新型 AIRE 序列变异与婴幼儿期干扰素-ω 抗体的检测
Novel sequence variation of AIRE and detection of interferon-omega antibodies in early infancy.
机构信息
Department of Infectious and Pediatric Immunology, University of Debrecen, Medical and Health Science Center, Debrecen, Hungary.
出版信息
Clin Endocrinol (Oxf). 2010 May;72(5):641-7. doi: 10.1111/j.1365-2265.2009.03740.x. Epub 2009 Oct 26.
OBJECTIVE
Autoimmune polyendocrine syndrome type I (APS I) is a rare primary immunodeficiency disorder characterized by chronic mucocutaneous candidiasis, multi-organ autoimmunity and ectodermal dysplasia. Autoantibodies to parathyroid and adrenal glands and type I interferons (IFN) are hallmarks of APS I, which results from mutations in the autoimmune regulator (AIRE) gene. We wished to study clinical, immunological and genetic features of APS I in Hungarian patients, and to correlate anti-IFN-omega serum concentration with APS I and other multi-organ autoimmune diseases.
DESIGN
Detailed analysis of patients with APS I and multi-organ autoimmune diseases.
PATIENTS
Seven patients with APS I and 11 patients with multi-organ autoimmune diseases were studied.
MEASUREMENTS
Mutational analysis was performed by bidirectional sequencing of AIRE. Antibodies against IFN-omega and endocrine organ-specific autoantigens were studied with radioimmunoassay. RFLP was performed by digestion of DNA with Hin6I restriction enzyme.
RESULTS
AIRE sequence analysis revealed homozygous c.769C>T mutations in three patients and compound heterozygous sequence variants (c.769C>T/c.44_66dup26bp; c.769C>T/c.965_977del13bp; c.769C>T/c.1344delC) in four patients with APS I. All the six live patients tested had markedly elevated IFN-omega antibodies, which were not found in heterozygous siblings or parents. One of the identified patients was negative for antibodies against IFN-omega at 6 weeks of age, but became positive at 7 months. At age 1, he is still without symptoms of the disease. In contrast to patients with APS I, no AIRE mutation or elevation of IFN-omega antibodies were detected in patients with multi-organ autoimmune diseases.
CONCLUSION
This is the first overview of patients diagnosed with APS I in Hungary. A novel c.1344delC mutation in AIRE was detected. Anti-IFN-omega antibodies seem to appear very early in life and are helpful to differentiate APS I from other multi-organ autoimmune diseases.
目的
自身免疫性多内分泌腺综合征 1 型(APS I)是一种罕见的原发性免疫缺陷病,其特征为慢性黏膜皮肤念珠菌病、多器官自身免疫和外胚层发育不良。甲状旁腺和肾上腺自身抗体以及 I 型干扰素(IFN)是 APS I 的标志,它是由自身免疫调节因子(AIRE)基因突变引起的。我们希望研究匈牙利患者 APS I 的临床、免疫和遗传特征,并将抗 IFN-ω 血清浓度与 APS I 和其他多器官自身免疫性疾病相关联。
设计
对 APS I 和多器官自身免疫性疾病患者进行详细分析。
患者
研究了 7 例 APS I 患者和 11 例多器官自身免疫性疾病患者。
测量
通过 AIRE 的双向测序进行突变分析。用放射免疫分析法研究针对 IFN-ω 和内分泌器官特异性自身抗原的抗体。通过 Hin6I 限制酶消化 DNA 进行 RFLP。
结果
AIRE 序列分析显示 3 例患者存在纯合 c.769C>T 突变,4 例患者存在复合杂合序列变异(c.769C>T/c.44_66dup26bp;c.769C>T/c.965_977del13bp;c.769C>T/c.1344delC)。所有 6 例存活患者的 IFN-ω 抗体明显升高,而杂合子兄弟姐妹或父母均未发现。其中一名确诊患者在 6 周龄时 IFN-ω 抗体检测为阴性,但在 7 个月时转为阳性。1 岁时,他仍然没有疾病症状。与 APS I 患者不同,多器官自身免疫性疾病患者未检测到 AIRE 突变或 IFN-ω 抗体升高。
结论
这是匈牙利首例诊断为 APS I 的患者概述。在 AIRE 中发现了一种新的 c.1344delC 突变。抗 IFN-ω 抗体似乎在生命早期就出现,有助于将 APS I 与其他多器官自身免疫性疾病区分开来。
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