Proteome activity landscapes of tumor cell lines determine drug responses

Author:

Frejno MartinORCID,Meng Chen,Ruprecht BenjaminORCID,Oellerich Thomas,Scheich SebastianORCID,Kleigrewe KarinORCID,Drecoll Enken,Samaras PatroklosORCID,Hogrebe AlexanderORCID,Helm DominicORCID,Mergner JuliaORCID,Zecha JanaORCID,Heinzlmeir StephanieORCID,Wilhelm MathiasORCID,Dorn Julia,Kvasnicka Hans-MichaelORCID,Serve Hubert,Weichert Wilko,Kuster BernhardORCID

Abstract

AbstractIntegrated analysis of genomes, transcriptomes, proteomes and drug responses of cancer cell lines (CCLs) is an emerging approach to uncover molecular mechanisms of drug action. We extend this paradigm to measuring proteome activity landscapes by acquiring and integrating quantitative data for 10,000 proteins and 55,000 phosphorylation sites (p-sites) from 125 CCLs. These data are used to contextualize proteins and p-sites and predict drug sensitivity. For example, we find that Progesterone Receptor (PGR) phosphorylation is associated with sensitivity to drugs modulating estrogen signaling such as Raloxifene. We also demonstrate that Adenylate kinase isoenzyme 1 (AK1) inactivates antimetabolites like Cytarabine. Consequently, high AK1 levels correlate with poor survival of Cytarabine-treated acute myeloid leukemia patients, qualifying AK1 as a patient stratification marker and possibly as a drug target. We provide an interactive web application termed ATLANTiC (http://atlantic.proteomics.wzw.tum.de), which enables the community to explore the thousands of novel functional associations generated by this work.

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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