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永生化Lin-Sca-1+心脏祖细胞在长期培养中的稳定表型和功能:向标准化迈进了一步。

Stable phenotype and function of immortalized Lin-Sca-1+ cardiac progenitor cells in long-term culture: a step closer to standardization.

作者信息

Freire Ana G, Nascimento Diana S, Forte Giancarlo, Valente Mariana, Resende Tatiana P, Pagliari Stefania, Abreu Cláudia, Carvalho Isabel, Di Nardo Paolo, Pinto-do-Ó Perpétua

机构信息

1 INEB-Instituto de Engenharia Biomédica, Universidade do Porto , Porto, Portugal .

出版信息

Stem Cells Dev. 2014 May 1;23(9):1012-26. doi: 10.1089/scd.2013.0305. Epub 2014 Feb 14.

DOI:10.1089/scd.2013.0305
PMID:24367889
Abstract

Putative cardiac progenitor cells (CPCs) have been identified in the myocardium and are regarded as promising candidates for cardiac cell-based therapies. Although two distinct populations of CPCs reached the clinical setting, more detailed studies are required to portray the optimal cell type and therapeutic setting to drive robust cell engraftment and cardiomyogenesis after injury. Owing to the scarcity of the CPCs and the need for reproducibility, the generation of faithful cellular models would facilitate this scrutiny. Here, we evaluate whether immortalized Lin(-)Sca-1(+) CPCs (iCPC(Sca-1)) represent their native-cell counterpart, thereby constituting a robust in vitro model system for standardized investigation in the cardiac field. iCPC(Sca-1) were established in vitro as plastic adherent cells endowed with robust self-renewal capacity while preserving a stable phenotype in long-term culture. iCPC(Sca-1) differentiated into cardiomyocytic-, endothelial-, and smooth muscle-like cells when subjected to appropriate stimuli. The cell line consistently displayed features of Lin(-)Sca-1(+) CPCs in vitro, as well as in vivo after intramyocardial delivery in the onset of myocardial infarction (MI). Transplanted iCPC(Sca-1) significantly attenuated the functional and anatomical alterations caused by MI while promoting neovascularization. iCPC(Sca-1) are further shown to engraft, establish functional connections, and differentiate in loco into cardiomyocyte- and vasculature-like cells. These data validate iCPC(Sca-1) as an in vitro model system for Lin(-)Sca-1(+) progenitors and for systematic dissection of mechanisms underlying CPC subsets engraftment/differentiation in vivo. Moreover, iCPC(Sca-1) can be regarded as a ready-to-use CPCs source for pre-clinical bioengineering studies toward the development of novel strategies for restoration of the damaged myocardium.

摘要

在心肌中已鉴定出推定的心脏祖细胞(CPC),它们被视为基于细胞的心脏治疗的有前景的候选者。尽管有两种不同类型的CPC进入了临床应用阶段,但仍需要更详细的研究来描绘最佳的细胞类型和治疗方案,以促使损伤后细胞有力地植入并发生心肌生成。由于CPC数量稀少且需要可重复性,因此建立可靠的细胞模型将有助于这种详细研究。在这里,我们评估永生化的Lin(-)Sca-1(+) CPC(iCPC(Sca-1))是否代表其天然细胞对应物,从而构成一个强大的体外模型系统,用于心脏领域的标准化研究。iCPC(Sca-1)在体外被建立为具有强大自我更新能力的贴壁细胞,同时在长期培养中保持稳定的表型。当受到适当刺激时,iCPC(Sca-1)可分化为心肌样、内皮样和平滑肌样细胞。该细胞系在体外以及在心肌梗死(MI)发作时心肌内注射后在体内均始终表现出Lin(-)Sca-1(+) CPC的特征。移植的iCPC(Sca-1)显著减轻了MI引起的功能和解剖学改变,同时促进了新血管形成。进一步表明,iCPC(Sca-1)能够植入、建立功能连接并在局部分化为心肌样和血管样细胞。这些数据验证了iCPC(Sca-1)作为Lin(-)Sca-1(+)祖细胞的体外模型系统,以及用于系统剖析体内CPC亚群植入/分化机制的有效性。此外,iCPC(Sca-1)可被视为一种现成的CPC来源,用于临床前生物工程研究,以开发修复受损心肌的新策略。

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