Proteogenomics of Colorectal Cancer Liver Metastases: Complementing Precision Oncology with Phenotypic Data

Overview

Journal Cancers (Basel)

Publisher MDPI

Specialty Oncology

Date 2019 Dec 7

PMID 31805664

Citations 7

Authors

Bernhard Blank-Landeshammer

Vincent R Richard

Georgia Mitsa

Maud Marques

Andre LeBlanc

Laxmikanth Kollipara

Ingo Feldmann

Mathilde Couetoux du Tertre

Karen Gambaro

Suzan McNamara

Alan Spatz

Rene P Zahedi

Albert Sickmann

Gerald Batist

Christoph H Borchers

Affiliations

Soon will be listed here.

Abstract

Hotspot testing for activating mutations is used in precision oncology to select colorectal cancer (CRC) patients who are eligible for anti-EGFR treatment. However, even for tumors anti-EGFR response rates are <30%, while mutated- does not entirely rule out response, indicating the need for improved patient stratification. We performed proteogenomic phenotyping of and CRC liver metastases (mCRC). Among >9000 proteins we detected considerable expression changes including numerous proteins involved in progression and resistance in CRC. We identified peptides representing a number of predicted somatic mutations, including KRAS. For eight of these, we developed a multiplexed parallel reaction monitoring (PRM) mass spectrometry assay to precisely quantify the mutated and canonical protein variants. This allowed phenotyping of eight mCRC tumors and six paired healthy tissues, by determining mutation rates on the protein level. Total KRAS expression varied between tumors (0.47-1.01 fmol/µg total protein) and healthy tissues (0.13-0.64 fmol/µg). In -mCRC, G12V-mutation levels were 42-100%, while one patient had only 10% KRAS but 90% KRAS. This might represent a missed therapeutic opportunity: based on hotspot sequencing, the patient was excluded from anti-EGFR treatment and instead received chemotherapy, while PRM-based tumor-phenotyping indicates the patient might have benefitted from anti-EGFR therapy.

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