您的位置:山东大学 -> 科技期刊社 -> 《山东大学学报(医学版)》

山东大学学报(医学版) ›› 2015, Vol. 53 ›› Issue (5): 55-59.doi: 10.6040/j.issn.1671-7554.0.2014.881

• 基础医学 • 上一篇    下一篇

miR-17对人包皮成纤维细胞衰老的影响

陈燕, 刘娟, 陈翰祥, 张魏芳, 赵蔚明   

  1. 山东大学医学院病原生物学系, 山东 济南 250012
  • 收稿日期:2014-11-27 修回日期:2015-01-20 出版日期:2015-05-10 发布日期:2015-05-10
  • 通讯作者: 赵蔚明。E-mail:zhaowm@sdu.edu.cn;张魏芳。E-mail:zhangweifang@sdu.edu.cn E-mail:zhaowm@sdu.edu.cn;zhangweifang@sdu.edu.cn
  • 基金资助:
    高等学校博士学科点专项科研基金(20110131120044);山东省优秀中青年科学家科研奖励基金(2011BSE27019)

Effects of miR-17 on the senescence of human foreskin fibroblasts

CHEN Yan, LIU Juan, CHEN Hanxiang, ZHANG Weifang, ZHAO Weiming   

  1. Department of Pathogenic Biology, School of Medicine, Shandong University, Jinan 250012, Shandong, China
  • Received:2014-11-27 Revised:2015-01-20 Online:2015-05-10 Published:2015-05-10

PDF (PC)

394

摘要: 目的 探讨miR-17对人包皮成纤维细胞(HFF)衰老的影响。方法 miR-17重组慢病毒感染细胞,qRT-PCR确定感染效率,CCK-8法观察miR-17对细胞增殖的影响,衰老相关 β-半乳糖苷酶染色观察miR-17对细胞衰老的影响,流式细胞法检测miR-17对细胞周期的影响,Western blotting检测cyclin D1和p21蛋白的表达。结果 成功分离得到HFF,并建立了稳定表达miR-17的 HFF-miR-17细胞系。且HFF-miR-17细胞增殖能力明显升高,β-半乳糖苷酶染色阳性率降低;S期细胞群比例明显增高,细胞周期蛋白cyclin D1表达显著上调,p21蛋白明显下调。结论 miR-17可通过上调cyclin D1蛋白、下调p21蛋白促进原代细胞的增殖,抑制原代细胞的衰老。

关键词: 人包皮成纤维细胞, miR-17, 衰老, 细胞周期

Abstract: Objective To study the effect of miR-17 on the senescence of human foreskin fibroblasts (HFF). Methods Recombinant lentivirus-expressed miR-17 infected HFF and miR-17 expression was examined with qRT-PCR. The proliferation and senescence of HFF were detected with CCK-8 and SA-β-Gal kit, respectively. Cell cycle profile was observed with flow cytometry. The protein levels of cyclin D1 and p21 were detected with Western blotting. Results HFF were successfully isolated. Compared with HFF-NC, the proliferation ability of HFF-miR-17 cells was obviously increased while the expression of SA-β-Gal in senescent cells decreased. S phase cells of HFF-miR-17 increased significantly and more HFF-NC cells arrested in the G1 phase. Expression of cyclin D1 was significantly up-regulated in HFF-miR-17, while p21 expression was attenuated. Conclusion miR-17 promotes the proliferation and inhibits senescence of primary cells by upregulating cyclin D1 and downregulating p21 proteins.

Key words: miR-17, Human foreskin fibroblasts, Cell cycle, Senescence

中图分类号: 

