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腱鞘来源的祖细胞以空间依赖的方式驱动屈肌腱损伤后的纤维化和再生。

Epitenon-derived progenitors drive fibrosis and regeneration after flexor tendon injury in a spatially-dependent manner.

作者信息

Nichols Anne E C, Benoodt Lauren, Adjei-Sowah Emmanuella, Jerreld Kyle, Kollar Alexander, Ketonis Constantinos, Loiselle Alayna E

机构信息

Center for Musculoskeletal Research, Department of Orthopaedics & Rehabilitation, University of Rochester Medical Center, Rochester, NY, USA.

Genomics Research Center, University of Rochester School of Medicine and Dentistry, Rochester, NY, USA.

出版信息

Nat Commun. 2025 Jul 1;16(1):5448. doi: 10.1038/s41467-025-60704-6.

Abstract

Flexor tendon injuries are common and heal poorly owing to both the deposition of function-limiting peritendinous scar tissue and insufficient healing of the tendon itself. Therapeutic options are limited due to a lack of understanding of the cell populations that contribute to these processes. Here, we identified the epitenon as a major source of cells that contribute to both peritendinous fibrosis and regenerative tendon healing following acute tendon injury. Using a combination of genetic lineage tracing and single cell RNA-sequencing (scRNA-seq), we profiled the behavior and contributions of each cell fate to the healing process in a spatio-temporal manner. Integrated scRNA-seq analysis of mouse healing with human peritendinous scar tissue revealed remarkable transcriptional similarity between mouse epitenon-derived cells and fibroblasts present in human peritendinous scar tissue, which was further validated by immunofluorescent staining for conserved markers. Finally, ablation of pro-fibrotic epitenon-derived cells post-tendon injury significantly improved functional recovery. Combined, these results clearly identify the epitenon as the cellular origin of an important progenitor cell population that could be leveraged to improve tendon healing.

摘要

屈肌腱损伤很常见,由于功能受限的腱周瘢痕组织沉积以及肌腱本身愈合不足,愈合情况较差。由于对导致这些过程的细胞群体缺乏了解,治疗选择有限。在这里,我们确定腱外膜是急性肌腱损伤后导致腱周纤维化和肌腱再生愈合的主要细胞来源。通过基因谱系追踪和单细胞RNA测序(scRNA-seq)相结合的方法,我们以时空方式分析了每种细胞命运对愈合过程的行为和贡献。对小鼠愈合过程与人腱周瘢痕组织进行的综合scRNA-seq分析显示,小鼠腱外膜来源的细胞与人腱周瘢痕组织中的成纤维细胞之间存在显著的转录相似性,这通过对保守标志物的免疫荧光染色得到进一步验证。最后,在肌腱损伤后消融促纤维化的腱外膜来源细胞可显著改善功能恢复。综合来看,这些结果明确将腱外膜确定为一个重要祖细胞群体的细胞起源,利用该群体有望改善肌腱愈合。

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