Intestinal tuft cell subtypes represent successive stages of maturation driven by crypt-villus signaling gradients

Julian R. Buissant des Amorie; Max A. Betjes; Jochem H. Bernink; Joris H. Hageman; Veerle E. Geurts; Harry Begthel; Dimitrios Laskaris; Maria C. Heinz; Ingrid Jordens; Tiba Vinck; Ronja M. Houtekamer; Ingrid Verlaan-Klink; Sascha R. Brunner; Jacco van Rheenen; Martijn Gloerich; Hans Clevers; Sander J. Tans; Jeroen S. van Zon; Hugo J.G. Snippert

doi:10.1038/s41467-025-61878-9

Intestinal tuft cell subtypes represent successive stages of maturation driven by crypt-villus signaling gradients

Julian R. Buissant des Amorie
, Max A. Betjes
, Jochem H. Bernink
, Joris H. Hageman
, Veerle E. Geurts
, Harry Begthel
, Dimitrios Laskaris
, Maria C. Heinz
, Ingrid Jordens
, Tiba Vinck
, Ronja M. Houtekamer
, Ingrid Verlaan-Klink
, Sascha R. Brunner
, Jacco van Rheenen
, Martijn Gloerich
, Hans Clevers
, Sander J. Tans
, Jeroen S. van Zon
, Hugo J.G. Snippert

Research output: Contribution to journal › Article › peer-review

4 Citations (Scopus)

Abstract

Intestinal tuft cells are epithelial sentinels that trigger host defense upon detection of parasite-derived compounds. While they represent potent targets for immunomodulatory therapies in inflammation-driven intestinal diseases, their functioning and differentiation are poorly understood. Here, we reveal common intermediary transcriptomes among the previously described tuft-1 and tuft-2 subtypes in mouse and human. Tuft cell subtype-specific reporter knock-ins in organoids show that the two subtypes reflect successive post-mitotic maturation stages within the tuft cell lineage. In vitro stimulation with interleukin-4 and 13 is sufficient to fuel the generation of new Nrep+ tuft-1 cells, arising from tuft precursors (tuft-p). Subsequently, changes in crypt-villus signaling gradients, such as BMP, and cholinergic signaling, are required to advance maturation towards Chat+ tuft-2 phenotypes. Functionally, we find chemosensory capacity to increase during maturation. Our tuft subtype-specific reporters and optimized differentiation strategy in organoids provide a platform to study immune-related tuft cell subtypes and their unique chemosensory properties.

Original language	English
Article number	6765
Journal	Nature communications
Volume	16
Issue number	1
DOIs	https://doi.org/10.1038/s41467-025-61878-9
Publication status	Published - 22 Jul 2025

Keywords

Interleukin-4/pharmacology
Intestinal Mucosa/cytology
Epithelial Cells/metabolism
Signal Transduction
Tuft Cells
Humans
Mice, Inbred C57BL
Transcriptome
Interleukin-13/pharmacology
Cell Lineage
Animals
Mice
Cell Differentiation
Organoids/cytology

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10.1038/s41467-025-61878-9

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Buissant des Amorie, J. R., Betjes, M. A., Bernink, J. H., Hageman, J. H., Geurts, V. E., Begthel, H., Laskaris, D., Heinz, M. C., Jordens, I., Vinck, T., Houtekamer, R. M., Verlaan-Klink, I., Brunner, S. R., van Rheenen, J., Gloerich, M., Clevers, H., Tans, S. J., van Zon, J. S., & Snippert, H. J. G. (2025). Intestinal tuft cell subtypes represent successive stages of maturation driven by crypt-villus signaling gradients. Nature communications, 16(1), Article 6765. https://doi.org/10.1038/s41467-025-61878-9

@article{ad7c4e1d718b4397b52f00a1080ed50f,

title = "Intestinal tuft cell subtypes represent successive stages of maturation driven by crypt-villus signaling gradients",

abstract = "Intestinal tuft cells are epithelial sentinels that trigger host defense upon detection of parasite-derived compounds. While they represent potent targets for immunomodulatory therapies in inflammation-driven intestinal diseases, their functioning and differentiation are poorly understood. Here, we reveal common intermediary transcriptomes among the previously described tuft-1 and tuft-2 subtypes in mouse and human. Tuft cell subtype-specific reporter knock-ins in organoids show that the two subtypes reflect successive post-mitotic maturation stages within the tuft cell lineage. In vitro stimulation with interleukin-4 and 13 is sufficient to fuel the generation of new Nrep+ tuft-1 cells, arising from tuft precursors (tuft-p). Subsequently, changes in crypt-villus signaling gradients, such as BMP, and cholinergic signaling, are required to advance maturation towards Chat+ tuft-2 phenotypes. Functionally, we find chemosensory capacity to increase during maturation. Our tuft subtype-specific reporters and optimized differentiation strategy in organoids provide a platform to study immune-related tuft cell subtypes and their unique chemosensory properties.",

keywords = "Interleukin-4/pharmacology, Intestinal Mucosa/cytology, Epithelial Cells/metabolism, Signal Transduction, Tuft Cells, Humans, Mice, Inbred C57BL, Transcriptome, Interleukin-13/pharmacology, Cell Lineage, Animals, Mice, Cell Differentiation, Organoids/cytology",

author = "\{Buissant des Amorie\}, \{Julian R.\} and Betjes, \{Max A.\} and Bernink, \{Jochem H.\} and Hageman, \{Joris H.\} and Geurts, \{Veerle E.\} and Harry Begthel and Dimitrios Laskaris and Heinz, \{Maria C.\} and Ingrid Jordens and Tiba Vinck and Houtekamer, \{Ronja M.\} and Ingrid Verlaan-Klink and Brunner, \{Sascha R.\} and \{van Rheenen\}, Jacco and Martijn Gloerich and Hans Clevers and Tans, \{Sander J.\} and \{van Zon\}, \{Jeroen S.\} and Snippert, \{Hugo J.G.\}",

