Literature DB >> 29242316

Colorectal Cancer Consensus Molecular Subtypes Translated to Preclinical Models Uncover Potentially Targetable Cancer Cell Dependencies.

Anita Sveen1,2, Jarle Bruun1,2,3, Peter W Eide1,2, Ina A Eilertsen1,2, Lorena Ramirez4, Astrid Murumägi3, Mariliina Arjama3, Stine A Danielsen1,2, Kushtrim Kryeziu1,2, Elena Elez4, Josep Tabernero4, Justin Guinney5, Hector G Palmer4, Arild Nesbakken2,6,7, Olli Kallioniemi3, Rodrigo Dienstmann4,5, Ragnhild A Lothe8,2,7.   

Abstract

Purpose: Response to standard oncologic treatment is limited in colorectal cancer. The gene expression-based consensus molecular subtypes (CMS) provide a new paradigm for stratified treatment and drug repurposing; however, drug discovery is currently limited by the lack of translation of CMS to preclinical models.Experimental Design: We analyzed CMS in primary colorectal cancers, cell lines, and patient-derived xenografts (PDX). For classification of preclinical models, we developed an optimized classifier enriched for cancer cell-intrinsic gene expression signals, and performed high-throughput in vitro drug screening (n = 459 drugs) to analyze subtype-specific drug sensitivities.
Results: The distinct molecular and clinicopathologic characteristics of each CMS group were validated in a single-hospital series of 409 primary colorectal cancers. The new, cancer cell-adapted classifier was found to perform well in primary tumors, and applied to a panel of 148 cell lines and 32 PDXs, these colorectal cancer models were shown to recapitulate the biology of the CMS groups. Drug screening of 33 cell lines demonstrated subtype-dependent response profiles, confirming strong response to EGFR and HER2 inhibitors in the CMS2 epithelial/canonical group, and revealing strong sensitivity to HSP90 inhibitors in cells with the CMS1 microsatellite instability/immune and CMS4 mesenchymal phenotypes. This association was validated in vitro in additional CMS-predicted cell lines. Combination treatment with 5-fluorouracil and luminespib showed potential to alleviate chemoresistance in a CMS4 PDX model, an effect not seen in a chemosensitive CMS2 PDX model.Conclusions: We provide translation of CMS classification to preclinical models and uncover a potential for targeted treatment repurposing in the chemoresistant CMS4 group. Clin Cancer Res; 24(4); 794-806. ©2017 AACR. ©2017 American Association for Cancer Research.

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Year:  2017        PMID: 29242316     DOI: 10.1158/1078-0432.CCR-17-1234

Source DB:  PubMed          Journal:  Clin Cancer Res        ISSN: 1078-0432            Impact factor:   12.531


  73 in total

Review 1.  Colorectal cancer: genetic abnormalities, tumor progression, tumor heterogeneity, clonal evolution and tumor-initiating cells.

Authors:  Ugo Testa; Elvira Pelosi; Germana Castelli
Journal:  Med Sci (Basel)       Date:  2018-04-13

2.  What Should We Do Better? Lessons from Negative Results of a Biomarker Validation Study.

Authors:  Francesca Battaglin; Heinz-Josef Lenz
Journal:  J Natl Cancer Inst       Date:  2019-08-01       Impact factor: 13.506

Review 3.  Molecular subtyping of colorectal cancer: Recent progress, new challenges and emerging opportunities.

Authors:  Wei Wang; Raju Kandimalla; Hao Huang; Lina Zhu; Ying Li; Feng Gao; Ajay Goel; Xin Wang
Journal:  Semin Cancer Biol       Date:  2018-05-18       Impact factor: 15.707

4.  Integrative multi-omics analysis of a colon cancer cell line with heterogeneous Wnt activity revealed RUNX2 as an epigenetic regulator of EMT.

Authors:  Hongyang Yi; Guipeng Li; Yongkang Long; Weizheng Liang; Huanhuan Cui; Bin Zhang; Ying Tan; Yunfei Li; Luochen Shen; Daqi Deng; Yisen Tang; Chenyu Mao; Shuye Tian; Yunting Cai; Qionghua Zhu; Yuhui Hu; Wei Chen; Liang Fang
Journal:  Oncogene       Date:  2020-06-13       Impact factor: 9.867

Review 5.  Biomarker-guided therapy for colorectal cancer: strength in complexity.

Authors:  Anita Sveen; Scott Kopetz; Ragnhild A Lothe
Journal:  Nat Rev Clin Oncol       Date:  2019-07-09       Impact factor: 66.675

6.  Low prevalence of deficient mismatch repair (dMMR) protein in locally advanced rectal cancers (LARC) and treatment outcomes.

Authors:  Vikas Ostwal; Nikhil S Pande; Reena Engineer; Avanish Saklani; Ashwin deSouza; Mukta Ramadwar; Suvarna Sawant; Sarika Mandavkar; Sameer Shrirangwar; Pritam Kataria; Prachi Patil; Omshree Shetty; Anant Ramaswamy
Journal:  J Gastrointest Oncol       Date:  2019-02

7.  PTGS2 Over-Expression: A Colorectal Carcinoma Initiator not an Invasive Factor.

Authors:  Tahereh Zahedi; Abasalt Hosseinzadeh Colagar; Habibollah Mahmoodzadeh
Journal:  Rep Biochem Mol Biol       Date:  2021-01

8.  Patient-Derived Xenografts and Matched Cell Lines Identify Pharmacogenomic Vulnerabilities in Colorectal Cancer.

Authors:  Luca Lazzari; Giorgio Corti; Gabriele Picco; Claudio Isella; Monica Montone; Pamela Arcella; Erika Durinikova; Eugenia R Zanella; Luca Novara; Fabiane Barbosa; Andrea Cassingena; Carlotta Cancelliere; Enzo Medico; Andrea Sartore-Bianchi; Salvatore Siena; Mathew J Garnett; Andrea Bertotti; Livio Trusolino; Federica Di Nicolantonio; Michael Linnebacher; Alberto Bardelli; Sabrina Arena
Journal:  Clin Cancer Res       Date:  2019-08-02       Impact factor: 12.531

9.  Prognostic value of the PrPC-ILK-IDO1 axis in the mesenchymal colorectal cancer subtype.

Authors:  Alexandre Ghazi; Delphine Le Corre; Camilla Pilati; Julien Taieb; Thomas Aparicio; Audrey Didelot; Shoukat Dedhar; Claire Mulot; Karine Le Malicot; Fatima Djouadi; Aurélien de Reynies; Jean-Marie Launay; Pierre Laurent-Puig; Sophie Mouillet-Richard
Journal:  Oncoimmunology       Date:  2021-06-28       Impact factor: 8.110

Review 10.  Colorectal Cancer: From Genetic Landscape to Targeted Therapy.

Authors:  Mouade El Bali; Joaira Bakkach; Mohcine Bennani Mechita
Journal:  J Oncol       Date:  2021-07-06       Impact factor: 4.375
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