A coordinated cellular network regulates tolerance to food

Anna Rudnitsky; Hanna Oh; Maya Margolin; Bareket Dassa; Inbar Shteinberg; Liat Stoler-Barak; Ziv Shulman; Ranit Kedmi

doi:10.1038/s41586-025-09173-x

^*Corresponding author for this work

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Abstract

To absorb nutrients and support commensal microorganisms, the host induces tolerogenic immune responses through peripheral regulatory T (pT_reg) cells^1,2. Previous studies identified conventional type 1 dendritic cells (cDC1s) as initiators of dietary pT_reg cells³. However, here we report that food-specific pT_reg cells are induced exclusively by the recently identified RORγt antigen-presenting cells^{4, 5, 6, 7–8} and not by conventional dendritic cells. Instead, our data suggest that pT_reg cell–cDC1 interactions during homeostasis limit the expansion of food-specific CD8αβ T cells. This regulation is disrupted by infection or food poisoning, enabling dietary CD8αβ T cells to expand and acquire effector functions in response to mimicked food antigens. Unlike in typical infections, after the pathogen is cleared, dietary CD8αβ T cells do not expand in response to their corresponding dietary antigens. Thus, we propose that, in response to dietary antigens, tolerance is mediated by a circuit of dedicated antigen-presenting cells and T cells. When the host is challenged by infection, this circuit permits the transient expansion of protective effector responses without compromising the overall strategy of tolerance that ensures safe food consumption.

Original language	English
Pages (from-to)	231-240
Number of pages	10
Journal	Nature
Volume	644
Issue number	8075
DOIs	https://doi.org/10.1038/s41586-025-09173-x
Publication status	Published Online - 27 May 2025

Funding

We thank members of the Kedmi laboratory, D. R. Littman, J. M. Gardner, J. Talbot, K. R. Mesa, O. J. Harrison and S. Naik for valuable discussion and critical reading of the manuscript; R. Dahan and T. Kaisho for sharing mice strains; staff at the Weizmann transgenic core unit for rederivation of mutant mice; and M. Kedmi for her support in generating the scRNA-seq data. R.K. is supported by European Research Council (ERC) grant no. 101164050. This work was also supported by the Abisch-Frenkel RNA Therapeutics Center and by a research grant from the Weizmann SABRA—Yeda-Sela—WRC Program, the Estate of Emile Mimran and The Maurice and Vivienne Wohl Biology Endowment.

All Science Journal Classification (ASJC) codes

General

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rk_Nature_ACoordinatedCellularNetwork_PV2025Final published version, 10.1 MBLicence: CC BY-NC-ND

Cite this

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title = "A coordinated cellular network regulates tolerance to food",

abstract = "To absorb nutrients and support commensal microorganisms, the host induces tolerogenic immune responses through peripheral regulatory T (pTreg) cells1,2. Previous studies identified conventional type 1 dendritic cells (cDC1s) as initiators of dietary pTreg cells3. However, here we report that food-specific pTreg cells are induced exclusively by the recently identified RORγt antigen-presenting cells4, 5, 6, 7–8 and not by conventional dendritic cells. Instead, our data suggest that pTreg cell–cDC1 interactions during homeostasis limit the expansion of food-specific CD8αβ T cells. This regulation is disrupted by infection or food poisoning, enabling dietary CD8αβ T cells to expand and acquire effector functions in response to mimicked food antigens. Unlike in typical infections, after the pathogen is cleared, dietary CD8αβ T cells do not expand in response to their corresponding dietary antigens. Thus, we propose that, in response to dietary antigens, tolerance is mediated by a circuit of dedicated antigen-presenting cells and T cells. When the host is challenged by infection, this circuit permits the transient expansion of protective effector responses without compromising the overall strategy of tolerance that ensures safe food consumption.",

author = "Anna Rudnitsky and Hanna Oh and Maya Margolin and Bareket Dassa and Inbar Shteinberg and Liat Stoler-Barak and Ziv Shulman and Ranit Kedmi",

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AU - Margolin, Maya

AU - Dassa, Bareket

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AU - Stoler-Barak, Liat

AU - Shulman, Ziv

AU - Kedmi, Ranit

PY - 2025/5/27

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N2 - To absorb nutrients and support commensal microorganisms, the host induces tolerogenic immune responses through peripheral regulatory T (pTreg) cells1,2. Previous studies identified conventional type 1 dendritic cells (cDC1s) as initiators of dietary pTreg cells3. However, here we report that food-specific pTreg cells are induced exclusively by the recently identified RORγt antigen-presenting cells4, 5, 6, 7–8 and not by conventional dendritic cells. Instead, our data suggest that pTreg cell–cDC1 interactions during homeostasis limit the expansion of food-specific CD8αβ T cells. This regulation is disrupted by infection or food poisoning, enabling dietary CD8αβ T cells to expand and acquire effector functions in response to mimicked food antigens. Unlike in typical infections, after the pathogen is cleared, dietary CD8αβ T cells do not expand in response to their corresponding dietary antigens. Thus, we propose that, in response to dietary antigens, tolerance is mediated by a circuit of dedicated antigen-presenting cells and T cells. When the host is challenged by infection, this circuit permits the transient expansion of protective effector responses without compromising the overall strategy of tolerance that ensures safe food consumption.

AB - To absorb nutrients and support commensal microorganisms, the host induces tolerogenic immune responses through peripheral regulatory T (pTreg) cells1,2. Previous studies identified conventional type 1 dendritic cells (cDC1s) as initiators of dietary pTreg cells3. However, here we report that food-specific pTreg cells are induced exclusively by the recently identified RORγt antigen-presenting cells4, 5, 6, 7–8 and not by conventional dendritic cells. Instead, our data suggest that pTreg cell–cDC1 interactions during homeostasis limit the expansion of food-specific CD8αβ T cells. This regulation is disrupted by infection or food poisoning, enabling dietary CD8αβ T cells to expand and acquire effector functions in response to mimicked food antigens. Unlike in typical infections, after the pathogen is cleared, dietary CD8αβ T cells do not expand in response to their corresponding dietary antigens. Thus, we propose that, in response to dietary antigens, tolerance is mediated by a circuit of dedicated antigen-presenting cells and T cells. When the host is challenged by infection, this circuit permits the transient expansion of protective effector responses without compromising the overall strategy of tolerance that ensures safe food consumption.

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