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斑秃中的HLA - D基因座关联。DRw52a可能赋予疾病抗性。

HLA-D locus associations in alopecia areata. DRw52a may confer disease resistance.

作者信息

Duvic M, Hordinsky M K, Fiedler V C, O'Brien W R, Young R, Reveille J D

机构信息

Department of Dermatology, University of Texas Medical School, Houston 77030.

出版信息

Arch Dermatol. 1991 Jan;127(1):64-8.

PMID:1670917
Abstract

Because predisposition to autoimmunity has been associated with HLA-D alleles and alopecia areata is hypothesized to be a T-cell mediated autoimmune hair loss, we determined DR and DQ alleles in 88 white and 10 American black patients with alopecia areata as well as controls with the use of restriction fragment length polymorphism typing with cDNA probes. White patients with alopecia areata have an increase in the phenotype frequencies of DR4 and DQw8 and an increase in genotype frequencies of DR4 and DR5 (now DRw11[5]). These associations are in agreement with those reported in two other studies but are not significant when corrected by the number of HLA antigens tested. Sixty-one percent of all patients with AA have DR4 and/or DRw11(5) specificities vs 40% of controls, with more DR4,DRw11(5) and DQw7(w3), DQw8(w3) heterozygotes among patients. DQw6(w1) phenotype frequencies and DRw52a phenotype and genotype frequencies are significantly decreased in patients with alopecia areata relative to controls. This highly significant negative association with the HLA DRB3 allele DRw52a in whites persisted even when DR4- or DRw11(5)-positive individuals were excluded from the patient and control groups. These data suggest that HLA-DR4 and DRw11(5) with their associated DQw7(w3) and DQw8(w3) specificities may confer susceptibility to alopecia areata, while DRw52a may confer resistance.

摘要

由于自身免疫易感性与HLA - D等位基因相关,且斑秃被认为是一种T细胞介导的自身免疫性脱发,我们使用cDNA探针通过限制性片段长度多态性分型法,对88名白人斑秃患者、10名美国黑人斑秃患者以及对照组进行了DR和DQ等位基因的检测。白人斑秃患者中DR4和DQw8的表型频率增加,DR4和DR5(现为DRw11[5])的基因型频率增加。这些关联与其他两项研究报告的结果一致,但经检测的HLA抗原数量校正后并不显著。所有斑秃患者中有61%具有DR4和/或DRw11(5)特异性,而对照组为40%,患者中DR4、DRw11(5)以及DQw7(w3)、DQw8(w3)杂合子更多。与对照组相比,斑秃患者的DQw6(w1)表型频率以及DRw52a表型和基因型频率显著降低。即使将DR4或DRw11(5)阳性个体从患者组和对照组中排除,白人中与HLA DRB3等位基因DRw52a的这种高度显著的负相关仍然存在。这些数据表明,具有相关DQw7(w3)和DQw8(w3)特异性的HLA - DR4和DRw11(5)可能使个体易患斑秃,而DRw52a可能具有抗性。

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