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内皮细胞直接重编程:过去、现在和未来。

Endothelial cell direct reprogramming: Past, present, and future.

机构信息

Division of Cardiology, Department of Medicine, Emory University School of Medicine, Atlanta, GA, USA.

Division of Cardiology, Department of Medicine, Emory University School of Medicine, Atlanta, GA, USA.

出版信息

J Mol Cell Cardiol. 2023 Jul;180:22-32. doi: 10.1016/j.yjmcc.2023.04.006. Epub 2023 Apr 18.

DOI:10.1016/j.yjmcc.2023.04.006
PMID:37080451
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10330356/
Abstract

Ischemic cardiovascular disease still remains as a leading cause of morbidity and mortality despite various medical, surgical, and interventional therapy. As such, cell therapy has emerged as an attractive option because it tackles underlying problem of the diseases by inducing neovascularization in ischemic tissue. After overall failure of adult stem or progenitor cells, studies attempted to generate endothelial cells (ECs) from pluripotent stem cells (PSCs). While endothelial cells (ECs) differentiated from PSCs successfully induced vascular regeneration, differentiating volatility and tumorigenic potential is a concern for their clinical applications. Alternatively, direct reprogramming strategies employ lineage-specific factors to change cell fate without achieving pluripotency. ECs have been successfully reprogrammed via ectopic expression of transcription factors (TFs) from endothelial lineage. The reprogrammed ECs induced neovascularization in vitro and in vivo and thus demonstrated their therapeutic value in animal models of vascular insufficiency. Methods of delivering reprogramming factors include lentiviral or retroviral vectors and more clinically relevant, non-integrative adenoviral and episomal vectors. Most studies made use of fibroblast as a source cell for reprogramming, but reprogrammability of other clinically relevant source cell types has to be evaluated. Specific mechanisms and small molecules that are involved in the aforementioned processes tackles challenges associated with direct reprogramming efficiency and maintenance of reprogrammed EC characteristics. After all, this review provides summary of past and contemporary methods of direct endothelial reprogramming and discusses the future direction to overcome these challenges to acquire clinically applicable reprogrammed ECs.

摘要

尽管有各种医学、外科和介入治疗方法,缺血性心血管疾病仍然是发病率和死亡率的主要原因。因此,细胞疗法作为一种有吸引力的选择出现了,因为它通过在缺血组织中诱导新血管生成来解决疾病的根本问题。在成年干细胞或祖细胞整体失败后,研究试图从多能干细胞 (PSC) 中产生内皮细胞 (EC)。虽然源自 PSC 的内皮细胞 (EC) 成功地诱导了血管再生,但分化的不稳定性和致瘤潜能是其临床应用的一个关注点。相反,直接重编程策略利用谱系特异性因子在不达到多能性的情况下改变细胞命运。已经通过异位表达内皮谱系中的转录因子 (TF) 成功地对 EC 进行了重编程。重编程的 EC 在体外和体内诱导了新血管生成,从而在血管功能不全的动物模型中证明了它们的治疗价值。递送重编程因子的方法包括慢病毒或逆转录病毒载体,以及更具临床相关性的非整合腺病毒和附加体载体。大多数研究都利用成纤维细胞作为重编程的源细胞,但必须评估其他临床相关源细胞类型的重编程能力。涉及上述过程的特定机制和小分子解决了与直接重编程效率和维持重编程 EC 特征相关的挑战。总之,本综述提供了直接内皮重编程过去和当代方法的总结,并讨论了克服这些挑战以获得临床适用的重编程 EC 的未来方向。

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