文章摘要
赵振宇卢亦成△ 陈菊祥侯立军胡国汉骆纯.基于生物信息学技术筛选影响胶质母细胞瘤化疗敏感性 相关基因的研究[J].,2011,11(19):3601-3604
基于生物信息学技术筛选影响胶质母细胞瘤化疗敏感性 相关基因的研究
Using Bioinformatics Method to Investigate the Genes Related toChemosensitivity in Human Glioblastoma
  
DOI:
中文关键词: 胶质母细胞瘤  基因芯片  生物信息学  化疗敏感性
英文关键词: Glioblastoma  Genechip  Bioinformatics  Chemosensitivity
基金项目:国家自然科学基金重点项目(30930094), 国家863 项目( 2007AA02Z483)
作者单位
赵振宇卢亦成△ 陈菊祥侯立军胡国汉骆纯 第二军医大学长征医院神经外科 
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中文摘要:
      目的:应用生物信息学技术筛选影响胶质母细胞瘤(GBM)化疗敏感性的相关基因。方法:对2 批胶质瘤患者BIOSTAR 基 因芯片进行分析。通过随访完善临床资料,筛选芯片中胶质母细胞瘤患者生存期长、短两组间的差异基因,明确差异基因参与的 功能和通路,并构建与烷化剂相关基因的信号传导网络,结合芯片数据、患者预后和信号传导网络,筛选GBM 化疗敏感性的相关 基因。结果:两组芯片中间差异基因有503 条。2 批芯片的差异基因主要参与62 项基因功能,主要参与31 条信号传导通路。通过 对差异基因功能、通路,烷化剂信号转导网络的分析,得到影响胶质母细胞瘤化疗敏感性的核心的差异基因IFNGR2、IL8、ITGA5、 TNFRSF1B。结论:通过严谨的实验设计和科学的统计学判别,结合患者完整的生存资料,本研究成功地应用生物信息学技术对基 因芯片的大量数据进行挖掘和分析,并筛选出了可能影响GBM 患者预后和化疗药物敏感性的基因,为进一步功能实验和患者个 体化治疗奠定了基础。
英文摘要:
      Objective: Bioinformatics method was used to analyze data of cDNA microarray to investigate the genes related to survival time and drug sensitivity in GBM. Methods: Biostar microarray of GBM patients were analyzed, and clinical data of these patients in the microarray were perfected through long-term follow-up study. Differential expression genes between the long- and short- survival groups were picked out, GO-analysis and pathway-analysis of the differential expression genes were performed. Drug-related signal transduction networks were constructed. The methods combined three steps before were used to screen core genes that influenced chemosensitivity. Results: There were 503 differentiate genes that influenced survival duration of GBM respectively. They mainly participated in 62 gene functions and 31 signaling transduction pathways, based on which 4 core genes that influenced chemosensitivity of GBM to Chemistry drug were obtained, including IFNGR2, IL8, ITGA5, TNFRSF1B. Conclusion: With complete clinical information, mass data of cDNA microaray can be further analyzed by using bioinformatics method. These genes were found to predict the clinical outcomes and have a significant influence on chemosensitivity in GBM. This study will provide a foundation not only for the further functional research but also for prediction of prognosis and fulfillment of personalization chemotherapy in GBM.
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