Spatially Restricted Immune and Microbiota-driven Adaptation of the Gut

Overview

Journal Nature

Specialty Science

Date 2024 Nov 20

PMID 39567686

Authors

Toufic Mayassi

Chenhao Li

Asa Segerstolpe

Eric M Brown

Rebecca Weisberg

Toru Nakata

Hiroshi Yano

Paula Herbst

David Artis

Daniel B Graham

Ramnik J Xavier

Affiliations

Soon will be listed here.

Abstract

The intestine is characterized by an environment in which host requirements for nutrient and water absorption are consequently paired with the requirements to establish tolerance to the outside environment. To better understand how the intestine functions in health and disease, large efforts have been made to characterize the identity and composition of cells from different intestinal regions. However, the robustness, nature of adaptability and extent of resilience of the transcriptional landscape and cellular underpinning of the intestine in space are still poorly understood. Here we generated an integrated resource of the spatial and cellular landscape of the murine intestine in the steady and perturbed states. Leveraging these data, we demonstrated that the spatial landscape of the intestine was robust to the influence of the microbiota and was adaptable in a spatially restricted manner. Deploying a model of spatiotemporal acute inflammation, we demonstrated that both robust and adaptable features of the landscape were resilient. Moreover, highlighting the physiological relevance and value of our dataset, we identified a region of the middle colon characterized by an immune-driven multicellular spatial adaptation of structural cells to the microbiota. Our results demonstrate that intestinal regionalization is characterized by robust and resilient structural cell states and that the intestine can adapt to environmental stress in a spatially controlled manner through the crosstalk between immunity and structural cell homeostasis.

Citing Articles

Cross-tissue multi-omics analyses reveal the gut microbiota's absence impacts organ morphology, immune homeostasis, bile acid and lipid metabolism.

Shen J, Liang W, Zhao R, Chen Y, Liu Y, Cheng W Imeta. 2025; 4(1):e272.

PMID: 40027481 PMC: 11865341. DOI: 10.1002/imt2.272.

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