Period1、Period2对胶质瘤细胞的生物节律性调控作用

Regulatory effect of Period1 and Period2 on biological rhythm in glioma cells

导出

摘要目的研究大鼠胶质瘤细胞内生物钟基因Period1(Per1)、Per2mRNA及蛋白的周期表达规律。方法将体外培养的大鼠胶质瘤C6细胞接种于SD大鼠右侧尾状核区,在12h光照和12h黑暗的标准昼夜节律环境下,采用RT-PCR和免疫组织化学方法分别检测成瘤后4、8、12、16、20、24h肿瘤组织中Per1、Per2 mRNA和蛋白的表达。结果在大鼠胶质瘤组织中,Per1、Per2mRNA及蛋白产物呈节律性表达,其表达周期为12h的超日节律。Per1mRNA和蛋白的高表达时间点均位于4、16h,低表达时间点位于12、24h;Per2mRNA和蛋白的高表达时间点位于12、24h,低表达时间点位于8、20h。结论在SD大鼠体内,胶质瘤细胞的Per1、Per2基因呈12h的超日节律表达,提示生物钟基因的表达异常与胶质瘤的发生发展具有相关性。 Objective To investigate the periodical regularity of mRNA and protein expressions of bioclock gene Periodl （Perl） and Per2 in rat glioma cells. Methods The C6 glioma cells were cultured in vitro and inoculated into the right caudal nucleus of sixty SD rats. And then the rats were bred under the circumstance of a standardized 12 h light and 12 h dark cycle. At 4,8,12,16,20,24 h after tumor formation, the rnRNA and protein expressions of Per2 and Per2 were detected by RT-PCR and immunohistochemistry, respectively. Results The mRNA and protein expressions of Per1 and Per2 in glioma tissues showed a 12-h ultradian rhythm. The mRNA and protein expressions of Per1 peaked at 4 and 16 h,which were the lowest at 12 and 24 h. The mRNA and protein expressions of Per2 peaked at 12 and 24 h,which were the lowest at 8 and 20 h. Conclusion The expressions of Perl and Per2 in the glioma tissues of SD rats present a 12-h ultradian rhythm, which suggests that the development of glioma may he correlated with the abnormal expression of hioclock gene.

作者李延辉王凡尹磊李张珂牛占峰夏鹤春

机构地区宁夏医科大学荆门市第一人民医院神经外科宁夏医科大学总院神经外科

出处《江苏医药》 CAS CSCD 北大核心 2012年第18期2109-2112,共4页 Jiangsu Medical Journal

基金国家自然科学基金(30860289) 宁夏医科大学科研基金(XM201039)

关键词 Period1 Period2 胶质瘤生物节律性 Periodl Period2 Glioma Biological rhythm

分类号 R73 [医药卫生—肿瘤]

引文网络
相关文献

参考文献9

1You S, Wood PA, Xiong Y, et al. Daily coordination of cancer growth and circadian clock gene expression[J], Breast Cancer Res Treat, 2005,91 (1) : 47-60.
2王凡,牛占峰,曹栓柱,夏鹤春.胶质瘤大鼠模型的建立[J].山东医药,2010,50(30):27-28. 被引量：3
3Straif K, Baan R, Grosse Y, et al. Carcinogenicity of shift work, painting, and fire-fighting [J]. Lancet Oncol, 2007, 8 (12):1065- 1066.
4Xia HC, Niu ZF, Ma H, et al. Deregulated expression of the Per1 and Per2 in human gliomas[J]. Can J Neurol Sci, 2010, 37(3):365-370.
5Sephton S, Spiegel D. Circadian disruption in cancer: a neuroendocrine-immune pathway from stress to disease [J]? Brain Bchav Immun,2003,17(5):321- 328.
6Mormont MC, Levi F. Cancer chronotherapy: principles, applications,and perspectives[J]. Cancer, 2003, 97 ( 1 ) : 155- 169.
7Li XM,Delaunay F, Dulong S, et al. Cancer inhibition through circadian reprogramming of tumor transcriptome with meal timing[J]. Cancer Res,2010,70(8) :3351 -3360.
8郁玮玮,陈不尤.重组腺病毒p53基因诱导人脑胶质瘤细胞U251凋亡和放射增敏作用[J].江苏医药,2009,35(9):1061-1064. 被引量：1
9Fu L, Pelicano H, Liu J, et al. The circadian gene Period2 plays an important role in tumor suppression and DNA damage response in vivo[J]. Cell, 2002,111 ( 1 ) : 41-50.

