| Literature DB >> 32396863 |
Clara Morral1, Jelena Stanisavljevic1, Xavier Hernando-Momblona2, Elisabetta Mereu3, Adrián Álvarez-Varela2, Carme Cortina2, Diana Stork1, Felipe Slebe1, Gemma Turon1, Gavin Whissell1, Marta Sevillano2, Anna Merlos-Suárez1, Àngela Casanova-Martí1, Catia Moutinho3, Scott W Lowe4, Lukas E Dow5, Alberto Villanueva6, Elena Sancho2, Holger Heyn7, Eduard Batlle8.
Abstract
Colorectal cancers (CRCs) are composed of an amalgam of cells with distinct genotypes and phenotypes. Here, we reveal a previously unappreciated heterogeneity in the biosynthetic capacities of CRC cells. We discover that the majority of ribosomal DNA transcription and protein synthesis in CRCs occurs in a limited subset of tumor cells that localize in defined niches. The rest of the tumor cells undergo an irreversible loss of their biosynthetic capacities as a consequence of differentiation. Cancer cells within the biosynthetic domains are characterized by elevated levels of the RNA polymerase I subunit A (POLR1A). Genetic ablation of POLR1A-high cell population imposes an irreversible growth arrest on CRCs. We show that elevated biosynthesis defines stemness in both LGR5+ and LGR5- tumor cells. Therefore, a common architecture in CRCs is a simple cell hierarchy based on the differential capacity to transcribe ribosomal DNA and synthesize proteins.Entities:
Keywords: CRC; Cancer Stem Cell; biosynthetic capacity; plasticity; stem cell hierarchy
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Year: 2020 PMID: 32396863 PMCID: PMC9006079 DOI: 10.1016/j.stem.2020.04.012
Source DB: PubMed Journal: Cell Stem Cell ISSN: 1875-9777 Impact factor: 24.633