高级搜索

人脑胶质瘤中Smad-1、Smad-2和Smad-4的表达及意义

陈彩霞, 蔡 军, 魏晓霞, 邹 杰, 鲍玉洲, 步星耀

陈彩霞, 蔡 军, 魏晓霞, 邹 杰, 鲍玉洲, 步星耀. 人脑胶质瘤中Smad-1、Smad-2和Smad-4的表达及意义[J]. 肿瘤防治研究, 2014, 41(01): 22-26. DOI: 10.3971/j.issn.1000-8578.2014.01.006
引用本文: 陈彩霞, 蔡 军, 魏晓霞, 邹 杰, 鲍玉洲, 步星耀. 人脑胶质瘤中Smad-1、Smad-2和Smad-4的表达及意义[J]. 肿瘤防治研究, 2014, 41(01): 22-26. DOI: 10.3971/j.issn.1000-8578.2014.01.006
shu
CHEN Caixia, CAI Jun, WEI Xiaoxia, ZOU Jie, BAO Yuzhou, BU Xingyao. Expression and Signifi cance of Smad-1, Smad-2 and Smad-4 in Human Glioma[J]. Cancer Research on Prevention and Treatment, 2014, 41(01): 22-26. DOI: 10.3971/j.issn.1000-8578.2014.01.006
Citation: CHEN Caixia, CAI Jun, WEI Xiaoxia, ZOU Jie, BAO Yuzhou, BU Xingyao. Expression and Signifi cance of Smad-1, Smad-2 and Smad-4 in Human Glioma[J]. Cancer Research on Prevention and Treatment, 2014, 41(01): 22-26. DOI: 10.3971/j.issn.1000-8578.2014.01.006
shu

人脑胶质瘤中Smad-1、Smad-2和Smad-4的表达及意义

  • 1.450003郑州,河南省人民医院检验科,2.眼科研究所,3.神经外科三

基金项目: 河南省科技创新杰出人才计划项目资助课题(084200410011)
详细信息
    作者简介:

    陈彩霞(1973-),女,硕士,主管技师,主要从事医学检验与分子生物化学研究

    通讯作者:

    鲍玉洲,E-mail:baoyuzhou@126.com

    步星耀,E-mail:buxingyao@126.com

  • 中图分类号: R739.41

Expression and Signifi cance of Smad-1, Smad-2 and Smad-4 in Human Glioma

  • 1.Clinical Laboratory,He'nan Province People's Hospital, Zhengzhou 450003,China,2.Ophthalmological Research Institute,3.Three Department of Neurosurgery

摘要

    摘要
  • 摘要: 目的 检测BMPs/BMPR/Smads信号转导通路上的人脑胶质瘤组织中Smad-1、Smad-2、Smad-4的表达,探讨其在人脑胶质瘤发生发展中的作用及其与临床病理分级的关系。方法 分别应用RT-PCR技术和免疫组织化学SABC法检测20例正常脑组织和40例不同级别人脑胶质瘤组织中Smad-1、Smad-2、Smad-4 mRNA和蛋白质表达量,并分析其与患者的年龄、性别、病理分级的相关性。结果 人脑胶质瘤组织Smad-1、Smad-2、Smad-4 mRNA表达量比正常脑组织显著降低(0.277±0.125 vs. 0.573±0.097,P<0.01;0.282±0.111 vs. 0.613±0.105,P<0.01;0.389±0.101 vs. 0.483±0.098,P<0.05),且Ⅲ+Ⅳ组显著低于Ⅰ+Ⅱ组(0.250±0.106 vs. 0.327±0.119,P<0.05;0.2451±0.109 vs. 0.315±0.113,P<0.05;0.347±0.121 vs. 0.434±0.102,P<0.05)。蛋白质表达的阳性率显著低于正常脑组织(37.50% vs. 75.00%,P<0.0 1;20.00% vs. 65.00%,P<0.01; 25.00% vs. 70.00%,P<0.01),且Ⅲ+Ⅳ组显著低于Ⅰ+Ⅱ组(16.67% vs. 54.55%,P<0.05;5.56% vs. 31.82%, P<0.05;5.56% vs. 40.91%,P<0.05)。上述指标的变化与患者的年龄及性别无关。结论 Smad-1、Smad-2、Smad-4 在人脑胶质瘤中的表达水平与胶质瘤的发生发展和恶性程度密切相关,提示Smad-1、Smad-2、Smad-4 可能参与胶质瘤发生发展过程。

     

    Abstract: Objective To detect the expressions of Smad-1,Smad-2 and Smad-4 of BMPs/BMPR/Smads signaling transduction pathway in human brain glioma, to research their role of them in tumorigenesis and progression of brain glioma and their correlation with clinical pathology. Methods The mRNA and protein expressions of Smad-1,Smad-2 and Smad-4 were detected in 20 normal brain tissues and 40 samples with human glioma by RT-PCR and SABC immunohistochemical methods, respectively, and analyzed the correlation with the patient's age, gender and pathological grade. Results Compared with normal brain tissues, Smad-1,Smad-2 and Smad-4 mRNA expressions in human glioma were reduced signifi cantly(0.277 ±0.125 vs. 0.573±0.097, P<0.01;0.282±0.111 vs. 0.613±0.105, P<0.01;0.389±0.101 vs. 0.483± 0.098,P<0.05 )especially in Ⅲ and Ⅳ stage tumor tissues(0.250±0.106 vs. 0.327±0.119,P<0.05;0.2451±0.109 vs. 0.315±0.113,P<0.05;0.347±0.121 vs. 0.434±0.102,P<0.05),and protein expressions in human glioma were reduced significantly(37.50% vs. 75.00% , P<0.0 1;20.00% vs. 65.00%,P<0.01;25.00% vs. 70.00%,P<0.01)especially in Ⅲ and Ⅳ stage tumor tissues(16.67% vs. 54.55%,P<0.05;5.56% vs. 31.82%,P<0.05;5.56% vs. 40.91%,P<0.05). The difference was not related with the patient's age and gender. Conclusion Expressions of Smad-1,Smad-2 and Smad-4 in human glioma are closely related with glioma malignant degree. It prompts Smad-1, Smad-2 and Smad-4 participate in brain glioma occurrence and development process.

