹患 T1D 的一个条件,特定的 HLA 基因型可以预测这种风险。对 CD 儿童进行乳糜泻自身免疫的早期筛查和随后的 HLA 分型有助于识别 T1D 的高风险人群,从而采取积极的干预措施和免疫疗法来保护β细胞功能。这些发现可能支持对 CD 儿童的 HLA 分型进行重新评估。
HLA Genotyping in Children With Celiac Disease Allows to Establish the Risk of Developing Type 1 Diabetes.
Introduction: Celiac disease (CD) and type 1 diabetes (T1D) often co-occur and share genetic components in the human leukocyte antigen (HLA) class II region. We aimed to study the usefulness of HLA genotyping in predicting the risk of developing T1D in patients with CD and the temporal relationship between these diseases.
Methods: A cohort of 1,886 Sardinian patients, including 822 with CD, 1,064 with T1D, and 627 controls, underwent HLA class II typing. Seventy-six of 822 patients with CD were also affected by T1D (CD-T1D), and their HLA genotypes were analyzed for specific HLA associations with CD, T1D, and controls.
Results: High-risk HLA-DQ genotypes, including HLA-DQ2.5/DQ8, -DQ2.5/DQ2.5, and -DQ2.5/DQ2.3, were strongly associated with CD-T1D with frequencies of 34.5%, 15.9%, and 18.8%, respectively. Conversely, certain HLA genotypes associated with CD seemed to confer protection against T1D development. Therefore, HLA genotyping allows for the identification of those patients with CD who might develop T1D. The frequency of patients with CD preceding T1D is higher in younger children than older ones, with implications for the early childhood approach to diabetes prevention.
Discussion: CD is a condition for future T1D development, and specific HLA genotypes can predict this risk. Early screening for celiac autoimmunity and subsequent HLA typing in CD children could help identify those at high risk of T1D, allowing for proactive interventions and immunotherapies to preserve β-cell function. These findings may support the re-evaluation of HLA typing in children with CD.
期刊介绍:
Clinical and Translational Gastroenterology (CTG), published on behalf of the American College of Gastroenterology (ACG), is a peer-reviewed open access online journal dedicated to innovative clinical work in the field of gastroenterology and hepatology. CTG hopes to fulfill an unmet need for clinicians and scientists by welcoming novel cohort studies, early-phase clinical trials, qualitative and quantitative epidemiologic research, hypothesis-generating research, studies of novel mechanisms and methodologies including public health interventions, and integration of approaches across organs and disciplines. CTG also welcomes hypothesis-generating small studies, methods papers, and translational research with clear applications to human physiology or disease.
Colon and small bowel
Endoscopy and novel diagnostics
Esophagus
Functional GI disorders
Immunology of the GI tract
Microbiology of the GI tract
Inflammatory bowel disease
Pancreas and biliary tract
Liver
Pathology
Pediatrics
Preventative medicine
Nutrition/obesity
Stomach.