Monocyte-macrophage spatial dynamics promote pre-crown-like niches in early obesity

crossref(2022)

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AbstractObjectiveObesity drives significant changes in adipose tissue that precede development of tissue and systemic insulin resistance. Immune cell infiltration and inflammation are known contributors to these changes but there is limited understanding of their spatial context tissue-wide. We sought to identify spatial patterning in epididymal adipose tissue immune cells in a time course of diet-induced obesity in mice.MethodsUsing spatial transcriptomics and single-cell RNA-sequencing, we identified dominant cell type signatures preserved in their anatomical context, quantified gene expression patterns at spots throughout adipose tissue, performed cell type network analysis, and investigated ligand-receptor colocalization.ResultsOur data support increased innate immune cells, including macrophages, monocytes, and innate lymphoid cells with tissue-wide interspersion, and dampened adaptive immune cell signatures with obesity. Network analysis identified increased heterogeneity in all major immune cell types, consistent with increased subtypes. To capture tissue dynamics at obesity onset, we draw on mathematical principles from linear algebra and spectral graph theory and provide a framework for better understanding cell cooperation toward emergence of multicellular tissue function. Ligand receptor analysis in spatial tran-scriptomics data at 8 and 14 weeks of high fat diet feeding shows colocalization of monocyte-macrophage ligand receptor expression consistent with increased crosstalk in obesity. Furthermore, we identify in spatial data crown-like structure neighborhoods and pre-crown-like niches, which are enriched in ligand receptor pairs that suggest monocyte-driven signaling to macrophages in early obesity.ConclusionThe culmination of these analyses revealed a widespread paradigm shift in ligand-receptor activity with near-exclusive macrophage-macrophage or monocyte-macrophage interactions at crown-like structures across adipose tissue in early obesity.HighlightsSpatial transcriptomics shows innate immune cell dominance in obese adipose tissueIncreased monocyte signaling accompanies infiltration in obesityPre-crown-like niches precede crown-like structure formationInfluential monocyte-macrophage ligand-receptor pairs emerge at crown-like niches
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