Stromal Contribution to the Colorectal Cancer Transcriptome

Overview

Journal Nat Genet

Specialty Genetics

Date 2015 Feb 24

PMID 25706627

Citations 356

Authors

Claudio Isella

Andrea Terrasi

Sara Erika Bellomo

Consalvo Petti

Giovanni Galatola

Andrea Muratore

Alfredo Mellano

Rebecca Senetta

Adele Cassenti

Cristina Sonetto

Giorgio Inghirami

Livio Trusolino

Zsolt Fekete

Mark De Ridder

Paola Cassoni

Guy Storme

Andrea Bertotti

Enzo Medico

Affiliations

Soon will be listed here.

Abstract

Recent studies identified a poor-prognosis stem/serrated/mesenchymal (SSM) transcriptional subtype of colorectal cancer (CRC). We noted that genes upregulated in this subtype are also prominently expressed by stromal cells, suggesting that SSM transcripts could derive from stromal rather than epithelial cancer cells. To test this hypothesis, we analyzed CRC expression data from patient-derived xenografts, where mouse stroma supports human cancer cells. Species-specific expression analysis showed that the mRNA levels of SSM genes were mostly due to stromal expression. Transcriptional signatures built to specifically report the abundance of cancer-associated fibroblasts (CAFs), leukocytes or endothelial cells all had significantly higher expression in human CRC samples of the SSM subtype. High expression of the CAF signature was associated with poor prognosis in untreated CRC, and joint high expression of the stromal signatures predicted resistance to radiotherapy in rectal cancer. These data show that the distinctive transcriptional and clinical features of the SSM subtype can be ascribed to its particularly abundant stromal component.

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