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MEK/ERK通路蛋白在肾癌骨转移患者的表达
引用本文:秦彩朋,刘春雷,赵燕辉,殷华奇,杜依青,胡风战,盛正祚,徐涛. MEK/ERK通路蛋白在肾癌骨转移患者的表达[J]. 北京大学学报(医学版), 2016, 48(4): 590-593. DOI: 10.3969/j.issn.1671-167X.2016.04.004
作者姓名:秦彩朋  刘春雷  赵燕辉  殷华奇  杜依青  胡风战  盛正祚  徐涛
作者单位:(1. 北京大学人民医院泌尿外科, 北京100044; 2. 北京大学国际医院泌尿外科, 北京102206; 3. 青岛市中心医院泌尿外科, 山东青岛266042)
基金项目:北京市科技计划项目(Z151100003915145)资助 Supported by the Beijing Science and Technology Planning Project (Z151100003915145)
摘    要:目的:探讨MEK/ERK通路蛋白在肾癌骨转移患者原发灶及转移灶表达的差异及其意义,并探索这种差异的发生机制。方法: 选择北京大学人民医院2009年1月至2010年1月 7例肾癌骨转移患者的原发灶及转移灶组织标本,应用免疫组织化学法分析VEGFR-2、MEK、ERK蛋白在原发灶与转移灶表达的差异,VEGFR-2、MEK、ERK的Ⅰ抗工作浓度(体积比)分别为1 ∶200、1 ∶25、1 ∶250,应用PCR技术检测PDGFRA基因20号外显子,K-ras基因2号外显子,Braf基因15号外显子和MEK1基因2号外显子的相关突变。结果:免疫组织化学结果判读:细胞阳性率≤ 5% 为1分, 6% ~50% 为2分, 51% ~ 100% 为3分; 染色强度: 不着色为1分, 淡黄色细颗粒状为2分, 黄色颗粒状为3分, 棕黄色粗颗粒状为4分,将两个得分数相乘得到其表达强度。本组7例肾癌骨转移患者VEGFR-2在原发灶(2.86±2.27)和骨转移灶(2.67±1.85)表达差异无统计学意义(P=0.901),而MEK(1.33±0.51 vs. 6.10±4.10,P=0.015)和ERK(4.43±2.84 vs.9.10±2.24, P=0.021)表达差异有统计学意义;在原发灶及转移灶标本中并未检测到相关的基因突变。结论:MEK/ERK通路蛋白在肾癌骨转移患者原发灶和转移灶表达的差异可能与其转移过程有关,也可能是影响靶向治疗效果的原因之一。

关 键 词:  肾细胞  MAP激酶信号系统  肿瘤转移    突变  

Expression of MEK/ERK signal pathways in renal cell carcinoma with bone metasta-sis
QIN Cai-peng,LIU Chun-lei,ZHAO Yan-hui,YIN Hua-qi,DU Yi-qing,HU Feng-zhan,SHENG Zheng-zuo,XU Tao. Expression of MEK/ERK signal pathways in renal cell carcinoma with bone metasta-sis[J]. Journal of Peking University. Health sciences, 2016, 48(4): 590-593. DOI: 10.3969/j.issn.1671-167X.2016.04.004
Authors:QIN Cai-peng  LIU Chun-lei  ZHAO Yan-hui  YIN Hua-qi  DU Yi-qing  HU Feng-zhan  SHENG Zheng-zuo  XU Tao
Affiliation:(1. Department of Urology, Peking University People’s Hospital, Beijing 100044,China; 2. Department of Urology, Peking University International Hospital, Beijing 102206, China; 3. Department of Urology, Central Hospital of Qingdao, Qingdao 266042, Shandong, China)
Abstract:Objective:To investigate the expression of MEK/ERK signaling pathways in renal cell car-cinoma with bone metastasis,and to analyze the differences of expressions of VEGFR-2,MEK,ERK on the primary and metastasis tissue and its mechanism.Methods:The tissue samples were obtained from 7 renal cell carcinoma patients kindly provided by Department of Urology,Peking University People’s Hos-pital from January 1,2009 to January 1,2010.The expression of MEK/ERK signaling pathways was de-tected in the 7 renal cell carcinoma patients`primary and matched metastatic tissues with ICH,The anti-body concentrations were 1 ∶200,1 ∶25,and 1 ∶250,respectively.The mutation of the twentieth exon of the PDGFRA gene,the second exon of the K-ras gene,the fifteenth exon of the Brafgene and the se-cond exon of the MEK1 gene were detected with PCR.Results:The expression intensities of VEGFR-2, MEK,and ERK were measured by H-score [intensity (1,2,3,or 4)multiplied by the distribution (%)].VEGFR-2,MEK,and ERK expressions were divided into 3 groups according to the positive dis-tribution of the tumor cells:1,0 -5%;2,6% -50%;and 3,>50%,To assess intratumor heteroge-neity,three distinct microscopic fields (×200)from each specimen were used to evaluate the expres-sions,Subsequently,the scores were averaged to obtain a single concatenated score for each tissue. VEGFR-2,MEK,and ERK expressions were assessed by 2 independent pathologists who were blinded to the clinicopathological data.The data were expressed as the mean value of the triplicate experiments.The expressions of MEK,and ERK were higher in the metastatic tissues than in the matched RCC tissues (6.10 ±4.10 vs.1.33 ±0.51,P =0.015;9.10 ±2.24 vs.4.43 ±2.84,P =0.021 )while the ex-pression of VEGFR-2 was not different between the primary and metastatic tissues (P =0.901).No mu-tation was detected on the twentieth exon of the PDGFRA gene,the second exon of the K-ras gene,the fifteenth exon of the Brafgene and the second exon of the MEK1 gene.Conclusion:MEK/ERK signa-ling pathways may play an important role in the metastasis and the resistance of sunitinib in RCC patients with bone metastasis.
Keywords:Carcinoma,renal cell  MAP kinase signaling system  Neoplasm metastasis  Bone  Muta-tion
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