Single-nucleus and spatial transcriptomics reveal intestinal cellular heterogeneity, differentiation, and cell communication mechanisms in SAP-induced intestinal injury

Key Points

Impaired epithelial regeneration is associated with altered cell communication in intestinal injury.
Epithelial immune interactions and ECM-centered FN1 signaling were identified as crucial factors.
Observational analysis reveals spatially organized remodeling in the ileum during SAP-induced damage.
These findings highlight potential pathways for future studies on intestinal repair mechanisms.

Abstract

Integrated single-nucleus and spatial transcriptomics reveal that SAP is accompanied by spatially organized ileal remodeling, epithelial immune-interacting rewiring, and altered neighborhood architecture, together with an ECM-centered FN1 signaling axis and attenuated Hmga2/Myb-associated regulatory programs in stem compartments. These findings provide a spatially informed cellular framework and generate testable hypotheses for mechanisms underlying impaired epithelial regeneration during SAP-associated intestinal injury.

Single-nucleus and spatial transcriptomics reveal intestinal cellular heterogeneity, differentiation, and cell communication mechanisms in SAP-induced intestinal injury

Key Points

Abstract

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