中华肝胆外科杂志
中華肝膽外科雜誌
중화간담외과잡지
Chinese Journal of Hepatobiliary Surgery
2015年
8期
517-522
,共6页
吴志豪%许远%刘海斌%郑敏
吳誌豪%許遠%劉海斌%鄭敏
오지호%허원%류해빈%정민
肝癌%微小RNA-132%转移
肝癌%微小RNA-132%轉移
간암%미소RNA-132%전이
Liver cancer%micRNA-132%Metastasis
目的 观察微小RNA-132(miR-132)对体内外人肝癌细胞侵袭和转移的影响,初步探讨其作用机制.方法 实时荧光定量逆转录-聚合酶链反应(实时-qPCR)检测miR-132在4种肝癌细胞株(MHCC97H、HCCLYH、MHCC97L和SMMC-7721)、人正常肝细胞株HL-7702以及20例发生转移的肝癌组织和25例未发生转移肝癌组织中的表达.采用划痕实验、Transwell小室实验和经裸鼠尾静脉注射肝癌细胞形成的肝癌肺转移模型检验转染miR-132后对体内外肝癌MHCC97H细胞侵袭和转移的影响.蛋白印迹检测体外MHCC97H细胞中钙黏蛋白E(E-cadherin)、钙黏蛋白α(α-cadherin)、波形蛋白(vimentin)、纤连蛋白(fibronectin)和锌指E金结合同源盒蛋白2(zinc finger E-boxbinding bomeobox protein 2,ZEB2)蛋白的表达.免疫组织化学法检测肝癌肺转移灶组织中ZEB2的表达.结果miR-132在4种肝癌细胞株中的表达均明显低于人正常肝细胞(P<0.05),在伴转移肝癌组织中miR-132的表达明显低于未转移肝癌组织,差异有统计学意义(P<0.05).在体外实验,转染组细胞中miR-132的表达明显升高,细胞迁移和侵袭明显抑制,与对照组相比较,差异有统计学意义(P<0.05).转染组细胞中E-cadherin和α-cadherin蛋白表达上调,而vimentin、fibronectin和ZEB2蛋白的表达下调,与对照组相比较,差异均有统计学意义(P<0.05).在体内实验中,转染组裸鼠肺转移灶数目明显减少,ZEB2蛋白表达下调.结论 miR-132对体内外肝癌细胞侵袭和转移有明显抑制作用,有望成为肝癌治疗的新靶点.
目的 觀察微小RNA-132(miR-132)對體內外人肝癌細胞侵襲和轉移的影響,初步探討其作用機製.方法 實時熒光定量逆轉錄-聚閤酶鏈反應(實時-qPCR)檢測miR-132在4種肝癌細胞株(MHCC97H、HCCLYH、MHCC97L和SMMC-7721)、人正常肝細胞株HL-7702以及20例髮生轉移的肝癌組織和25例未髮生轉移肝癌組織中的錶達.採用劃痕實驗、Transwell小室實驗和經裸鼠尾靜脈註射肝癌細胞形成的肝癌肺轉移模型檢驗轉染miR-132後對體內外肝癌MHCC97H細胞侵襲和轉移的影響.蛋白印跡檢測體外MHCC97H細胞中鈣黏蛋白E(E-cadherin)、鈣黏蛋白α(α-cadherin)、波形蛋白(vimentin)、纖連蛋白(fibronectin)和鋅指E金結閤同源盒蛋白2(zinc finger E-boxbinding bomeobox protein 2,ZEB2)蛋白的錶達.免疫組織化學法檢測肝癌肺轉移竈組織中ZEB2的錶達.結果miR-132在4種肝癌細胞株中的錶達均明顯低于人正常肝細胞(P<0.05),在伴轉移肝癌組織中miR-132的錶達明顯低于未轉移肝癌組織,差異有統計學意義(P<0.05).在體外實驗,轉染組細胞中miR-132的錶達明顯升高,細胞遷移和侵襲明顯抑製,與對照組相比較,差異有統計學意義(P<0.05).轉染組細胞中E-cadherin和α-cadherin蛋白錶達上調,而vimentin、fibronectin和ZEB2蛋白的錶達下調,與對照組相比較,差異均有統計學意義(P<0.05).在體內實驗中,轉染組裸鼠肺轉移竈數目明顯減少,ZEB2蛋白錶達下調.結論 miR-132對體內外肝癌細胞侵襲和轉移有明顯抑製作用,有望成為肝癌治療的新靶點.
