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单细胞转录组谱分析揭示了人类脐带组织和培养扩增的间充质干细胞中的分子异质性。

Single-cell transcriptome profiling reveals molecular heterogeneity in human umbilical cord tissue and culture-expanded mesenchymal stem cells.

机构信息

BGI Education Center, University of Chinese Academy of Sciences, Shenzhen, China.

BGI-Shenzhen, China.

出版信息

FEBS J. 2021 Sep;288(18):5311-5330. doi: 10.1111/febs.15834. Epub 2021 May 11.

Abstract

Human umbilical cord-derived mesenchymal stem/stromal cells (UMSCs) demonstrate great therapeutic potential in regenerative medicine. The use of UMSCs for clinical applications requires high quantity and good quality of cells usually by in vitro expansion. However, the heterogeneity and the characteristics of cultured UMSCs and the cognate human umbilical cord tissue at single-cell resolution remain poorly defined. In this study, we created a single-cell transcriptome profile of human umbilical cord tissue and the cognate culture-expanded UMSCs. Based on the inferred characteristics of cell clusters and trajectory analysis, we identified three subgroups in culture-expanded UMSCs and putative novel transcription factors (TFs) in regulating UMSC state transition. Further, putative ligand-receptor interaction analysis demonstrated that cellular interactions most frequently occurred in epithelial-like cells with other cell groups in umbilical cord tissue. Moreover, we dissected the transcriptomic differences of in vitro and in vivo subgroups and inferred the telomere-related molecules and pathways that might be activated in UMSCs for cell expansion in vitro. Our study provides a comprehensive and integrative study of the transcriptomics of human umbilical cord tissue and their cognate-cultured counterparts, which paves the way for a deeper understanding of cellular heterogeneity and offers fundamental biological insight of UMSCs-based cell therapy.

摘要

人脐带间充质干细胞(UMSC)在再生医学中具有巨大的治疗潜力。UMSC 用于临床应用需要大量高质量的细胞,通常通过体外扩增来实现。然而,培养的 UMSC 和同源人脐带组织的异质性和特征在单细胞分辨率下仍然定义不明确。在这项研究中,我们创建了人脐带组织和同源培养扩增的 UMSC 的单细胞转录组图谱。基于推断的细胞簇特征和轨迹分析,我们在培养扩增的 UMSC 中鉴定出三个亚群,并确定了调节 UMSC 状态转变的潜在新型转录因子(TFs)。此外,推测的配体-受体相互作用分析表明,细胞间相互作用最常发生在与脐带组织中其他细胞群类似上皮样细胞的细胞中。此外,我们剖析了体外和体内亚群的转录组差异,并推断了在体外细胞扩增中可能被激活的与端粒相关的分子和途径。我们的研究提供了人脐带组织及其同源培养物的转录组的全面综合研究,为深入了解细胞异质性铺平了道路,并为基于 UMSC 的细胞治疗提供了基本的生物学见解。

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