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year = "2025",

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doi = "10.1038/s41467-025-61878-9",

language = "English",

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Buissant des Amorie, JR, Betjes, MA, Bernink, JH, Hageman, JH, Geurts, VE, Begthel, H, Laskaris, D, Heinz, MC, Jordens, I, Vinck, T, Houtekamer, RM, Verlaan-Klink, I, Brunner, SR, van Rheenen, J, Gloerich, M, Clevers, H, Tans, SJ, van Zon, JS & Snippert, HJG 2025, 'Intestinal tuft cell subtypes represent successive stages of maturation driven by crypt-villus signaling gradients', Nature communications, vol. 16, no. 1, 6765. https://doi.org/10.1038/s41467-025-61878-9

TY - JOUR

T1 - Intestinal tuft cell subtypes represent successive stages of maturation driven by crypt-villus signaling gradients

AU - Buissant des Amorie, Julian R.

AU - Betjes, Max A.

AU - Bernink, Jochem H.

AU - Hageman, Joris H.

AU - Geurts, Veerle E.

AU - Begthel, Harry

AU - Laskaris, Dimitrios

AU - Heinz, Maria C.

AU - Jordens, Ingrid

AU - Vinck, Tiba

AU - Houtekamer, Ronja M.

AU - Verlaan-Klink, Ingrid

AU - Brunner, Sascha R.

AU - van Rheenen, Jacco

AU - Gloerich, Martijn

AU - Clevers, Hans

AU - Tans, Sander J.

AU - van Zon, Jeroen S.

AU - Snippert, Hugo J.G.

PY - 2025/7/22

Y1 - 2025/7/22

N2 - Intestinal tuft cells are epithelial sentinels that trigger host defense upon detection of parasite-derived compounds. While they represent potent targets for immunomodulatory therapies in inflammation-driven intestinal diseases, their functioning and differentiation are poorly understood. Here, we reveal common intermediary transcriptomes among the previously described tuft-1 and tuft-2 subtypes in mouse and human. Tuft cell subtype-specific reporter knock-ins in organoids show that the two subtypes reflect successive post-mitotic maturation stages within the tuft cell lineage. In vitro stimulation with interleukin-4 and 13 is sufficient to fuel the generation of new Nrep+ tuft-1 cells, arising from tuft precursors (tuft-p). Subsequently, changes in crypt-villus signaling gradients, such as BMP, and cholinergic signaling, are required to advance maturation towards Chat+ tuft-2 phenotypes. Functionally, we find chemosensory capacity to increase during maturation. Our tuft subtype-specific reporters and optimized differentiation strategy in organoids provide a platform to study immune-related tuft cell subtypes and their unique chemosensory properties.

AB - Intestinal tuft cells are epithelial sentinels that trigger host defense upon detection of parasite-derived compounds. While they represent potent targets for immunomodulatory therapies in inflammation-driven intestinal diseases, their functioning and differentiation are poorly understood. Here, we reveal common intermediary transcriptomes among the previously described tuft-1 and tuft-2 subtypes in mouse and human. Tuft cell subtype-specific reporter knock-ins in organoids show that the two subtypes reflect successive post-mitotic maturation stages within the tuft cell lineage. In vitro stimulation with interleukin-4 and 13 is sufficient to fuel the generation of new Nrep+ tuft-1 cells, arising from tuft precursors (tuft-p). Subsequently, changes in crypt-villus signaling gradients, such as BMP, and cholinergic signaling, are required to advance maturation towards Chat+ tuft-2 phenotypes. Functionally, we find chemosensory capacity to increase during maturation. Our tuft subtype-specific reporters and optimized differentiation strategy in organoids provide a platform to study immune-related tuft cell subtypes and their unique chemosensory properties.

KW - Interleukin-4/pharmacology

KW - Intestinal Mucosa/cytology

KW - Epithelial Cells/metabolism

KW - Signal Transduction

KW - Tuft Cells

KW - Humans

KW - Mice, Inbred C57BL

KW - Transcriptome

KW - Interleukin-13/pharmacology

KW - Cell Lineage

KW - Animals

KW - Mice

KW - Cell Differentiation

KW - Organoids/cytology

UR - https://www.scopus.com/pages/publications/105011251633

UR - https://www.mendeley.com/catalogue/cf3a6806-df62-3e4e-baa3-8d57617a3b76/

U2 - 10.1038/s41467-025-61878-9

DO - 10.1038/s41467-025-61878-9

M3 - Article

C2 - 40695798

AN - SCOPUS:105011251633

SN - 2041-1723

VL - 16

JO - Nature communications

JF - Nature communications

IS - 1

M1 - 6765

ER -

Intestinal tuft cell subtypes represent successive stages of maturation driven by crypt-villus signaling gradients

Abstract

Keywords

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