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短发夹状RNA对GRP78基因在结直肠癌RKO细胞中表达的抑制作用 被引量:1

DEPRESSANT EFFECT OF SHORT HAIRPIN RNA ON GRP78 EXPRESSION OF RKO CELLS IN COLORECTAL CARCINOMA
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摘要 目的探讨短发夹状RNA对糖调节蛋白78(GRP78)在结直肠癌RKO细胞中表达抑制作用。方法以脂质体Lipofectamine2000介导GRP78短发卡状RNA(shRNA-GRP78)质粒表达载体转染RKO细胞,G418筛选得到稳定表达株,半定量RT-PCR和Westernblooting方法检测GRP78mRNA和蛋白水平变化。结果转染成功并筛选出稳定表达RKO细胞株。与对照组相比,shRNA-GRP78转染RKO细胞GRP78的mRNA及蛋白水平均显著下降(t=7.079、7.510,P<0.05)。结论 shRNA-GRP78能明显抑制RKO细胞GRP78mRNA及蛋白的表达,为进一步在体内外研究GRP78在结直肠癌中的作用奠定了基础。 Objective To explore the supression of glucose-regulated protein 78(GRP78)expression in human colorectal carcinoma cells RKO by short hairpin RNA(shRNA)interference.Methods The shRNA plasmid expression vector(shRNA-GRP78)was transfected into cells with Lipofectamine 2000.After selection with G418,the stable cell clones were attained.GRP78 expression was assayed with real-time quantitative PCR and Western blotting at both mRNA and protein levels.ResultsThe transfection was successful and stable RKO cell clones with shRNA-GRP78 plasmid were obtained.Compared with the control,the shRNA-GRP78 plasmid caused significant reduction of GRP78 expression at mRNA and protein levels(t=7.079,7.510;P〈0.01).Conclusion The shRNA-GRP78 plasmid can significantly inhibit the expressions of GRP78 mRNA and protein le-vels,which establishes a foundation for further study,in vivo and in vitro,of the role of GRP78 in colorectal carcinoma.
作者 王丽丽 邢晓明 李玉军
机构地区 青岛大学医学院附属医院病理科
出处 《青岛大学医学院学报》 CAS 2010年第5期387-389,共3页 Acta Academiae Medicinae Qingdao Universitatis
基金 山东省优秀中青年科学家奖励基金资助项目(2006BSB14001) 山东省自然科学基金资助项目(2009ZRA02112)
关键词 葡萄糖调节蛋白78 结直肠肿瘤 RNA干扰 glucose-regulated protein 78 colorectal neoplasms RNA interference
分类号 R735.3 [医药卫生—肿瘤]
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参考文献9

  • 1MUNRO S,PELHAM H R.An Hsp70-like protein in the ER:identity with the 78 kd glucose-regulated protein and immunoglobulin heavy chain binding protein[J].Cell,1986,46:291-300.
  • 2FU Y,WEY S,WANG M,et al.Pten null prostate tumorigenesis and AKT activation are blocked by targeted knockout of ER chaperone GRP78/Bip in prostate epithelium[J].Proc Natl Acad Sci USA,2008,105:19444-19449.
  • 3DONG D,NI M,LI J,et al.Critical role of the stress chaperone GRP78/Bip in tumor proliferation,survival and tumor angiogenesis in transgene induced mammary tumor development[J].Cancer Res,2008,68:498-505.
  • 4GAZIT B,LU J,LEE A S.De-regulation of GRP stress protein expression in human breast cancer cell lines[J].Breast Cancer Res Treat,1999,54:135-146.
  • 5MIYAKE H,HARA I,ARAKAWA S,et al.Stress protein GRP78 prevents apoptosis induced by calcium ionophore,io-nomycin,but not by glycosylation inhibitor,tunicamycin,in human prostate cancer cells[J].J Cell Biochem,2000,77:396-408.
  • 6GETHIN M J,SAMBROOK J.Protein folding in the cell[J].Nature,1992,355:33-45.
  • 7刘芳,邢晓明,李玉军,赵洁.结直肠腺癌组织Grp78表达及意义[J].青岛大学医学院学报,2009,45(3):252-254. 被引量:10
  • 8HUPPI K,MARTIN S E,CAPIEN N J.Defining and assaying RNAi in mammalian cells[J].Mol Cell,2005,17:1-10.
  • 9ELBASHIR S M,HARBORTH J,LENDERCKLE W,et al.Duplexes of 21-nucleotide RNAs mediate RNA interference in cultured mammalian cells[J].Nature,2001,411:494-498.

