Jürgen Laufs, Hjalti Andrason, Andres Sigvaldason, Eva Halapi, Leifur Thorsteinsson, Kristján Jónasson, Emilía Söebech, Thorarinn Gislason, Jeffrey R Gulcher, Kari Stefansson, Hakon Hakonarson
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引用次数: 40
Abstract
Background: Previous studies of vitamin D binding protein (VDBP, also known as group-specific component, Gc, encoded by the GC gene) have implicated two gene variants, GC*2 and GC*1F, as possible contributors with chronic obstructive pulmonary disease (COPD) protection and susceptibility, respectively. The objective of this study was to examine the association of VDBP to different subtypes of COPD.
Study design: The association of the various GC genotypes to the COPD phenotype was examined in Icelandic COPD patients who were followed by pulmonary physicians at the University Hospital of Iceland.
Methods: All patients were genotyped for the known alleles of the GC gene. The single nucleotide polymorphisms (SNPs) were identified by a restriction fragment length polymorphism procedure. Study power was estimated based on allele frequencies of the variants, and risk ratios were calculated from the prevalence of genotypes in the affected group divided by its prevalence in the control population. Statistical analyses were performed using the 2-tailed Fisher's Exact Test and chi(2) test, where appropriate.
Patient group: One hundred and two COPD patients and 183 controls, together with 46 asthma patients and 48 patients with chronic mucous hypersecretion (CMH) were examined.
Main outcome measure and results: The results demonstrate similar allele and genotype frequencies of GC in COPD patients overall and healthy controls. However, there was a higher prevalence of genotypes carrying a GC*1F allele and lower prevalence of genotypes with a GC*2 allele in the CMH patients than in controls. This difference was most notable in the homozygous form: 8.3% vs 1.1% for the GC*1F/*1F, and 0.0% vs 7.6% for the GC*2/*2 genotypes, respectively. When controlled for smoking, only the non-smoking CMH patients demonstrated a significantly altered frequency of the GC*1F/*1F genotype (p = 0.0001). The prevalence of the GC*2/*2 genotype was also significantly lower in patients with bronchial hypersecretion with airflow obstruction compared with the control group (2.9% vs 7.6%). Taken together, these results demonstrate that the GC*1F and GC*2 alleles are associated with sputum hypersecretion in individuals who are at increased risk of developing COPD.
背景:先前关于维生素D结合蛋白(VDBP,也称为群体特异性成分Gc,由Gc基因编码)的研究表明,Gc *2和Gc *1F两种基因变体可能分别与慢性阻塞性肺疾病(COPD)的保护和易感性有关。本研究的目的是检查VDBP与不同亚型COPD的关系。研究设计:在冰岛大学医院的肺病医生随访的冰岛COPD患者中,研究了各种GC基因型与COPD表型的关系。方法:对所有患者进行已知的GC基因等位基因分型。单核苷酸多态性(SNPs)通过限制性片段长度多态性程序进行鉴定。根据变异的等位基因频率估计研究能力,并根据受影响群体中基因型的患病率除以其在对照人群中的患病率计算风险比。统计分析采用双尾Fisher精确检验和chi(2)检验。患者组:慢性阻塞性肺病患者102例,对照组183例,哮喘患者46例,慢性粘液分泌过多(CMH)患者48例。主要结局测量和结果:结果显示,COPD患者和健康对照组中GC的等位基因和基因型频率相似。然而,与对照组相比,CMH患者中携带GC*1F等位基因的基因型患病率较高,携带GC*2等位基因的基因型患病率较低。这种差异在纯合子型中最为显著:GC*1F/*1F基因型为8.3% vs 1.1%, GC*2/*2基因型为0.0% vs 7.6%。当控制吸烟时,只有不吸烟的CMH患者显示GC*1F/*1F基因型频率显著改变(p = 0.0001)。支气管高分泌伴气流阻塞患者GC*2/*2基因型的患病率也显著低于对照组(2.9% vs 7.6%)。综上所述,这些结果表明GC*1F和GC*2等位基因与COPD发病风险增加的个体痰分泌过多有关。
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