목적 관찰미소RNA-132(miR-132)대체내외인간암세포침습화전이적영향,초보탐토기작용궤제.방법 실시형광정량역전록-취합매련반응(실시-qPCR)검측miR-132재4충간암세포주(MHCC97H、HCCLYH、MHCC97L화SMMC-7721)、인정상간세포주HL-7702이급20례발생전이적간암조직화25례미발생전이간암조직중적표체.채용화흔실험、Transwell소실실험화경라서미정맥주사간암세포형성적간암폐전이모형검험전염miR-132후대체내외간암MHCC97H세포침습화전이적영향.단백인적검측체외MHCC97H세포중개점단백E(E-cadherin)、개점단백α(α-cadherin)、파형단백(vimentin)、섬련단백(fibronectin)화자지E금결합동원합단백2(zinc finger E-boxbinding bomeobox protein 2,ZEB2)단백적표체.면역조직화학법검측간암폐전이조조직중ZEB2적표체.결과miR-132재4충간암세포주중적표체균명현저우인정상간세포(P<0.05),재반전이간암조직중miR-132적표체명현저우미전이간암조직,차이유통계학의의(P<0.05).재체외실험,전염조세포중miR-132적표체명현승고,세포천이화침습명현억제,여대조조상비교,차이유통계학의의(P<0.05).전염조세포중E-cadherin화α-cadherin단백표체상조,이vimentin、fibronectin화ZEB2단백적표체하조,여대조조상비교,차이균유통계학의의(P<0.05).재체내실험중,전염조라서폐전이조수목명현감소,ZEB2단백표체하조.결론 miR-132대체내외간암세포침습화전이유명현억제작용,유망성위간암치료적신파점.
Objective To observe the biological role and the underlying mechanisms of miR-132 in liver cancer on invasion and metastasis.Methods Real-time quantitative polymerase chain reaction (RT-qPCR) analysis was used to examine the expression of miR-132 in four liver cancer cell lines (MHCC97H,HCCLYH,MHCC97L and SMMC-7721),a normal liver cell line HL-7702,and in liver tumor tissues with or without metastases.The biological effects of miR-132 transfection on human liver can-cer cells were assessed by wound assay,matrigel counting and in vivo experiments in nude mice.Western blotting was used to detect the expression of E-cadherin,α-cadherin,vimentin,fibronectin and ZEB2 in li-ver cancer cells.Immunohistochemistry was used to detect positive expression of ZEB2 in xenograft tumors.Results The expressions of miR-132 were downregulated in the four liver cancer cell lines when compared with the normal liver cell line (P < 0.05),and in the liver cancer tissues with distant metastases when compared with the tissues without metastases (P < 0.05).After transfection,ectopic expressions of miR-132 markedly inhibited cell migration and invasion in liver cancer cells.When compared with the control group,the expressions of E-cadherin and α-cadherin in the miR-132 transfection group were significantly increased,but the expressions of vimentin,fibronectin and ZEB2 were decreased.In addition,the numbers of metastatic lung lesions in nude mice in the miR-132 transfection group was markedly decreased when compared with the control group.The expressions of ZEB2 in the miR-132 transfection group was also significantly decreased when compared with the control group.Conclusions Transfection of miR-132 effectively inhibited invasion and metastasis of liver cancer cells in vitro and in vivo.miR-132 may become a new target for regulation of gene expression in liver cancer.