Journal of Experimental & Clinical Cancer Research (Jan 2023)

“Proteotranscriptomic analysis of advanced colorectal cancer patient derived organoids for drug sensitivity prediction”

  • Federica Papaccio,
  • Blanca García-Mico,
  • Francisco Gimeno-Valiente,
  • Manuel Cabeza-Segura,
  • Valentina Gambardella,
  • María Fernanda Gutiérrez-Bravo,
  • Clara Alfaro-Cervelló,
  • Carolina Martinez-Ciarpaglini,
  • Pilar Rentero-Garrido,
  • Sheila Zúñiga-Trejos,
  • Juan Antonio Carbonell-Asins,
  • Tania Fleitas,
  • Susana Roselló,
  • Marisol Huerta,
  • Manuel M. Sánchez del Pino,
  • Luís Sabater,
  • Desamparados Roda,
  • Noelia Tarazona,
  • Andrés Cervantes,
  • Josefa Castillo

DOI
https://doi.org/10.1186/s13046-022-02591-z
Journal volume & issue
Vol. 42, no. 1
pp. 1 – 22

Abstract

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Abstract Background Patient-derived organoids (PDOs) from advanced colorectal cancer (CRC) patients could be a key platform to predict drug response and discover new biomarkers. We aimed to integrate PDO drug response with multi-omics characterization beyond genomics. Methods We generated 29 PDO lines from 22 advanced CRC patients and provided a morphologic, genomic, and transcriptomic characterization. We performed drug sensitivity assays with a panel of both standard and non-standard agents in five long-term cultures, and integrated drug response with a baseline proteomic and transcriptomic characterization by SWATH-MS and RNA-seq analysis, respectively. Results PDOs were successfully generated from heavily pre-treated patients, including a paired model of advanced MSI high CRC deriving from pre- and post-chemotherapy liver metastasis. Our PDOs faithfully reproduced genomic and phenotypic features of original tissue. Drug panel testing identified differential response among PDOs, particularly to oxaliplatin and palbociclib. Proteotranscriptomic analyses revealed that oxaliplatin non-responder PDOs present enrichment of the t-RNA aminoacylation process and showed a shift towards oxidative phosphorylation pathway dependence, while an exceptional response to palbociclib was detected in a PDO with activation of MYC and enrichment of chaperonin T-complex protein Ring Complex (TRiC), involved in proteome integrity. Proteotranscriptomic data fusion confirmed these results within a highly integrated network of functional processes involved in differential response to drugs. Conclusions Our strategy of integrating PDOs drug sensitivity with SWATH-mass spectrometry and RNA-seq allowed us to identify different baseline proteins and gene expression profiles with the potential to predict treatment response/resistance and to help in the development of effective and personalized cancer therapeutics.

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