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HLA-DQB1*0201: a marker for good prognosis in British and Dutch patients with sarcoidosis.

作者信息

Sato Hiroe, Grutters Jan C, Pantelidis Panagiotis, Mizzon A Neil, Ahmad Tariq, Van Houte Arend-Jan, Lammers Jan-Willem J, Van Den Bosch Jules M M, Welsh Kenneth I, Du Bois Roland M

机构信息

Clinical Genomics Group, Department of Occupational and Environmental Medicine, Imperial College of Science, Technology and Medicine, National Heart and Lung Institute, London, United Kingdom.

出版信息

Am J Respir Cell Mol Biol. 2002 Oct;27(4):406-12. doi: 10.1165/rcmb.4782.

Abstract

Human leukocyte antigen (HLA)-DQB1 is one of the intriguing candidate genes in sarcoidosis. We performed high resolution molecular HLA-DQB1 typing on two groups of white patients (British [UK] and Dutch [NL]) in order to investigate the relationship between 19 DQB1 alleles and disease severity and progression. A total of 803 individuals were studied (133 UK and 102 NL patients, and 354 UK and 214 NL control subjects). Disease severity data included extrapulmonary disease, chest X-ray stage, lung diffusing capacity for carbon monoxide, and FVC. Progression was evaluated on follow-up chest radiographs (2 and 4 yr). The results showed DQB10201 to be strongly protective against severe sarcoidosis in both populations; in other words, it localized to Stage I at all time points (P < 0.0001, P(corrected) (P(c)) = 0.002), whereas another DQB1 allele, 0602, tended to have opposite effects. Further, a clear association was found between the 0201 allele and Löfgren's syndrome (P < 0.0001, P(c) = 0.001). More importantly, carriage of this allele reduced the risk of disease progression. In contrast, the other common split of DQB102, 0202, did not affect disease severity but was mildly protective against sarcoidosis in the UK population (P = 0.02, p(c) not significant). In conclusion, this study shows that DQB10201 is a strong marker for mild sarcoidosis. Additional mapping across the DQB10201-DRB10301 haplotype, including specific alleles at genes such as DRB3, tumor necrosis factor, lymphotoxin-alpha, I-kappa-B-like protein, and B-associated transcript 1, is necessary for a final localization of the protective effect on this haplotype.

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