  • R392.2
[1] Kuilman T, Michaloglou C, Mooi WJ, et al. The essence of senescence[J]. Gene Dev, 2010, 24(22): 2463-2479.
[2] Bartel DP. MicroRNAs: genomics, biogenesis, mechanism, and, function[J]. Cell, 2004, 116(2): 281-297.
[3] Jasinski-Bergner S, Mandelboim O, Seliger B. The role of microRNAs in the control of innate immune response in cancer[J]. J Natl Cancer Inst, 2014, 106(10). pii: dju257. doi: 10.1093/jnci/dju257. Print 2014 Oct.
[4] Gama-Carvalho M, Andrade J, Brás-Rosário L. Regulation of cardiac cell fate by microRNAs: implications for Heart Regeneration[J]. Cells, 2014, 3(4): 996-1026.
[5] Ma Y, Yang HZ, Dong BJ, et al. Biphasic regulation of autophagy by miR-96 in prostate cancer cells under hypoxia[J]. Oncotarget, 2014, 5(19): 9169-9182.
[6] Guo J, Feng Z, Huang Z, et al. MicroRNA-217 functions as a tumour suppressor gene and correlates with cell resistance to cisplatin in lung cancer[J]. Mol Cells, 2014, 37(9): 664-671.
[7] Andorfer CA, Necela BM, Thompson EA, et al. MicroRNA signatures: clinical biomarkers for the diagnosis and treatment of breast cancer[J]. Trends Mol Med, 2011, 17(6): 313-319.
[8] Bonauer A, Dimmeler S. The microRNA-17-92 cluster still amiracle?[J]. Cell Cycle, 2009, 23(8): 3866-3873.
[9] Hackl M, Brunner S, Fortschegger K, et al. mirR-17, mirR-19b, mirR-20a, and mirR-106a are down-regulated in human aging[J]. Aging cell, 2010, 9(2): 291-296.
[10] Campisi J. Aging, cellular senescence, and cancer[J]. Annu Rev Physiol, 2013, 75: 685-705.
[11] Li G, Luna C, Qiu J, et al. Alterations in microRNA Expression in Stress-induced Cellular Senescence[J]. Mech Ageing Dev, 2009, 130(11-12): 731-741.
[12] Wang M, Cheng Z, Tian T, et al. Differential expression of oncogenicmiRNAs in proliferating and senescent human fibroblasts[J]. Mol Cell Biochem, 2011, 352 (1-2): 271-279.
[13] Klein EA, Assoian RK. Transcriptional regulation of the cyclin D1 gene at a glance[J]. J Cell Sci, 2008, 121(23): 3853-3857
[14] Harper JW, Adami GR, Wei N, et al. The p21 Cdk-interacting protein Cip1 is a potent inhibitor of G1 cyclin-dependent kinases[J]. Cell, 1993, 75(4): 805-816.
[15] 田兴松, 王新刚, 周文红, 等. 乳腺癌细胞中p16、p21、cyclin D1的表达及临床意义[J]. 山东大学学报: 医学版, 2005, 43(6): 532-543. TIAN Xingsong, WANG Xingang, ZHOU Wenhong, et al. Expressions of p16, p21, and cyclin D1 in breast cancer cells and their clinical significance[J]. Journal of Shandong University: Health Sciences, 2005, 43(6): 532-543.
[1] 王艺博,王颖超,徐琳琳,黄淑红,党宁宁. 烟草烟雾提取物通过Klotho-CHRNA5轴诱发皮肤衰老的机制[J]. 山东大学学报 (医学版), 2026, 64(1): 88-98.
[2] 余玉楠,王平,代君怡,刘军锋,昝俊峰. 茯苓三种活性成分对秀丽隐杆线虫的体内抗衰老作用[J]. 山东大学学报 (医学版), 2025, 63(6): 1-10.
[3] 刘萌,侯丛哲,麻焕玉,张震,赵新蕊,张萍,朱琳. β-雌二醇对宫颈癌Hela细胞增殖的影响[J]. 山东大学学报 (医学版), 2023, 61(2): 9-15.
[4] 刘腾,马迎春. 基于生物信息库病例分析ECT2在子宫内膜癌中的表达及临床意义[J]. 山东大学学报 (医学版), 2022, 60(8): 63-71.
[5] 罗湘杭,周若玙. 骨质疏松的病因及发病机制研究进展[J]. 山东大学学报 (医学版), 2021, 59(6): 10-14.
[6] 李文清,叶兰,姜玉华. CDK7抑制剂THZ1对人胶质瘤细胞U251放疗的增敏性[J]. 山东大学学报 (医学版), 2021, 59(1): 8-13.
[7] 崔锡铭,王霜,许顺江,张睿,谢冰,崔冬生,赵占胜. 白藜芦醇对高糖环境下人视网膜血管内皮细胞增殖的影响及分子机制[J]. 山东大学学报 (医学版), 2019, 57(3): 19-24.
[8] 王世宣,张金金. 卵巢衰老的机制与预防研究进展[J]. 山东大学学报 (医学版), 2019, 57(2): 16-22.
[9] 阎慧丽,魏慕筠,颜磊,赵跃然. FK506结合蛋白52对人子宫内膜间质细胞增殖作用的影响[J]. 山东大学学报 (医学版), 2019, 57(2): 80-87.
[10] 赵迪,冯秀娟,侯芳艳,吕高荣,徐晓芳,厉萍. 山东农村中年女性绝经综合征与生殖衰老分期、人格和正念的关系[J]. 山东大学学报 (医学版), 2019, 57(12): 92-96.
[11] 李晓梅,梁婷,张超,曹慧,侯桂华. 抑制T细胞CDK9对TLR5靶向监测同种异体移植排斥的影响[J]. 山东大学学报 (医学版), 2018, 56(7): 1-6.
[12] 兰静,李栋,时庆,刘子琳,周盼盼,鞠秀丽. 脐血NK细胞改善亚急性衰老大鼠肝脏损伤[J]. 山东大学学报 (医学版), 2018, 56(10): 64-71.
[13] 刘京康,杨建勇,孟丽华,姜洁. 血清miR-17-92簇在HPV阳性宫颈癌中的早期诊断价值[J]. 山东大学学报(医学版), 2017, 55(5): 86-90.
[14] 张雪群,高卫,潘盼,高骏逸. PI3K/AKT及其相关因子在结肠癌中的表达[J]. 山东大学学报(医学版), 2016, 54(1): 52-57.
[15] 刘辉, 陈桐帅, 李娜, 王舒健, 李静媛, 卜培莉. Sirt3对人脐静脉内皮细胞衰老的影响[J]. 山东大学学报(医学版), 2015, 53(5): 41-45.
Viewed
Full text


Abstract

Cited
  Shared   
  Discussed   
No Suggested Reading articles found!
版权所有 © 2018 《山东大学学报(医学版)》编辑部 
地址:山东大学科技期刊社(济南市历城区山大南路27号山东大学中心校区明德楼B座721室) 电话: 0531-88366918 E-mail: xbyxb@sdu.edu.cn
本系统由北京玛格泰克科技发展有限公司设计开发