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悬浮驯化人基质干细胞(S-hMSCs)用于可扩展制造细胞外囊泡。

Generating suspension-adapted human mesenchymal stromal cells (S-hMSCs) for the scalable manufacture of extracellular vesicles.

机构信息

Department of Biochemical Engineering, Advanced Centre for Biochemical Engineering, University College London, London, UK.

Kendall Innovations, Cambridge, Massachusetts, USA.

出版信息

Cytotherapy. 2024 Dec;26(12):1532-1546. doi: 10.1016/j.jcyt.2024.06.011. Epub 2024 Jul 3.

DOI:10.1016/j.jcyt.2024.06.011
PMID:39269403
Abstract

BACKGROUD

Human mesenchymal stromal cells (hMSCs) are a naturally adherent cell type and one of the most studied cellular agents used in cell therapy over the last 20 years. Their mechanism of action has been primarily associated with paracrine signaling, which has contributed to an increase in the number of studies focused on hMSC-related extracellular vesicles (EVs).

METHODS

In this study, we demonstrate for the first time that human telomerase reverse transcriptase (hTERT) immortalized hMSCs can be adapted to suspension culture, eliminating the need for microcarriers or other matrixes to support cell growth.

RESULTS

This novel cell line, named suspension hMSCs (S-hMSCs), has a doubling time of approximately 55 hours, with a growth rate of 0.423/d. Regarding its immunophenotype characteristics, S-hMSCs retained close to 90% of CD73 and CD105 expression levels, with the CD90 receptor being downregulated during the adherent to suspension adaptation process. An RNA sequencing analysis showed an upregulation of the transcripts coding for CD44, CD46 and CD47 compared to the expression levels in AT-hMSCs and hTERT-hMSCs. The cell line herein established was able to generate EVs using a chemically defined medium formulation with these nanoparticles averaging 150 nm in size and displaying the markers CD63, CD81, and TSG101, while not expressing the negative marker calnexin.

CONCLUSION

This body of evidence, combined with the visual confirmation of EV presence using transmission electron microscopy, demonstrates the EV-producing capabilities of the novel S-hMSCs. This cell line provides a platform for process development, drug discovery and translational studies in the EV field.

摘要

背景

人类间充质基质细胞(hMSCs)是一种天然贴壁细胞类型,也是过去 20 年来细胞治疗中研究最多的细胞制剂之一。其作用机制主要与旁分泌信号有关,这促使越来越多的研究集中在与 hMSC 相关的细胞外囊泡(EVs)上。

方法

在这项研究中,我们首次证明人类端粒酶逆转录酶(hTERT)永生化 hMSCs 可以适应悬浮培养,从而无需使用微载体或其他基质来支持细胞生长。

结果

这种新型细胞系,命名为悬浮 hMSCs(S-hMSCs),倍增时间约为 55 小时,生长速度为 0.423/d。关于其免疫表型特征,S-hMSCs 保持了接近 90%的 CD73 和 CD105 表达水平,而 CD90 受体在从贴壁到悬浮适应过程中下调。RNA 测序分析显示,与 AT-hMSCs 和 hTERT-hMSCs 的表达水平相比,编码 CD44、CD46 和 CD47 的转录物上调。在此建立的细胞系能够使用化学定义的培养基配方生成 EVs,这些纳米颗粒平均大小为 150nm,并显示出 CD63、CD81 和 TSG101 等标记物,而不表达阴性标记物 calnexin。

结论

这些证据表明,新型 S-hMSCs 具有产生 EV 的能力,结合使用透射电子显微镜对 EV 存在的直观确认。该细胞系为 EV 领域的工艺开发、药物发现和转化研究提供了平台。

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