     

    • HTML全文
    • 参考文献(16)
  • [1] Yang T,Zhang X,Zhou L,et al.Expression and Signifi cance of p57kip2 and p21cip1 in Human Glioma[J].Xi’an Jiao Tong Da Xue Xue Bao(Yi Xue Ban),2008, 29(5): 562-5.[杨涛,张熙,周 乐,等. p57kip2和p21cip1 在人脑胶质瘤中的表达和临床意义 [J] 西安交通大学学报(医学版), 2008, 29(5): 562-5].
    [2] Amos S,Redpath GT,Polar G,et al.Farnesylthiosalicylic acid induces caspase activation and apoptosis in glioblastoma cells[J]. Cell Death Differ,2006,13(4):642-51.
    [3] Parsa AT,Waldron JS,Panner A,et al.Loss of tumor suppressor PTEN function increase B7-H1 expression and immunoresistance in glioma[J]. Nat Med,2007,13(1):84-8.
    [4] MassaguéJ .How cells read TGF-beta signals[J].Nat Rev Mol Cell Biol,2000,1 (3):169-78.
    [5] Zhang WL,Sun WW,Bu LS,et al.Smad protein families and BMPs signaling transduction [J].Zhongguo Di Fang Bing Xue Za Zhi, 20 02,21(4):325-6.[张文岚,孙文伟,卜丽莎,等.Smad蛋白 家族与骨形态发生蛋白信号传导[J].中国地方病学杂志, 20 02,21(4):325-6.]
    [6] Li L,Xin H,Xu X,et al.CHIP mediates degradation of Smad proteins and potentially regulates Smad-induced transcription[J]. Mol Cell Biol,2004,24(2):856-64.
    [7] Song XX.Bone morphogenetic proteins in basic study and clinical application[J].Xian Dai Yi Yao Wei Sheng, 2007,23(7): 10 03-4.[宋兴贤.骨形态发生蛋白的基础研究及临床应用[J].现 代医药卫生,2007,23(7): 1003-4.]
    [8] Xiangming C, Natsugoe S, Takao S, et al.Preserved Smad4 expression in the transforming growth factor beta signaling pathway is a favorable prognostic factor in patients with advanced gastric cancer [J]. Clin Cancer Res,2001,7(2):277-82.
    [9] Piestrzeniewicz Ulanska D,Brys M,Semczuk A,et al. Expression and intracellular localization of Smad proteins in human endometrial cancer[J].Oncol Rep, 2003,10(5):1539-44.
    [10] Derynck R, Zhang YE. Smad-dependent and Smad-independent pathways in TGF-beta family signalling[J]. Nature,2003,425(695 8) :577-84.
    [11] Nicolás FJ, Hill CS. Attenuation of the TGF-beta-Smad signaling path way in pancreatic tumor cells confers resistance to TGF-betainduced growth arrest [J]. Oncogene,2003,22(24):3698-711.
    [12] Maliekal TT,Antony ML,Nair A,et al. Loss of expression,and mutation of Smad-2 and Smad-4 in human cervical cancer[J]. Oncogene 2003,22(31):4889-97.
    [13] Kim YH, Lee HS, Lee HJ, et al.Prognostic significance of the expression of Smad4 and Smad7 in human gastric carcinomas [J]. Ann Oncol,2004,15(4):574-80.
    [14] Liu S. Glioma BMPs/Smad, signal paths in the expression and function of the study[D]. Beijing:Academy of Military Medical Sciences, 2007. [刘爽. 胶质瘤中BMPs/Smad信号路径的表达及 功能研究[D].北京:军事医学科学院,2007.]
    [15] Rosenzweig BL, Imamura T, Okadome T, et al. Cloning and characterization of a human type II receptor for bone morphogenetic proteins[J]. Proc Natl Sci U S A,1995,92(17):7632-6.
    [16] Shao BY, Chen QX, Liu G, et al. Expression and Effects of Smad4 and Smad7 in Human Glioma[J]. Zhong Liu Fang Zhi Yan Jiu,2005,32(3):132-4.[邵步云,陈谦学,刘刚,等. Smad4 和Smad7在人脑胶质瘤中的表达及意义[ J ] . 肿瘤防治研 究,2005,32(3):132-4.]
    • 相关文章
    • 施引文献
    • 资源附件(0)
计量
  • 文章访问数:  1504
  • HTML全文浏览量:  323
  • PDF下载量:  833
  • 被引次数: 0
出版历程
  • 收稿日期:  2012-10-14
  • 修回日期:  2013-02-21
  • 刊出日期:  2014-01-24

目录

摘要
HTML全文
    参考文献(16)
    相关文章
    施引文献
    资源附件(0)

    /

    返回文章
    返回

    下载中心

    友情链接

    联系我们

    地址:武汉市洪山区卓刀泉南路116号(430079)

    电话:027-87670126

    Email:zlfzyjzz@vip.163.com

    This work is licensed under a Creative Commons Attribution 3.0 License.

    邮件订阅 RSS
    总访问量:12056696 今日访问:20375

    版权所有 © 《肿瘤防治研究》编辑部 鄂公网安备 42011102005013号 鄂ICP备2022015867号

    本系统由北京仁和汇智信息技术有限公司开发  百度统计

    x 关闭 永久关闭