Mature tuft cell phenotypes are sequentially expressed along the intestinal crypt-villus axis following cytokine-induced tuft cell hyperplasia

Julian R. Buissant des Amorie(University Medical Center Utrecht), Max A. Betjes(Institute for Atomic and Molecular Physics), Jochem H. Bernink(Royal Netherlands Academy of Arts and Sciences), Joris H. Hageman(University Medical Center Utrecht), Maria C. Heinz(University Medical Center Utrecht), Ingrid Jordens(University Medical Center Utrecht), Tiba Vinck(University Medical Center Utrecht), Ronja M. Houtekamer(University Medical Center Utrecht), Ingrid Verlaan-Klink(University Medical Center Utrecht), Sascha R. Brunner(University Medical Center Utrecht), Dimitrios Laskaris(The Netherlands Cancer Institute), Jacco van Rheenen(The Netherlands Cancer Institute), Martijn Gloerich(University Medical Center Utrecht), Hans Clevers(Royal Netherlands Academy of Arts and Sciences), Jeroen S. van Zon(Institute for Atomic and Molecular Physics), Sander J. Tans(Institute for Atomic and Molecular Physics), Hugo J.G. Snippert(University Medical Center Utrecht)
bioRxiv (Cold Spring Harbor Laboratory)
November 29, 2024
Cited by 2Open Access
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Abstract

Intestinal tuft cells are epithelial sentinels that trigger host defense upon detection of parasite-derived compounds. While representing interesting targets for immunomodulatory therapies in inflammation-driven intestinal diseases, their detailed functioning is poorly understood. Although two distinct intestinal tuft cell types have been described, we reveal common intermediary transcriptomes among tuft cells in mouse and human. Tuft cell-specific reporter knock-ins in organoids show that the two tuft types are sequentially expressed transcriptomic states that represent different maturation stages. Moreover, cytokines interleukin-4 and interleukin-13 only induce lineage specification to Nrep + tuft-1 cells, while BMP and cholinergic signalling advance differentiation towards immune-related ChAT + tuft-2 phenotypes. Functionally, both tuft cell states have chemosensory capacity and respond to stimuli like succinate, but reaction probability increases during tuft cell maturation. Our tuft type-specific reporters and optimized differentiation strategy in organoids provide an experimental platform to study the functioning of tuft cells and their unique chemosensory properties.


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