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结节病的遗传学

Genetics of sarcoidosis.

作者信息

Iannuzzi Michael C

机构信息

Division of Pulmonary, Critical Care and Sleep Medicine, The Mount Sinai School of Medicine, New York, New York 10029, USA.

出版信息

Semin Respir Crit Care Med. 2007 Feb;28(1):15-21. doi: 10.1055/s-2007-970330.

Abstract

Sarcoidosis likely results from an interplay of environmental and genetic factors. Despite a recent large multicenter study, A Case-Control Etiologic Study of Sarcoidosis (ACCESS), no single causative environmental agent has been identified. Family clustering and differences in racial incidence of sarcoidosis support an inherited susceptibility to sarcoidosis. Siblings of patients with sarcoidosis have about a fivefold increased risk of developing sarcoidosis. Certain human leukocyte antigen (HLA) alleles have been consistently associated with sarcoidosis susceptibility. Furthermore, HLA-DRB10301/DQB10201 has been associated with good prognosis in Löfgren's syndrome. Many candidate genes studied based on their potential function in immunopathogenesis have been evaluated in case-control studies, but few have been consistently associated with sarcoidosis across populations. Two genome scans have been reported in sarcoidosis. One in African Americans reporting linkage to chromosome 5 and the other in German families reporting linkage to chromosome 6. Follow-up studies on chromosome 6 identified the BTNL2 gene, a B7 family costimulatory molecule to be associated with sarcoidosis. Advances in genotyping and statistical analysis are helping to elucidate the genetics of sarcoidosis.

摘要

结节病可能是环境因素和遗传因素相互作用的结果。尽管最近进行了一项大型多中心研究——结节病病例对照病因研究(ACCESS),但尚未确定单一的致病性环境因素。结节病的家族聚集现象以及种族发病率差异支持结节病存在遗传易感性。结节病患者的兄弟姐妹患结节病的风险大约增加五倍。某些人类白细胞抗原(HLA)等位基因一直与结节病易感性相关。此外,HLA-DRB10301/DQB10201与 Löfgren 综合征的良好预后相关。基于其在免疫发病机制中的潜在功能,许多候选基因已在病例对照研究中进行了评估,但很少有基因在不同人群中都与结节病持续相关。关于结节病已报道了两项全基因组扫描研究。一项是在非裔美国人中进行的,报告称与 5 号染色体存在连锁关系;另一项是在德国家庭中进行的,报告称与 6 号染色体存在连锁关系。对 6 号染色体的后续研究确定了 BTNL2 基因,一种 B7 家族共刺激分子,与结节病相关。基因分型和统计分析方面的进展有助于阐明结节病的遗传学机制。

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