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SP-D Polymorphisms and the Risk of COPD

机译:SP-D多态性与COPD风险

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摘要

Introduction: There are limited data linking serum levels of surfactant protein D, its genetic polymorphisms to the risk of Chronic Obstructive Pulmonary Disease (COPD). Objectives: We sought to investigate these relationships using a case control study design. Methods: Post bronchodilator values of FEV1/FVC <0.7 were used to diagnose COPD patients (n = 115). Controls were healthy subjects with normal spirometry (n = 106) Single nucleotide polymorphisms (rs721917, rs2243639, rs3088308) were genotyped using polymerase chain reaction (PCR) and restriction analysis. Serum SP-D levels were measured using a specific immunoassay. Results: Allele ‘A’ at rs3088308 (p < 0.00, B = −0.41) and ‘C’ allele at rs721917 (p = 0.03; B = −0.30) were associated with reduced serum SP-D levels. Genotype ‘T/T’ at rs721917 was significantly associated with risk of COPD (p = 0.01). Patients with repeat exacerbations had significantly higher serum SP-D even after adjusting for genetic factors. Conclusions: We report for the first time that rs3088308 is an important factor influencing systemic SP-D levels and confirm the previous association of rs721917 to the risk of COPD and serum SP-D levels.
机译:简介:血清表面活性剂蛋白D的水平,其基因多态性与慢性阻塞性肺疾病(COPD)的风险相关的数据有限。目标:我们试图使用病例对照研究设计来调查这些关系。方法:将支气管扩张剂后FEV1 / FVC <0.7的值用于诊断COPD患者(n = 115)。对照是具有正常肺活量测定(n = 106)的健康受试者。使用聚合酶链反应(PCR)和限制性酶切分析对单核苷酸多态性(rs721917,rs2243639,rs3088308)进行基因分型。使用特异性免疫测定法测量血清SP-D水平。结果:rs3088308的等位基因“ A”(p <0.00,B = -0.41)和rs721917的等位基因“ C”(p = 0.03; B = -0.30)与血清SP-D水平降低相关。 rs721917基因型“ T / T”与COPD风险显着相关(p = 0.01)。即使经过遗传因素调整,反复发作的患者血清SP-D仍显着升高。结论:我们首次报道rs3088308是影响全身SP-D水平的重要因素,并证实了先前rs721917与COPD风险和血清SP-D水平的关联。

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