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Improved drug therapy: triangulating phenomics with genomics and metabolomics

机译:改进的药物治疗:利用基因组学和代谢组学对表观基因组学进行三角剖分

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摘要

Embracing the complexity of biological systems has a greater likelihood to improve prediction of clinical drug response. Here we discuss limitations of a singular focus on genomics, epigenomics, proteomics, transcriptomics, metabolomics, or phenomics—highlighting the strengths and weaknesses of each individual technique. In contrast, ‘systems biology’ is proposed to allow clinicians and scientists to extract benefits from each technique, while limiting associated weaknesses by supplementing with other techniques when appropriate. Perfect predictive modeling is not possible, whereas modeling of intertwined phenomic responses using genomic stratification with metabolomic modifications may greatly improve predictive values for drug therapy. We thus propose a novel-integrated approach to personalized medicine that begins with phenomic data, is stratified by genomics, and ultimately refined by metabolomic pathway data. Whereas perfect prediction of efficacy and safety of drug therapy is not possible, improvements can be achieved by embracing the complexity of the biological system. Starting with phenomics, the combination of linking metabolomics to identify common biologic pathways and then stratifying by genomic architecture, might increase predictive values. This systems biology approach has the potential, in specific subsets of patients, to avoid drug therapy that will be either ineffective or unsafe.
机译:拥抱生物系统的复杂性更有可能改善对临床药物反应的预测。在这里,我们讨论对基因组学,表观基因组学,蛋白质组学,转录组学,代谢组学或表组学的单一关注的局限性,从而突出每种技术的优缺点。相反,提出“系统生物学”的目的是允许临床医生和科学家从每种技术中受益,同时通过在适当时补充其他技术来限制相关的弱点。不可能建立完美的预测模型,而使用基因组分层和代谢组学修饰对交织的表型反应进行建模可能会大大改善药物治疗的预测价值。因此,我们提出了一种新型的个性化医学整合方法,该方法以表型学数据开始,通过基因组学进行分层,最后通过代谢组学途径数据进行完善。尽管不可能完美预测药物治疗的功效和安全性,但可以通过拥抱生物系统的复杂性来实现改善。从表型学出发,将代谢组学联系起来以识别常见的生物学途径,然后通过基因组结构进行分层,可能会增加预测价值。这种系统生物学方法在特定的患者亚群中有可能避免无效或不安全的药物治疗。

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