Metabolic Response to Small Molecule Therapy in Colorectal Cancer Tracked with Raman Spectroscopy and Metabolomics

Author:

Cutshaw Gabriel12,Joshi Neeraj3,Wen Xiaona2ORCID,Quam Elizabeth12,Bogatcheva Galina3,Hassan Nora12,Uthaman Saji12ORCID,Waite Joshua4,Sarkar Soumik4,Singh Bhuminder3,Bardhan Rizia12ORCID

Affiliation:

1. Department of Chemical and Biological Engineering Iowa State University Ames IA 50011 USA

2. Nanovaccine Institute Iowa State University Ames IA 50012 USA

3. Department of Medicine Vanderbilt University Medical Center Nashville TN 37232 USA

4. Department of Mechanical Engineering Iowa State University Ames IA 50012 USA

Abstract

AbstractDespite numerous screening tools for colorectal cancer (CRC), 25 % of patients are diagnosed with advanced disease. Novel diagnostic technologies that are early, accurate, and rapid are imperative to assess the therapeutic efficacy of clinical drugs and identify new biomarkers of treatment response. Here Raman spectroscopy (RS) was used to track metabolic reprogramming in KRAS‐mutant HCT116 and SW837 cells, and KRAS wild‐type CC cells. RS combined with multivariate analysis methods distinguished nonresponsive, partially responsive, and responsive cells treated with cetuximab, a monoclonal antibody for EGFR inhibition, sotorasib, a clinically approved KRAS inhibitor, and various doses of trametinib, an inhibitor of the MAPK pathway. Cells treated with a combination of subtoxic doses of trametinib and BKM120, an inhibitor of the PI3K pathway, showed a synergistic response between the two pathways. Using a supervised machine learning regression model, we established a scoring methodology trained to a priori predict therapeutic response to new treatment combinations. RS metabolites were verified with mass spectrometry, and enrichment pathways were identified, including amino acid, purine, and nicotinate and nicotinamide metabolism that differentiated monotherapy from combination therapy. Our approach may ultimately be applicable to patient‐derived primary cells and cultures of patient tumors to predict effective drugs for individualized care.

Publisher

Wiley

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