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Systematic use of computational methods allows stratification of treatment responders in glioblastoma multiforme

机译:系统地使用计算方法可以对多形性胶质母细胞瘤中的治疗反应者进行分层

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Background:?Cancers are complex diseases whose comprehensive characterization requires genome-scale molecular data at multiple levels from genetics to transcriptomics and clinical data. Using our recently published Anduril bioinformatics framework and novel computational approaches, such as dependency analysis, we identify key variables at miRNA, copy number variation, expression, methylation, and pathway levels in glioblastoma multiforme (GBM) progression and drug resistance. Furthermore, we identify characteristics of clinically relevant subgroups, such as patients treated with temozolomide and patients with an EGFRvIII mutation, which is a constitutively active variant of EGFR.Results:?We identify several novel genomic regions and transcript profiles that may contribute to GBM progression and drug resistance. All results and Anduril scripts are available at http://csbi.ltdk.helsinki.fi/camda/.Conclusions:?Our results highlight the need for approaches that define context at several levels in order to identify genomic regions or transcript profiles playing key roles in cancer progression and drug resistance.
机译:背景:癌症是复杂的疾病,其全面表征需要从遗传学到转录组学以及临床数据等多个层面的基因组规模分子数据。使用我们最近发布的Anduril生物信息学框架和新颖的计算方法(例如依赖性分析),我们可以识别miRNA的关键变量,拷贝数变异,表达,甲基化以及胶质母细胞瘤(GBM)进展和耐药性中的途径水平。此外,我们确定了临床相关亚组的特征,例如用替莫唑胺治疗的患者和EGFRvIII突变的患者,后者是EGFR的组成性活性变异体。结果:我们鉴定了一些可能有助于GBM进展的新型基因组区域和转录谱和耐药性。所有结果和Anduril脚本都可以在http://csbi.ltdk.helsinki.fi/camda/上获得。结论:我们的结果强调了需要在几个级别上定义上下文的方法,以便识别基因组区域或转录本概况在癌症进展和耐药性中的作用。

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