Cross-tissue organization of the fibroblast lineage

成纤维细胞 生物 纤维化 细胞生物学 表型 转录组 癌症研究 细胞培养 病理 遗传学 基因表达 基因 医学
作者
Matthew B. Buechler,Rachana Pradhan,Akshay T. Krishnamurty,Christian Cox,Aslihan Karabacak Calviello,Amber W. Wang,Yeqing Angela Yang,Lucinda Tam,Roger Caothien,Merone Roose‐Girma,Zora Modrušan,Joseph R. Arron,Richard Bourgon,Sören Müller,Shannon J. Turley
出处
期刊:Nature [Springer Nature]
卷期号:593 (7860): 575-579 被引量:579
标识
DOI:10.1038/s41586-021-03549-5
摘要

Fibroblasts are non-haematopoietic structural cells that define the architecture of organs, support the homeostasis of tissue-resident cells and have key roles in fibrosis, cancer, autoimmunity and wound healing1. Recent studies have described fibroblast heterogeneity within individual tissues1. However, the field lacks a characterization of fibroblasts at single-cell resolution across tissues in healthy and diseased organs. Here we constructed fibroblast atlases by integrating single-cell transcriptomic data from about 230,000 fibroblasts across 17 tissues, 50 datasets, 11 disease states and 2 species. Mouse fibroblast atlases and a DptIRESCreERT2 knock-in mouse identified two universal fibroblast transcriptional subtypes across tissues. Our analysis suggests that these cells can serve as a reservoir that can yield specialized fibroblasts across a broad range of steady-state tissues and activated fibroblasts in disease. Comparison to an atlas of human fibroblasts from perturbed states showed that fibroblast transcriptional states are conserved between mice and humans, including universal fibroblasts and activated phenotypes associated with pathogenicity in human cancer, fibrosis, arthritis and inflammation. In summary, a cross-species and pan-tissue approach to transcriptomics at single-cell resolution has identified key organizing principles of the fibroblast lineage in health and disease. Single-cell and genetic tools are used to characterize the diversity of fibroblasts across healthy and perturbed tissues in mice and humans.
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