机构:[1]The Ministry-Province Jointly Constructed Base for State Key Lab and Shenzhen Technology and Engineering Labfor Personalized Cancer Diagnostics and Therapeutics Tsinghua University Shenzhen Graduate School, and ShenzhenKivita Innovative Drug Discovery Institute, Shenzhen, 518055, P.R. China.[2]Institute of Molecular Biology (IMB),Ackermannweg 4, 55128 Mainz, Germany.[3]Department of Pharmacy, and Center for Computational Science andEngineering, National University of Singapore, Blk S16, Level 8, 3 Science Drive 2, 117543 Singapore.[4]State KeyLaboratory of Biotherapy, West China Hospital, West China School of Medicine, Sichuan University, Chengdu, China.四川大学华西医院
Synergistic drug combinations enable enhanced therapeutics. Their discovery typically involves the measurement and assessment of drug combination index (CI), which can be facilitated by the development and applications of in-silico CI predictive tools. In this work, we developed and tested the ability of a mathematical model of drug-targeted EGFR-ERK pathway in predicting CIs and in analyzing multiple synergistic drug combinations against observations. Our mathematical model was validated against the literature reported signaling, drug response dynamics, and EGFR-MEK drug combination effect. The predicted CIs and combination therapeutic effects of the EGFR-BRaf, BRaf-MEK, FTI-MEK, and FTI-BRaf inhibitor combinations showed consistent synergism. Our results suggest that existing pathway models may be potentially extended for developing drug-targeted pathway models to predict drug combination CI values, isobolograms, and drug-response surfaces as well as to analyze the dynamics of individual and combinations of drugs. With our model, the efficacy of potential drug combinations can be predicted. Our method complements the developed in-silico methods (e.g. the chemogenomic profile and the statistically-inferenced network models) by predicting drug combination effects from the perspectives of pathway dynamics using experimental or validated molecular kinetic constants, thereby facilitating the collective prediction of drug combination effects in diverse ranges of disease systems.
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外文
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出版当年[2017]版:
大类|3 区综合性期刊
小类|3 区综合性期刊
最新[2023]版:
大类|2 区综合性期刊
小类|2 区综合性期刊
第一作者:
第一作者机构:[1]The Ministry-Province Jointly Constructed Base for State Key Lab and Shenzhen Technology and Engineering Labfor Personalized Cancer Diagnostics and Therapeutics Tsinghua University Shenzhen Graduate School, and ShenzhenKivita Innovative Drug Discovery Institute, Shenzhen, 518055, P.R. China.[2]Institute of Molecular Biology (IMB),Ackermannweg 4, 55128 Mainz, Germany.[3]Department of Pharmacy, and Center for Computational Science andEngineering, National University of Singapore, Blk S16, Level 8, 3 Science Drive 2, 117543 Singapore.
通讯作者:
通讯机构:[3]Department of Pharmacy, and Center for Computational Science andEngineering, National University of Singapore, Blk S16, Level 8, 3 Science Drive 2, 117543 Singapore.[4]State KeyLaboratory of Biotherapy, West China Hospital, West China School of Medicine, Sichuan University, Chengdu, China.
推荐引用方式(GB/T 7714):
Huang Lu,Jiang Yuyang,Chen Yuzong.Predicting Drug Combination Index and Simulating the Network-Regulation Dynamics by Mathematical Modeling of Drug-Targeted EGFR-ERK Signaling Pathway.[J].Scientific reports.2017,7:40752.doi:10.1038/srep40752.
APA:
Huang Lu,Jiang Yuyang&Chen Yuzong.(2017).Predicting Drug Combination Index and Simulating the Network-Regulation Dynamics by Mathematical Modeling of Drug-Targeted EGFR-ERK Signaling Pathway..Scientific reports,7,
MLA:
Huang Lu,et al."Predicting Drug Combination Index and Simulating the Network-Regulation Dynamics by Mathematical Modeling of Drug-Targeted EGFR-ERK Signaling Pathway.".Scientific reports 7.(2017):40752
