Illuminating phenotypic drug responses of sarcoma cells to kinase inhibitors by phosphoproteomics

Author:

Lee Chien-YunORCID,The MatthewORCID,Meng ChenORCID,Bayer Florian P,Putzker KerstinORCID,Müller JulianORCID,Streubel Johanna,Woortman JuliaORCID,Sakhteman Amirhossein,Resch Moritz,Schneider AnnikaORCID,Wilhelm StephanieORCID,Kuster BernhardORCID

Abstract

AbstractKinase inhibitors (KIs) are important cancer drugs but often feature polypharmacology that is molecularly not understood. This disconnect is particularly apparent in cancer entities such as sarcomas for which the oncogenic drivers are often not clear. To investigate more systematically how the cellular proteotypes of sarcoma cells shape their response to molecularly targeted drugs, we profiled the proteomes and phosphoproteomes of 17 sarcoma cell lines and screened the same against 150 cancer drugs. The resulting 2550 phenotypic profiles revealed distinct drug responses and the cellular activity landscapes derived from deep (phospho)proteomes (9–10,000 proteins and 10–27,000 phosphorylation sites per cell line) enabled several lines of analysis. For instance, connecting the (phospho)proteomic data with drug responses revealed known and novel mechanisms of action (MoAs) of KIs and identified markers of drug sensitivity or resistance. All data is publicly accessible via an interactive web application that enables exploration of this rich molecular resource for a better understanding of active signalling pathways in sarcoma cells, identifying treatment response predictors and revealing novel MoA of clinical KIs.

Funder

Bundesministerium für Bildung und Forschung

EC | ERC | HORIZON EUROPE European Research Council

Ministry of Science and Technology, Taiwan

TUM University Foundation Fellowship

Publisher

Springer Science and Business Media LLC

Subject

Applied Mathematics,Computational Theory and Mathematics,General Agricultural and Biological Sciences,General Immunology and Microbiology,General Biochemistry, Genetics and Molecular Biology,Information Systems

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