二级参考文献14

  • 1LEE A S.The glucose-regulated proteins:stress induction and clinical applications[J].Trends Biochem Sci,2001,26(8):504-510.
  • 2FU Y,LEE A S.Glucose regulated proteins in cancer progression,drug resistance and immunotherapy[J].Cancer Biol Ther,2006,5(7):741-744.
  • 3FERNANDEZ P M,TABBARA S O,JACOBS L K,et al.Overexpression of the glucose-regulated stress gene Grp78 in malignant but not benign human breast lesions[J].Breast Cancer Res Treat,2000,59(1):15-26.
  • 4URAMOTO H,SUGIO K,OYAMA T,et al.Expression of endoplasmic reticulum molecular chaperone Grp78 in human lung cancer and its clinical significance[J].Lung Cancer,2005,49(1):55-62.
  • 5SONG M S,PARK Y K,LEE J H,et al.Induction of glucose-regulated protein 78 by chronic hypoxia in human gastric tumor cells through a protein kinase C-epsilon/ ERK/AP-1 signaling cascade[J].Cancer Res,2001,61(22):8322-8330.
  • 6XING X,LAI M,WANG Y,et al.Overexpression of glucose-regulated protein 78 in colon cancer[J].Clin Chim Acta,2006,364(1-2):308-315.
  • 7RAO R V,CASTRO-OBREQON S,FRANKOWSKI H,et al.Coupling endoplasmic reticulum stress to the cell death program.An Apaf-1-independent intrinsic pathway[J].Biol Chem,2002,277(24):21836-21842.
  • 8YU Z,LOU H,FU W,et al.The endoplasmic reticulum stress-responsive protein Grp78 protects neurons against excitotoxicity apoptosis:suppression of oxidative stress and stabilization calcium homeostasis[J].Exp Neurol,1999,155(2):302-314.
  • 9RAUSCHERT N,BRANDLEIN S,HOLZINGER E,et al.A new tumor-specific variant of Grp78 as target for antibody-based therapy[J].Lab Invest,2008,88(4):375-386.
  • 10SVETLANA P,ERMAKOVA KANG B S,CHOI BY,et al.(-)-Epigallocatechin gallate overcomes resistance to etoposide-induced cell death by targeting the molecular chaperone glucose-regulated protein 78[J].Cancer Res,2006,66(18):9260-9269.

共引文献9

同被引文献11

  • 1HAAS I G. BiP (GRP78), an essential HSP70 resident protein in the endoplasmic reticulum [J]. Experientia, 1994,50 (11/ 12) : 1012-1020. in.
  • 2CHANG Y J, HUANG Y P, L1 Z L, et al. GRP78 knock- down enhances apoptosis via the down-regulation of oxidative stress and Akt pathway after epirubicin treatment in colon cancer DLD-1 cells[J]. Plos One, 2012,7(4):e35123.
  • 3LI J, LEE A S. Stress induction of GRP78/BiP and its role cancer [J]. Curr Mol Med, 2006,6(1)..45-54.
  • 4FU Y, LEE A S. Glucose regulated proteins in cancer progres- sion, drug resistance and immunotherapy [J]. Cancer Biol Ther, 2006,5(7) :741-744.
  • 5KOUMENIS C. ER stress, hypoxia tolerance and tumor pro- gression [J]. Curr Mol Med, 2006,6(1): 55-69.
  • 6JAMORA C, DENNETT G, LEE A S. Inhibition of tumor progression by suppression of stress protein GRP78/BiP induc- tion in fibrosarcoma B/C10ME [J]. Proe Natl Aead Sei U S A, 1996,93 (15) .. 7690-7694.
  • 7DONG D, DUBEAU L, BADING J, et al. Spontaneous and controllable activation of suicide gene expression driven by the stress-inducible GRP78 promoter resulting in eradication of sizable human tumors [J]. Hum Gene Ther, 2004,15(6) :553- 561.
  • 8MISRA U K, DEEDWANIA R, PIZZO S V. Activation and cross-talk between Akt, NF-kappaB, and unfolded protein re- sponse signaling in 1-LN prostate cancer cells consequent to ligation of cell surface-associated GRP78[J]. J Biol Chem, 2006,281(19) : 13694-13707.
  • 9SU R, LI Z, LI H, et al. GRP78 promotes the invasion of he- patocellular carcinoma [J]. BMC Cancer, 2010,10 : 20.
  • 10刘芳,邢晓明,李玉军,赵洁.结直肠腺癌组织Grp78表达及意义[J].青岛大学医学院学报,2009,45(3):252-254. 被引量:10

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青岛大学医学院学报
2010年 第5期

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