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Publication : Dynamic pathological analysis reveals a protective role against skin fibrosis for TREM2-dependent macrophages.

First Author  Liang Y Year  2024
Journal  Theranostics Volume  14
Issue  5 Pages  2232-2245
PubMed ID  38505612 Mgi Jnum  J:346378
Mgi Id  MGI:7615747 Doi  10.7150/thno.94121
Citation  Liang Y, et al. (2024) Dynamic pathological analysis reveals a protective role against skin fibrosis for TREM2-dependent macrophages. Theranostics 14(5):2232-2245
abstractText  Rationale: Systemic sclerosis (SSc) is a chronic and incurable autoimmune disease with high mortality rates, and skin fibrosis is one of distinguishing hallmarks in the pathogenesis. However, macrophage heterogeneity regulating skin fibrosis remain largely unknown. Methods: We established mouse disease model and performed single-cell RNA-sequencing (scRNA-seq) to resolve the dynamic and heterogenous characteristics of macrophages in skin fibrosis, and the role of TREM2-dependent macrophages in the pathological process was investigated using knockout mice and intraperitoneal transferring TREM2(+) macrophages combining with functional assays. Results: We show that TREM2-expressing macrophages (TREM2(+) Mcapital EF, Cyrillics) accumulate in injured skin of mice treated by bleomycin (BLM) and human SSc, and their gene signatures and functional pathways are identified in the course of disease. Genetic ablation of Trem2 in mice globally accelerates and aggravates skin fibrosis, whereas transferring TREM2(hi) macrophages improves and alleviates skin fibrosis. Amazingly, we found that disease-associated TREM2(+) Mcapital EF, Cyrillics in skin fibrosis exhibit overlapping signatures with fetal skin counterparts in mice and human to maintain skin homeostasis, but each has merits in skin remodeling and development respectively. Conclusion: This study identifies that TREM2 acts as a functional molecule and a major signaling by which macrophage subpopulations play a protective role against fibrosis, and disease-associated TREM2(+) Mcapital EF, Cyrillics in skin fibrosis might undergo a fetal-like reprogramming similar to fetal skin counterparts.
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