组织工程与重建外科杂志 ›› 2025, Vol. 21 ›› Issue (2): 162-.

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先天性巨痣自发消退患者的单细胞测序分析

  

  • 出版日期:2025-04-01 发布日期:2025-05-13

Single-cell sequencing of spontaneous regressed giant congenital melanocytic nevus( GCMN)

  • Online:2025-04-01 Published:2025-05-13

摘要: 目的 探究先天性巨痣(GCMN)自发消退背后的细胞群更替和生物学行为。方法 对先天性巨痣患者的正 常组织、巨痣的颜色消退组织和未消退组织进行 10×单细胞测序。先量化原始数据的基因表达,再依次对数据进行降 维、聚类、分群和可视化,根据差异基因对细胞群进行注释,并对差异基因进行通路富集和可视化。最后进行组织学染 色验证。结果 GCMN中以黑色素细胞群占比最大。在组织消退过程中,黑色素细胞减少,角质细胞和成纤维细胞增 多。免疫细胞同时存在免疫激活和免疫抑制状态。消退组织中黑色素细胞同时表达角质细胞标志基因,成纤维细胞则 富集增殖和细胞外基质相关通路。免疫荧光染色发现可同时表达 SOX10和 Keratin的细胞,时序分析发现黑色素细胞 向角质细胞转变。结论 GCMN 消退过程是一种长期慢性炎症过程,该过程中黑色素细胞出现转化,从表皮层脱落。 成纤维细胞参与组织修复重建。

关键词: 先天性巨痣,  单细胞测序,  肿瘤微环境

Abstract: Objective To explore the cellular turnover and biological mechanisms underlying the spontaneous regression of giant congenital melanocytic nevus( GCMN). Methods 10× single-cell RNA sequencing was performed on normal skin, depigmented nevus, and non-regressed nevus from patients with spontaneous regressed GCMN. Raw data were first used to quantify gene expression, followed by dimensionality reduction, clustering, cell population identification, and visualization. Cell populations were annotated based on differentially expressed genes (DEGs), and pathway enrichment and visualization of DEGs were carried out. Finally, histological staining was performed for validation. Results  In GCMN, melanocytes constituted the largest proportion. During the regression process, the number of melanocytes decreased, while keratinocytes and fibroblasts increased. Immune cells exhibited a coexistence of both immune activation and suppression. In regressed tissues, melanocytes also expressed keratinocyte marker genes, while fibroblasts were enriched in pathways related to proliferation and extracellular matrix. Immunofluorescence staining revealed cells co-expressing SOX10 and Keratin, and pseudotime analysis indicated a transition of melanocytes into keratinocytes. Conclusion The regression of GCMN is a longterm chronic inflammatory process, during which melanocytes undergo transformation and detach from the epidermal layer. Fibroblasts contribute to tissue repair and reconstruction.

Key words: Giant congenital pigmented nevus,  Single-cell sequencing,  Tumor microenvironment