Immunological mechanisms underlying fibrotic diseases via single-cell technologies
Yuzo Koda, Nobuhiro Nakamoto, Takanori Kanai

TL;DR
This review explores how immune cells contribute to fibrosis and how single-cell technologies help understand and treat this condition.
Contribution
The paper introduces novel strategies for fibrosis treatment using recent advancements in single-cell analysis.
Findings
Immune cells play a role in both the progression and resolution of fibrotic diseases.
Single-cell technologies enable precise analysis of cell phenotypes and interactions in fibrosis.
Integration of multi-omics data reveals key interactions between immune and parenchymal cells.
Abstract
Fibrosis is an organ dysfunction caused by excessive deposition of fibrous components produced by parenchymal cells. Effective treatments are lacking for this progressive pathological condition that manifests in various organs and can lead to mortality. The involvement of the immune system in various aspects of fibrosis development, including chronic organ damage induced by macrophages and T cells, wound healing by macrophages and growth factors such as TGF-β, and polarization toward the type II cytokine phenotype, has been widely reported. Recently, immune cells were also reported to contribute to the resolution phase of fibrotic conditions, highlighting the relevance of immune cell analysis in the understanding of both progression and recovery of fibrotic pathologies. However, owing to the complexity and diversity of disease progression, conventional pathological analyses that focus…
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Taxonomy
TopicsInterstitial Lung Diseases and Idiopathic Pulmonary Fibrosis · Single-cell and spatial transcriptomics · IL-33, ST2, and ILC Pathways
