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Pan-cancer proteogenomic investigations identify post-transcriptional kinase targets

Abdülkadir Elmas, Serena Tharakan, Suraj K. Jaladanki, Matthew D. Galsky, Tao Liu, Kuan‐lin Huang

2021Communications Biology17 citationsDOIOpen Access PDF

Abstract

Identifying genomic alterations of cancer proteins has guided the development of targeted therapies, but proteomic analyses are required to validate and reveal new treatment opportunities. Herein, we develop a new algorithm, OPPTI, to discover overexpressed kinase proteins across 10 cancer types using global mass spectrometry proteomics data of 1,071 cases. OPPTI outperforms existing methods by leveraging multiple co-expressed markers to identify targets overexpressed in a subset of tumors. OPPTI-identified overexpression of ERBB2 and EGFR proteins correlates with genomic amplifications, while CDK4/6, PDK1, and MET protein overexpression frequently occur without corresponding DNA- and RNA-level alterations. Analyzing CRISPR screen data, we confirm expression-driven dependencies of multiple currently-druggable and new target kinases whose expressions are validated by immunochemistry. Identified kinases are further associated with up-regulated phosphorylation levels of corresponding signaling pathways. Collectively, our results reveal protein-level aberrations-sometimes not observed by genomics-represent cancer vulnerabilities that may be targeted in precision oncology.

Topics & Concepts

DruggabilityProteomicsKinaseBiologyComputational biologyProteogenomicsCancerGenomicsCancer researchPhosphorylationBioinformaticsGeneGeneticsGenomeCancer-related Molecular PathwaysUbiquitin and proteasome pathwaysCancer Genomics and Diagnostics
Pan-cancer proteogenomic investigations identify post-transcriptional kinase targets | Litcius