中华生物医学工程杂志
中華生物醫學工程雜誌
중화생물의학공정잡지
CHINESE JOURNAL OF BIOMEDICAL ENGINEERING
2014年
3期
185-190
,共6页
程璘令%刘雅雅%刘君%李晓燕%刘升明%李冰%冉丕鑫
程璘令%劉雅雅%劉君%李曉燕%劉升明%李冰%冉丕鑫
정린령%류아아%류군%리효연%류승명%리빙%염비흠
肺疾病,慢性阻塞性%疾病遗传易感性%DNA甲基化%谷氨酰半胱氨酸连接酶
肺疾病,慢性阻塞性%疾病遺傳易感性%DNA甲基化%穀氨酰半胱氨痠連接酶
폐질병,만성조새성%질병유전역감성%DNA갑기화%곡안선반광안산련접매
Pulmonary disease,chronic obstructive%Genetic predisposition to disease%DNA methylation%Glutamate-cysteine ligase
目的 探讨谷氨酰半胱氨酸连接酶催化亚单位(GCLC)基因多态性和甲基化与慢性阻塞性肺疾病(COPD)易感的相关性.方法 收集166例COPD患者为COPD组,同期与上述COPD患者相似的非COPD人群166例为对照组.使用基因测序法检测两组人群GCLC基因启动子区域的单核苷酸多态性(SNP),分析各SNP位点的单倍体型与COPD发病的关系.使用甲基化DNA免疫共沉淀芯片(MeDIP-chip)检测两组人群GCLC启动子区域甲基化水平,进行两组人群GCLC mRNA表达水平和血谷胱甘肽(GSH)浓度的比较.结果 通过直接测序法在GCLC启动子区域鉴定出12个SNP,其中4个SNP,即-2137MT、-129C/T、+27591C/G和+37764MG在COPD组和对照组人群中的发生率超过10%.-129C/T与-2137MT、+27591C/G、+37764MG均处于连锁不平衡.COPD组和对照组人群上述4个SNP的等位基因频率和基因型频率差异均无统计学意义(均P>0.05).MeDIP-chip检测显示COPD组GCLC启动子区域甲基化水平明显高于对照组(P<0.001).COPD组肺组织标本GCLC mRNA表达水平明显低于对照组(3.71±0.48比5.16±0.39,P<0.05),血谷胱甘肽(GSH)水平也低于对照组[109.72±32.38)mg/L比(179.87±46.23) mg/L,P<0.05].结论 中国人群GCLC启动子区域甲基化而非GCLC基因多态性与COPD相关.
目的 探討穀氨酰半胱氨痠連接酶催化亞單位(GCLC)基因多態性和甲基化與慢性阻塞性肺疾病(COPD)易感的相關性.方法 收集166例COPD患者為COPD組,同期與上述COPD患者相似的非COPD人群166例為對照組.使用基因測序法檢測兩組人群GCLC基因啟動子區域的單覈苷痠多態性(SNP),分析各SNP位點的單倍體型與COPD髮病的關繫.使用甲基化DNA免疫共沉澱芯片(MeDIP-chip)檢測兩組人群GCLC啟動子區域甲基化水平,進行兩組人群GCLC mRNA錶達水平和血穀胱甘肽(GSH)濃度的比較.結果 通過直接測序法在GCLC啟動子區域鑒定齣12箇SNP,其中4箇SNP,即-2137MT、-129C/T、+27591C/G和+37764MG在COPD組和對照組人群中的髮生率超過10%.-129C/T與-2137MT、+27591C/G、+37764MG均處于連鎖不平衡.COPD組和對照組人群上述4箇SNP的等位基因頻率和基因型頻率差異均無統計學意義(均P>0.05).MeDIP-chip檢測顯示COPD組GCLC啟動子區域甲基化水平明顯高于對照組(P<0.001).COPD組肺組織標本GCLC mRNA錶達水平明顯低于對照組(3.71±0.48比5.16±0.39,P<0.05),血穀胱甘肽(GSH)水平也低于對照組[109.72±32.38)mg/L比(179.87±46.23) mg/L,P<0.05].結論 中國人群GCLC啟動子區域甲基化而非GCLC基因多態性與COPD相關.
목적 탐토곡안선반광안산련접매최화아단위(GCLC)기인다태성화갑기화여만성조새성폐질병(COPD)역감적상관성.방법 수집166례COPD환자위COPD조,동기여상술COPD환자상사적비COPD인군166례위대조조.사용기인측서법검측량조인군GCLC기인계동자구역적단핵감산다태성(SNP),분석각SNP위점적단배체형여COPD발병적관계.사용갑기화DNA면역공침정심편(MeDIP-chip)검측량조인군GCLC계동자구역갑기화수평,진행량조인군GCLC mRNA표체수평화혈곡광감태(GSH)농도적비교.결과 통과직접측서법재GCLC계동자구역감정출12개SNP,기중4개SNP,즉-2137MT、-129C/T、+27591C/G화+37764MG재COPD조화대조조인군중적발생솔초과10%.-129C/T여-2137MT、+27591C/G、+37764MG균처우련쇄불평형.COPD조화대조조인군상술4개SNP적등위기인빈솔화기인형빈솔차이균무통계학의의(균P>0.05).MeDIP-chip검측현시COPD조GCLC계동자구역갑기화수평명현고우대조조(P<0.001).COPD조폐조직표본GCLC mRNA표체수평명현저우대조조(3.71±0.48비5.16±0.39,P<0.05),혈곡광감태(GSH)수평야저우대조조[109.72±32.38)mg/L비(179.87±46.23) mg/L,P<0.05].결론 중국인군GCLC계동자구역갑기화이비GCLC기인다태성여COPD상관.
Objective To investigate the association between susceptibility to chronic obstructive pulmonary disease (COPD) and the polymorphisms and methylation of glutamate-cysteine ligase catalytic subunit (GCLC) gene.Methods One hundred and sixty-six patients with COPD (COPD group) and 166subjects without COPD (control group) were recruited in this study.The single nucleotide polymorphisms (SNPs) of GCLC promoter region of two groups were investigated by DNA sequencing,which entailed the analysis on the association between haplotypes of individual SNP locus of GCLC gene and the risk of developing COPD.The level of GCLC promoter methylation was determined by using methylated DNA immunoprecipitation chip (MeDIPchip).The GCLC mRNA expressions and the levels of serum glutathione (GSH) were examined and compared between two groups.Results Twelve SNPs in GCLC gene promoter region were identified by direct DNA sequencing.Only 4 SNPs (-2137MT,-129C/T,+27591C/G,+37764MG) were found to harbor 10% incidence in both groups.The-129C/T was in linkage disequilibrium with-2137A/T,+27591C/G and + 37764A/G.However,no difference in GCLC SNP allele frequency or genotype frequency was observed between COPD patients and controls (all P>0.05).Compared with the control group,the methylation level of GCLC promoter was significantly increased in COPD patients (P<0.001),as evidenced by the MeDIP-chip assay,and the expression of GCLC mRNA was down-regulated in the lung tissues (3.71±0.48 vs 5.16±0.39,P<0.05) and serum GSH levels decreased [(109.72±32.38) mg/L vs (179.87±46.23) mg/L,P<0.05] in COPD patients.Conclusion Methylation,but not polymorphisms of GCLC promoter is associated with the susceptibility to COPD in Chinese population.