二级参考文献21

1彭朝晖,张晓志.国外重组腺病毒-p53制品对肿瘤基因治疗临床研究的概况[J].中华医学杂志,2003,83(23):2098-2100. 被引量：37
2王煜,牛洪泉,董芳永,董震,柳再明,雷霆,薛德麟.大鼠树突状细胞疫苗治疗脑胶质瘤的实验研究[J].中国临床神经外科杂志,2005,10(2):115-117. 被引量：12
3张华蓉,陈飞兰,陈剑鸿,蒋雪峰,王清良,赵雯,卞修武.立体定向接种胶质瘤细胞系C6形成大鼠脑内原位移植瘤的生长特性[J].第三军医大学学报,2005,27(10):957-960. 被引量：9
4李明,冯华,李飞,王宪荣,吴南,陈志,吴国材,卢佳友,林江凯.大鼠C6脑胶质瘤模型的病理特征与MRI的观察[J].中华神经外科杂志,2005,21(5):279-282. 被引量：37
5Kaplan S, Etlin S, Novikov I,et al. Occupational risks for the development of brain tumors[J]. Am Jind Med, 1997,31(1) : 15.
6Reiser M, Neumann I, Schmiegel W, et al. Induction of cell proliferation arrest and apoptosis in hepatoma cells through adenoviral-mediated transfer of p53 gene[J]. J Hepatol, 2000,5(4): 771-782.
7Swither SC, Roth JA, Komaki R, et al. Induction of p53- regulated genes and tumor regression in lung cancer patients after intratumoral delivery of adenovirual p53 (INGN201) and radiation therapy[J]. Clin Cancer Res, 2003,9(1): 93-101.
8张均田.现代药理实验方法[M].第2版.北京医科大学中国协和医科大学联合出版社,1998:952-953.
9Janus F, Albrechtsn N, Dornreiter I, et al. The dual role model for p53 in maintaining genomic integrity [J]. Cell Mol Life Sci, 1999,55(4): 12-27.
10Smith ND, Rubenstein JN, Eggener SE,et al. The p53 tumor suppressor gene and nuclear protein: basic science review and relevance in the management of bladder cancer [J]. J Urol, 2003,169(4): 1219-1228.

共引文献2

1杨堃,李争争,郑传宜,覃西,白恩琪.大鼠脑内C6胶质瘤模型的建立[J].中国临床神经外科杂志,2012,17(3):165-167. 被引量：2
2宫崧峰,苏娟,颜杰,陈群芳,王晓彬,李新钢.聚乳酸乙醇酸阿霉素缓释棒对荷脑胶质瘤大鼠生存期及脑组织病理形态的影响[J].山东医药,2014,54(31):37-39.

1王兰芳,林娟,王小敏.胃癌组织中节律基因Period1和Period2的表达变化及意义[J].山东医药,2016,56(34):33-35. 被引量：2
2王华国.酶联免疫吸附法测定胃癌患者血清中Exosome、Dickkopf-1含量的临床价值[J].海南医学院学报,2017,23(2):205-208.
3韩晓燕,钟山,陈小希,张元珍,姚爱香,鄢学菊,周蕾.Per2基因可增强人宫颈癌对射线的敏感性[J].中国妇幼保健,2013,28(30):5038-5041.
4侯雯雯,李波,鲁成,刘俊.促凋亡基因Bax在胰腺癌中的研究进展[J].现代生物医学进展,2010,10(3):581-584. 被引量：7
5王成泉,王珺,尹磊,夏鹤春.裸鼠体内人U343胶质瘤中Period2对胶质瘤p53的调控作用及意义[J].宁夏医科大学学报,2015,37(6):620-625. 被引量：3
6李翠丽,王朝霞,李莉,李风艳.生物钟基因Period2对裸鼠卵巢癌移植瘤生长和血管生成抑制作用的机制研究[J].现代妇产科进展,2017,26(3):169-173. 被引量：3
7王朝霞,李莉,李风艳,张三元.生物钟基因Period2对卵巢癌裸鼠移植瘤生长抑制作用的机制研究[J].现代妇产科进展,2016,25(1):42-46. 被引量：4
8刘振,杨建青,潘光栋.Period 1基因功能与肿瘤抑制[J].中国普通外科杂志,2009,18(5):508-510. 被引量：2
9王健君,王琳.白细胞介素12在肝癌基因治疗中的应用[J].吉林大学学报（医学版）,2008,34(1):160-162. 被引量：1
10李晗雪,杨凯,付小娟,赵钦.生物钟基因Per1对人口腔鳞癌细胞生物学行为的影响和调控机制[J].中国医学科学院学报,2016,38(2):155-163. 被引量：6

江苏医药

2012年第18期

浏览历史

内容加载中请稍等...

Period1、Period2对胶质瘤细胞的生物节律性调控作用

参考文献9

二级参考文献21

共引文献2

相关作者

相关机构

相关主题

浏览历史