中华肝脏病杂志
中華肝髒病雜誌
중화간장병잡지
CHINESE JOURNAL OF HEPATOLOGY
2010年
4期
271-275
,共5页
李龙嫚%曾小云%纪龙%范雪娇%李永强%胡晓桦%仇小强%余红平
李龍嫚%曾小雲%紀龍%範雪嬌%李永彊%鬍曉樺%仇小彊%餘紅平
리룡만%증소운%기룡%범설교%리영강%호효화%구소강%여홍평
癌,肝细胞%多态性,单核苷酸%XPC基因%XPG基因
癌,肝細胞%多態性,單覈苷痠%XPC基因%XPG基因
암,간세포%다태성,단핵감산%XPC기인%XPG기인
Carcinoma,hepatocellular%Polymorphism,single nucleotide%XPC%XPG
目的 探讨广西地区DNA修复基因XPC(Ala499Va1、Lys939G1n)和XPG(His1104Asp)单核苷酸多态性与肝细胞癌(HCC)易感性的关系.方法 采用以医院为基础的病例对照研究.经组织病理学确诊的HCC患者500例,相同地区,年龄、性别和民族频数匹配的非肿瘤患者507例.采用TaqMan MGB实时荧光定量PCR检测XPC和XPG基因多态性,比较不同基因型与HCC患病风险的关系.分别用t检验和X2检验对计量资料和计数资料进行统计分析;采用非条件的Logistic同归计算比值比(OR)及其95%可信区间(CI).结果 与XPC基因Ala499Va1位点CC基因型相比,CT或者TT基因型与HCC患病风险无相关性(校正OR=1.34,95%CI:0.85~2.12;校正OR=1.30,95%CI:0.68~2.51);与Lys939G1n位点AA基因理相比,AC或者CC基因型与HCC患病风险无相关性(校正OR=1.20,95%CI:0.78~1.85;校正OR=1.81,95%CI:0.88~3.73).与XPG基因His1104Asp位点CC基因型相比,CG或者GG基因型与HCC患病风险尢相关性(校正OR=0.85,95%CI:0.56~1.27;校正OR=1.12,95%CI:0.67~1.87).分层分析结果显示,与携带XPC基因Lys939G1n位点AA基因型女性相比,携带AC+CC基因型的女性患HCC的风险增加2.17倍(95%CI:01~4.64).结论 XPC基因Ala499Va1和Lys939G1n位点以及XPG基因His1104Asp位点SNP的单独效应可能与HCC易感性无相关性,但是XPC基因Lys939G1n位点C等位基因可协同增加女性患HCC的风险.
目的 探討廣西地區DNA脩複基因XPC(Ala499Va1、Lys939G1n)和XPG(His1104Asp)單覈苷痠多態性與肝細胞癌(HCC)易感性的關繫.方法 採用以醫院為基礎的病例對照研究.經組織病理學確診的HCC患者500例,相同地區,年齡、性彆和民族頻數匹配的非腫瘤患者507例.採用TaqMan MGB實時熒光定量PCR檢測XPC和XPG基因多態性,比較不同基因型與HCC患病風險的關繫.分彆用t檢驗和X2檢驗對計量資料和計數資料進行統計分析;採用非條件的Logistic同歸計算比值比(OR)及其95%可信區間(CI).結果 與XPC基因Ala499Va1位點CC基因型相比,CT或者TT基因型與HCC患病風險無相關性(校正OR=1.34,95%CI:0.85~2.12;校正OR=1.30,95%CI:0.68~2.51);與Lys939G1n位點AA基因理相比,AC或者CC基因型與HCC患病風險無相關性(校正OR=1.20,95%CI:0.78~1.85;校正OR=1.81,95%CI:0.88~3.73).與XPG基因His1104Asp位點CC基因型相比,CG或者GG基因型與HCC患病風險尢相關性(校正OR=0.85,95%CI:0.56~1.27;校正OR=1.12,95%CI:0.67~1.87).分層分析結果顯示,與攜帶XPC基因Lys939G1n位點AA基因型女性相比,攜帶AC+CC基因型的女性患HCC的風險增加2.17倍(95%CI:01~4.64).結論 XPC基因Ala499Va1和Lys939G1n位點以及XPG基因His1104Asp位點SNP的單獨效應可能與HCC易感性無相關性,但是XPC基因Lys939G1n位點C等位基因可協同增加女性患HCC的風險.
