Macrophages upregulate mural cell-like markers and support healing of ischemic injury by adopting functions important for vascular support

IF 9.4 Q1 CARDIAC & CARDIOVASCULAR SYSTEMS
Catarina Amoedo-Leite, Kristel Parv, Chiara Testini, Carmen Herrera-Hidalgo, Feifei Xu, Antoine Giraud, Marta Malaquias, Erik Fasterius, Daniel Holl, Cedric Seignez, Christian Göritz, Gustaf Christoffersson, Mia Phillipson
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Abstract

Sterile inflammation after injury is important for tissue restoration. In injured human and mouse tissues, macrophages were recently found to accumulate perivascularly. This study investigates if macrophages adopt a mural cell phenotype important for restoration after ischemic injury. Single-cell RNA sequencing of fate-mapped macrophages from ischemic mouse muscles demonstrates a macrophage-toward-mural cell switch of a subpopulation of macrophages with downregulated myeloid cell genes and upregulated mural cell genes, including PDGFRβ. This observation was further strengthened when including unspliced transcripts in the analysis. The macrophage switch was proven functionally relevant, as induction of macrophage-specific PDGFRβ deficiency prevented their perivascular macrophage phenotype, impaired vessel maturation and increased vessel leakiness, which ultimately reduced limb function. In conclusion, macrophages in adult ischemic tissue were demonstrated to undergo a cellular program to morphologically, transcriptomically and functionally resemble mural cells while weakening their macrophage identity. The macrophage-to-mural cell-like phenotypic switch is crucial for restoring tissue function and warrants further exploration as a potential target for immunotherapies to enhance healing. Amoedo-Leite et al. report that, in ischemic tissue, a subset of macrophages adopts mural cell-like morphology, gene expression and function, which is crucial for injury healing.

Abstract Image

巨噬细胞上调壁细胞样标志物,并通过承担对血管支持很重要的功能来支持缺血性损伤的愈合
损伤后的无菌炎症对组织恢复非常重要。最近发现,在受伤的人类和小鼠组织中,巨噬细胞在血管周围聚集。本研究探讨了巨噬细胞是否具有对缺血性损伤后的恢复非常重要的壁细胞表型。对缺血小鼠肌肉中命运图谱巨噬细胞的单细胞 RNA 测序表明,巨噬细胞亚群的髓细胞基因下调,而壁细胞基因(包括 PDGFRβ)上调,巨噬细胞向壁细胞转换。将未剪接的转录本纳入分析后,这一观察结果得到了进一步加强。巨噬细胞的转换被证明与功能相关,因为诱导巨噬细胞特异性 PDGFRβ 缺乏症可阻止其血管周围巨噬细胞表型,损害血管成熟并增加血管渗漏,最终降低肢体功能。总之,成人缺血组织中的巨噬细胞被证明经历了一个细胞程序,在形态学、转录组学和功能上与壁细胞相似,同时削弱了其巨噬细胞身份。巨噬细胞到壁细胞样表型的转换对恢复组织功能至关重要,值得进一步探索,以作为加强愈合的免疫疗法的潜在靶点。Amoedo-Leite 等人报告说,在缺血组织中,巨噬细胞的一个亚群采用壁细胞样形态、基因表达和功能,这对损伤愈合至关重要。
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CiteScore
5.70
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