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A New Mathematical Model for the Interpretation of Translational Research Evaluating Six CTLA-4 Polymorphisms in High-Risk Melanoma Patients Receiving Adjuvant Interferon

机译:一种新的数学模型解释研究评估高危黑色素瘤患者接受佐剂干扰素的六种CTLA-4多态性的翻译研究。

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摘要

Adjuvant therapy of stage IIB/III melanoma with interferon reduces relapse and mortality by up to 33% but is accompanied by toxicity-related complications. Polymorphisms of the CTLA-4 gene associated with autoimmune diseases could help in identifying interferon treatment benefits. We previously genotyped 286 melanoma patients and 288 healthy (unrelated) individuals for six CTLA-4 polymorphisms (SNP). Previous analyses found no significant differences between the distributions of CTLA-4 polymorphisms in the melanoma population vs. controls, no significant difference in relapse free and overall survivals among patients and no correlation between autoimmunity and specific alleles. We report new analysis of these CTLA-4 genetic profiles, using Network Phenotyping Strategy (NPS). It is graph-theory based method, analyzing the SNP patterns. Application of NPS on CTLA-4 polymorphism captures allele relationship pattern for every patient into 6-partite mathematical graph P. Graphs P are combined into weighted 6-partite graph S, which subsequently decomposed into reference relationship profiles (RRP). Finally, every individual CTLA-4 genotype pattern is characterized by the graph distances of P from eight identified RRP's. RRP's are subgraphs of S, collecting equally frequent binary allele co-occurrences in all studied loci. If S topology represents the genetic “dominant model”, the RRP's and their characteristic frequencies are identical to expectation-maximization derived haplotypes and maximal likelihood estimates of their frequencies. The graph-representation allows showing that patient CTLA-4 haplotypes are uniquely different from the controls by absence of specific SNP combinations. New function-related insight is derived when the 6-partite graph reflects allelic state of CTLA-4. We found that we can use differences between individual P and specific RRPs to identify patient subpopulations with clearly different polymorphic patterns relatively to controls as well as to identify patients with significantly different survival.
机译:干扰素辅助治疗IIB / III期黑色素瘤可将复发和死亡率降低多达33%,但伴随有毒性相关的并发症。与自身免疫性疾病相关的CTLA-4基因多态性可以帮助确定干扰素治疗的益处。我们先前对286位黑色素瘤患者和288位健康(无关)个体进行了6种CTLA-4多态性(SNP)的基因分型。先前的分析发现,黑色素瘤人群与对照组的CTLA-4多态性分布之间无显着差异,患者之间的无复发生存率和总生存率无显着差异,自身免疫性与特定等位基因之间无相关性。我们使用网络表型分析策略(NPS)报告了这些CTLA-4遗传图谱的新分析。它是基于图论的方法,用于分析SNP模式。 NPS在CTLA-4多态性上的应用将每个患者的等位基因关系模式捕获到6部分数学图P中。图P组合为加权6部分图形S,随后将其分解为参考关系曲线(RRP)。最后,每个单独的CTLA-4基因型模式的特征是P与八个已识别RRP的图距。 RRP是S的子图,它在所有研究的基因座中收集同等频繁的二进制等位基因共现。如果S拓扑表示遗传“主导模型”,则RRP及其特征频率与期望最大化派生的单倍型及其频率的最大似然估计相同。该图表示允许显示患者CTLA-4单倍型由于不存在特定SNP组合而与对照唯一不同。当6部分图反映CTLA-4的等位基因状态时,将获得新的功能相关见解。我们发现,我们可以利用个体P和特定RRP之间的差异来鉴定相对于对照具有明显不同多态型的患者亚群,以及鉴定具有明显不同生存率的患者。

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