Author
Listed:
- Costanza Borrelli
(University of Zurich
Department of Biosystems Science and Engineering, ETH Zurich)
- Tomas Valenta
(University of Zurich
Institute of Molecular Genetics of the ASCR, v. v. i.)
- Kristina Handler
(Department of Biosystems Science and Engineering, ETH Zurich)
- Karelia Vélez
(Department of Biosystems Science and Engineering, ETH Zurich)
- Alessandra Gurtner
(University of Zurich)
- Giulia Moro
(University of Zurich)
- Atefeh Lafzi
(Department of Biosystems Science and Engineering, ETH Zurich)
- Laura de Vargas Roditi
(Department of Biosystems Science and Engineering, ETH Zurich)
- George Hausmann
(University of Zurich)
- Isabelle C. Arnold
(University of Zurich)
- Andreas E. Moor
(Department of Biosystems Science and Engineering, ETH Zurich)
- Konrad Basler
(University of Zurich)
Abstract
The homeostasis of the gut epithelium relies upon continuous renewal and proliferation of crypt-resident intestinal epithelial stem cells (IESCs). Wnt/β-catenin signaling is required for IESC maintenance, however, it remains unclear how this pathway selectively governs the identity and proliferative decisions of IESCs. Here, we took advantage of knock-in mice harboring transgenic β-catenin alleles with mutations that specifically impair the recruitment of N- or C-terminal transcriptional co-factors. We show that C-terminally-recruited transcriptional co-factors of β-catenin act as all-or-nothing regulators of Wnt-target gene expression. Blocking their interactions with β-catenin rapidly induces loss of IESCs and intestinal homeostasis. Conversely, N-terminally recruited co-factors fine-tune β-catenin’s transcriptional output to ensure proper self-renewal and proliferative behaviour of IESCs. Impairment of N-terminal interactions triggers transient hyperproliferation of IESCs, eventually resulting in exhaustion of the self-renewing stem cell pool. IESC mis-differentiation, accompanied by unfolded protein response stress and immune infiltration, results in a process resembling aberrant “villisation” of intestinal crypts. Our data suggest that IESC-specific Wnt/β-catenin output requires selective modulation of gene expression by transcriptional co-factors.
Suggested Citation
Costanza Borrelli & Tomas Valenta & Kristina Handler & Karelia Vélez & Alessandra Gurtner & Giulia Moro & Atefeh Lafzi & Laura de Vargas Roditi & George Hausmann & Isabelle C. Arnold & Andreas E. Moor, 2021.
"Differential regulation of β-catenin-mediated transcription via N- and C-terminal co-factors governs identity of murine intestinal epithelial stem cells,"
Nature Communications, Nature, vol. 12(1), pages 1-16, December.
Handle:
RePEc:nat:natcom:v:12:y:2021:i:1:d:10.1038_s41467-021-21591-9
DOI: 10.1038/s41467-021-21591-9
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