Abstract

The Data Generation Core will focus on measuring the effect of drug combinations and individual drugs on cell types associated with hepatic toxicity, cardiac toxicity and peripheral neuropathy adverse events observed at the organism level. These are all serious adverse events that alter drug usage and development. A novel feature of our experimental design is our selection of drug combinations. Most Americans take multiple drugs. Exhaustively testing all potential drug combinations is intractable due to the combinatorial explosion of possibilities and has not been done by any previous large scale effort. Our preliminary data based on analysis of serious drug adverse events as reported in FAERS has revealed 120 drug combinations involving 130 individual drugs whereby addition of a second drug significantly mitigates the serious toxicity induced by the first drug. We will use a panel of human cardiomyocytes, hepatocytes, and neuronal cell lines from primary/established lines, as well as those derived from human induced pluripotent stem cells. The total of number of cell lines is 18. The experimental data will be high-throughput, producing greater than 1 million data points per year. It will be on the genome-wide whole cell level and include changes in mRNA levels (microarray) and changes in protein levels (mass spec). We expect that a combination of mRNA and protein level data will synergize in signature generation. Our use of established yet cost effective methodologies is desirable since it enables immediate production and facilitates more widespread uptake and reproduction. These data together will be used to develop cellular signatures for the drugs or drug combinations in the Data Analysis and Signature Generation Core. The signatures will highlight key pathways that inform targeted, medium-throughput measurements of protein states by microwestern array. These targeted measurements will characterize dose and dynamic responses of biological states relevant to our drugs and drug combinations. Throughout we focus on careful annotation and quality control for dissemination of these data to the community, and also are open to community feedback in altering our preliminary plan.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Human Genome Research Institute (NHGRI)
Type
Specialized Center--Cooperative Agreements (U54)
Project #
5U54HG008098-02
Application #
8925129
Study Section
Special Emphasis Panel (ZRG1-CB-D)
Project Start
Project End
Budget Start
2015-07-01
Budget End
2016-06-30
Support Year
2
Fiscal Year
2015
Total Cost
$921,906
Indirect Cost
$308,772

  Institution

Name
Icahn School of Medicine at Mount Sinai
Department
Type
DUNS #
078861598
City
New York
State
NY
Country
United States
Zip Code
10029

  Publications

Jones, DeAnalisa C; Gong, Jingqi Q X; Sobie, Eric A (2018) A privileged role for neuronal Na+ channels in regulating ventricular [Ca2+] and arrhythmias. J Gen Physiol 150:901-905
Barrette, Anne Marie; Bouhaddou, Mehdi; Birtwistle, Marc R (2018) Integrating Transcriptomic Data with Mechanistic Systems Pharmacology Models for Virtual Drug Combination Trials. ACS Chem Neurosci 9:118-129
Keenan, Alexandra B; Jenkins, Sherry L; Jagodnik, Kathleen M et al. (2018) The Library of Integrated Network-Based Cellular Signatures NIH Program: System-Level Cataloging of Human Cells Response to Perturbations. Cell Syst 6:13-24
Bouhaddou, Mehdi; Barrette, Anne Marie; Stern, Alan D et al. (2018) A mechanistic pan-cancer pathway model informed by multi-omics data interprets stochastic cell fate responses to drugs and mitogens. PLoS Comput Biol 14:e1005985
Koch, Rick J; Barrette, Anne Marie; Stern, Alan D et al. (2018) Validating Antibodies for Quantitative Western Blot Measurements with Microwestern Array. Sci Rep 8:11329
Sobie, Eric A; Williams, George S B; Lederer, W J (2017) Ambiguous interactions between diastolic and SR Ca2+in the regulation of cardiac Ca2+release. J Gen Physiol 149:847-855
Xiong, Yuguang; Soumillon, Magali; Wu, Jie et al. (2017) A Comparison of mRNA Sequencing with Random Primed and 3'-Directed Libraries. Sci Rep 7:14626
Shim, Jaehee V; Chun, Bryan; van Hasselt, Johan G C et al. (2017) Mechanistic Systems Modeling to Improve Understanding and Prediction of Cardiotoxicity Caused by Targeted Cancer Therapeutics. Front Physiol 8:651
Gong, Jingqi Q X; Shim, Jaehee V; Núñez-Acosta, Elisa et al. (2017) I love it when a plan comes together: Insight gained through convergence of competing mathematical models. J Mol Cell Cardiol 102:31-33
Stern, Alan D; Rahman, Adeeb H; Birtwistle, Marc R (2017) Cell size assays for mass cytometry. Cytometry A 91:14-24

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