| Literature DB >> 33332285 |
Yuchen Guo1, Monica Gabola1, Rossano Lattanzio2,3, Conception Paul1, Valérie Pinet1, Ruizhi Tang1, Hulya Turali1, Julie Bremond1, Ciro Longobardi1, Chloé Maurizy1, Quentin Da Costa4, Pascal Finetti4, Florence Boissière-Michot5, Benjamin Rivière1, Céline Lemmers6, Séverine Garnier4, François Bertucci4,7, Inti Zlobec8, Karim Chebli1, Jamal Tazi1, Rania Azar9, Jean-Marie Blanchard1, Peter Sicinski10, Emilie Mamessier4, Bénédicte Lemmers1, Michael Hahne1.
Abstract
To clarify the function of cyclin A2 in colon homeostasis and colorectal cancer (CRC), we generated mice deficient for cyclin A2 in colonic epithelial cells (CECs). Colons of these mice displayed architectural changes in the mucosa and signs of inflammation, as well as increased proliferation of CECs associated with the appearance of low- and high-grade dysplasias. The main initial events triggering those alterations in cyclin A2-deficient CECs appeared to be abnormal mitoses and DNA damage. Cyclin A2 deletion in CECs promoted the development of dysplasia and adenocarcinomas in a murine colitis-associated cancer model. We next explored the status of cyclin A2 expression in clinical CRC samples at the mRNA and protein levels and found higher expression in tumors of patients with stage 1 or 2 CRC compared with those of patients with stage 3 or 4 CRC. A meta-analysis of 11 transcriptome data sets comprising 2239 primary CRC tumors revealed different expression levels of CCNA2 (the mRNA coding for cyclin A2) among the CRC tumor subtypes, with the highest expression detected in consensus molecular subtype 1 (CMS1) and the lowest in CMS4 tumors. Moreover, we found high expression of CCNA2 to be a new, independent prognosis factor for CRC tumors.Entities:
Keywords: Cell cycle; Colorectal cancer; Inflammation; Mouse models; Oncology
Year: 2021 PMID: 33332285 PMCID: PMC7880422 DOI: 10.1172/JCI131517
Source DB: PubMed Journal: J Clin Invest ISSN: 0021-9738 Impact factor: 14.808