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家族性和散发性 1 型糖尿病患者共存自身免疫性疾病的风险与糖尿病发病年龄有关。

Risk for Coexistent Autoimmune Diseases in Familial and Sporadic Type 1 Diabetes is Related to Age at Diabetes Onset.

机构信息

Department of Clinical and Experimental Medicine, Endocrinology Section, University of Catania Medical School, Catania, Italy.

Department of Medicine, University of Perugia, Perugia, Italy.

出版信息

Endocr Pract. 2021 Feb;27(2):110-117. doi: 10.1016/j.eprac.2020.09.012. Epub 2020 Dec 13.

DOI:10.1016/j.eprac.2020.09.012
PMID:33616044
Abstract

OBJECTIVE

Type 1 diabetes (T1D) is frequently associated with other autoimmune diseases (AIDs). Although most of T1D patients are sporadic cases (S-T1D), 10% to 15% have a familial form (F-T1D) involving 2 or more first-degree relatives. This study evaluated the effect of T1D family aggregation and age onset on AIDs occurrence.

METHODS

In this observational, cross-sectional, case-control, single center study, we enrolled 115 F-T1D and 115 S-T1D patients matched for gender, age, T1D age onset, and duration. With respect to T1D age onset (before or after 18 years), both groups were further subdivided into young- or adult-onset F-T1D and young- or adult-onset S-T1D. The presence of organ-specific antibodies and/or overt AIDs was evaluated.

RESULTS

The F-T1D group had a higher percentage of AIDs (29.8% vs 18.4%, P = .04) and a significant earlier onset of AIDs at Cox regression analysis (P = .04) than the S-T1D group. Based on multivariate analysis, the adult-onset F-T1D subgroup had the highest prevalence of both additional organ-specific antibodies (60.5%) and overt AIDs (34.9%), whereas the adult S-T1D subgroup was the least frequently involved (29.1% and 12.7%, respectively). In F-T1D patients, offsprings develop T1D and AIDs earlier than their parents do.

CONCLUSIONS

In T1D patients, familial aggregation and adult-onset of T1D increase the risk for coexistent AIDs. These clinical predictors could guide clinicians to address T1D patients for the screening of T1D-related AIDs.

摘要

目的

1 型糖尿病(T1D)常与其他自身免疫性疾病(AIDs)相关。虽然大多数 T1D 患者为散发病例(S-T1D),但有 10%至 15%的患者存在涉及 2 个或更多一级亲属的家族性形式(F-T1D)。本研究评估了 T1D 家族聚集和发病年龄对 AIDs 发生的影响。

方法

在这项观察性、横断面、病例对照、单中心研究中,我们纳入了 115 例 F-T1D 和 115 例 S-T1D 患者,这些患者在性别、年龄、T1D 发病年龄和病程方面相匹配。根据 T1D 发病年龄(18 岁之前或之后),两组进一步分为年轻或成年发病的 F-T1D 和年轻或成年发病的 S-T1D。评估了器官特异性抗体和/或显性 AIDs 的存在。

结果

F-T1D 组的 AIDs 发生率(29.8%比 18.4%,P=0.04)和 Cox 回归分析中的 AIDs 发病年龄更早(P=0.04)均高于 S-T1D 组。基于多变量分析,成年发病的 F-T1D 亚组的两种额外器官特异性抗体(60.5%)和显性 AIDs(34.9%)的患病率最高,而成年 S-T1D 亚组的患病率最低(分别为 29.1%和 12.7%)。在 F-T1D 患者中,子女发生 T1D 和 AIDs 的年龄早于其父母。

结论

在 T1D 患者中,家族聚集和 T1D 的成年发病增加了共存 AIDs 的风险。这些临床预测因素可以指导临床医生对 T1D 患者进行 T1D 相关 AIDs 的筛查。

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