목적 탐토엄서지구DNA수복기인XPC(Ala499Va1、Lys939G1n)화XPG(His1104Asp)단핵감산다태성여간세포암(HCC)역감성적관계.방법 채용이의원위기출적병례대조연구.경조직병이학학진적HCC환자500례,상동지구,년령、성별화민족빈수필배적비종류환자507례.채용TaqMan MGB실시형광정량PCR검측XPC화XPG기인다태성,비교불동기인형여HCC환병풍험적관계.분별용t검험화X2검험대계량자료화계수자료진행통계분석;채용비조건적Logistic동귀계산비치비(OR)급기95%가신구간(CI).결과 여XPC기인Ala499Va1위점CC기인형상비,CT혹자TT기인형여HCC환병풍험무상관성(교정OR=1.34,95%CI:0.85~2.12;교정OR=1.30,95%CI:0.68~2.51);여Lys939G1n위점AA기인리상비,AC혹자CC기인형여HCC환병풍험무상관성(교정OR=1.20,95%CI:0.78~1.85;교정OR=1.81,95%CI:0.88~3.73).여XPG기인His1104Asp위점CC기인형상비,CG혹자GG기인형여HCC환병풍험왕상관성(교정OR=0.85,95%CI:0.56~1.27;교정OR=1.12,95%CI:0.67~1.87).분층분석결과현시,여휴대XPC기인Lys939G1n위점AA기인형녀성상비,휴대AC+CC기인형적녀성환HCC적풍험증가2.17배(95%CI:01~4.64).결론 XPC기인Ala499Va1화Lys939G1n위점이급XPG기인His1104Asp위점SNP적단독효응가능여HCC역감성무상관성,단시XPC기인Lys939G1n위점C등위기인가협동증가녀성환HCC적풍험.
Objective To investigate whether the polymorphism of DNA repair genes XPC(Ala499Va1 and Lys939G1n)and XPG(His1104Asp)is associated with the susceptibility to hepatocellular carcinoma (HCC).Methods A hospital-based case-control study was conducted in 500 cases with HCC and 507 controls.Genotypes of XPC and XPG were determined by real-time polymerase chain reaction with the TaqMan MGB probe.Results Compared to the CC genotype,the CT genotype and the Tr genotype of XPCAla499Va1 were not associated with the susceptibility to HCC(adjusted OR=1.34,95%CI:0.85-2.12;adjusted OR=1.30,95%CI:0.68-2.51,respectively).Compared to the AA genotype,the AC genotype and the CC genotype of Lys939G1n were not associated with the susceptibility to HCC(adjusted OR=1.20,95%CI:0.78-1.85;adjusted OR=1.81,95%CI:0.88-3.73,respectively).Compared to the CC genotype,the CG genotype and the GG genotype of XPG His1104Asp were not associated with the susceptibility to HCC(adjusted OR=0.85.95%CI:0.56-1.27;adjusted OR=1.12,95%CI:0.67-1.87,respectively)However,the stratified analysis revealed that the females with the AC+CC genotype of XPC Lys939G1n had increasod risk of HCC compared to those with AA genotype(OR=2.17,95%CI:1.01-4.64).Conclusion Ourr esults suggest that XPC and XPG polymorphisms do not independently affect on the susceptibility to HCC,but the joint effect of C allele of XPC Lys939G1n and female may modify the risk of HCC.
