人类白细胞抗原II类抗原关联有助于定义两种斑秃类型。

HLA class II antigen associations help to define two types of alopecia areata.

作者信息

Colombe B W, Price V H, Khoury E L, Garovoy M R, Lou C D

机构信息

Department of Surgery, University of California, San Francisco, USA.

出版信息

J Am Acad Dermatol. 1995 Nov;33(5 Pt 1):757-64.

PMID:7593774

Abstract

BACKGROUND

Multiple HLA class I and class II antigen associations have been described for alopecia areata (AA). As in other immune-mediated diseases, the HLA antigens associated with AA could influence the patient's ability to respond to immune challenge from both self- and non-self-antigens and may offer clues to the cause and prognosis of and potential therapy for the disease.

OBJECTIVE

Our purpose was to determine which HLA class II antigens are associated with two forms of long-standing AA, which we define to be long-standing patchy AA and long-standing alopecia totalis (AT) and alopecia universalis (AU). We also examined other factors such as age at onset of disease and familial and patient histories of autoimmune disease for correlation with the two groupings.

METHODS

Patients were typed for HLA class I and class II antigens by serologic methods and were typed by molecular methods for the subtypes of the HLA class II antigens.

RESULTS

HLA-DR11 (DRB11104) and HLA-DQ7 (DQB10301) were found to be highly significantly increased in frequency in patients with long-standing AT/AU (group III) but not in patients with long-standing patchy AA (group II); both patient groups showed increased frequencies of HLA-DQ3 (DQB1*03). Group III patients were unique in their early age at onset of disease. Familial incidence of AA was 37% in patients who had their first patch by 30 years of age and 7.1% with the first patch after 30 years of age.

CONCLUSION

The data support the differential association of two well-defined clinical forms of AA, namely long-standing AT/AU and long-standing patchy AA, with specific HLA antigens and age at onset; they also suggest that the broad antigen HLA-DQ3, DQB1*03, is a likely candidate for general susceptibility to AA. Our findings also suggest a bimodal pattern of disease with an early-onset form associated with greater severity, long duration, and family history of the disease and a late-onset form characterized by milder severity, shorter duration, and low family incidence.

摘要

背景

斑秃（AA）已被描述与多种 HLA Ⅰ类和Ⅱ类抗原相关。与其他免疫介导的疾病一样，与 AA 相关的 HLA 抗原可能会影响患者对自身和非自身抗原免疫挑战的反应能力，并可能为该疾病的病因、预后及潜在治疗提供线索。

目的

我们的目的是确定哪些 HLA Ⅱ类抗原与两种长期存在的 AA 形式相关，我们将其定义为长期存在的斑秃和长期存在的全秃（AT）及普秃（AU）。我们还研究了其他因素，如发病年龄以及自身免疫性疾病的家族史和患者病史，以与这两组进行相关性分析。

方法

通过血清学方法对患者进行 HLA Ⅰ类和Ⅱ类抗原分型，并通过分子方法对 HLA Ⅱ类抗原的亚型进行分型。

结果

发现 HLA - DR11（DRB11104）和 HLA - DQ7（DQB10301）在长期存在的 AT/AU 患者（Ⅲ组）中的频率显著升高，但在长期存在的斑秃患者（Ⅱ组）中未升高；两组患者的 HLA - DQ3（DQB1*03）频率均有所增加。Ⅲ组患者在发病年龄上具有独特性。30 岁前首次出现斑秃的患者中 AA 的家族发病率为 37%，30 岁后首次出现斑秃的患者中家族发病率为 7.1%。

结论

数据支持两种明确的 AA 临床形式，即长期存在的 AT/AU 和长期存在的斑秃，与特定的 HLA 抗原和发病年龄存在差异关联；它们还表明广泛的抗原 HLA - DQ3，DQB1*03，可能是 AA 普遍易感性的一个候选因素。我们的研究结果还提示了一种双峰模式的疾病，早发型与更严重的病情、更长的病程和家族病史相关，晚发型则表现为病情较轻、病程较短和家族发病率较低。