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分离和鉴定人胚干细胞源性心前体细胞特异性心肌细胞,揭示了其在转录和电生理特征方面的新见解。

Isolation and characterization of human embryonic stem cell-derived heart field-specific cardiomyocytes unravels new insights into their transcriptional and electrophysiological profiles.

机构信息

Division of Cardiology, Department of Internal Medicine, David Geffen School of Medicine, University of California, Los Angeles, CA 90095, USA.

Eli and Edythe Broad Stem Cell Research Center, University of California, Los Angeles, CA 90095, USA.

出版信息

Cardiovasc Res. 2022 Feb 21;118(3):828-843. doi: 10.1093/cvr/cvab102.

Abstract

AIMS

We prospectively isolate and characterize first and second heart field- and nodal-like cardiomyocytes using a double reporter line from human embryonic stem cells. Our double reporter line utilizes two important transcription factors in cardiac development, TBX5 and NKX2-5. TBX5 expression marks first heart field progenitors and cardiomyocytes while NKX2-5 is expressed in nearly all myocytes of the developing heart (excluding nodal cells). We address the shortcomings of prior work in the generation of heart field-specific cardiomyocytes from induced pluripotent stem cells and provide a comprehensive early developmental transcriptomic as well as electrophysiological analyses of these three populations.

METHODS AND RESULTS

Transcriptional, immunocytochemical, and functional studies support the cellular identities of isolated populations based on the expression pattern of NKX2-5 and TBX5. Importantly, bulk and single-cell RNA sequencing analyses provide evidence of unique molecular signatures of isolated first and second heart field cardiomyocytes, as well as nodal-like cells. Extensive electrophysiological analyses reveal dominant atrial action potential phenotypes in first and second heart fields in alignment with our findings in single-cell RNA sequencing. Lastly, we identify two novel surface markers, POPDC2 and CORIN, that enable purification of cardiomyocytes and first heart field cardiomyocytes, respectively.

CONCLUSIONS

We describe a high-yield approach for isolation and characterization of human embryonic stem cell-derived heart field-specific and nodal-like cardiomyocytes. Obtaining enriched populations of these different cardiomyocyte subtypes increases the resolution of gene expression profiling during early cardiogenesis, arrhythmia modelling, and drug screening. This paves the way for the development of effective stem cell therapy to treat diseases that affect specific regions of the heart- or chamber-specific congenital heart defects.

摘要

目的

我们使用来自人类胚胎干细胞的双报告系,前瞻性地分离和鉴定第一和第二心前体细胞和类似节点的心肌细胞。我们的双报告系利用了心脏发育过程中的两个重要转录因子 TBX5 和 NKX2-5。TBX5 的表达标志着第一心前体细胞和心肌细胞,而 NKX2-5 则在发育心脏的几乎所有心肌细胞(节点细胞除外)中表达。我们解决了先前从诱导多能干细胞生成心前体细胞特异性心肌细胞的工作中的缺陷,并提供了这些三种细胞群体的全面早期发育转录组学和电生理分析。

方法和结果

基于 NKX2-5 和 TBX5 的表达模式,转录、免疫细胞化学和功能研究支持分离群体的细胞身份。重要的是,批量和单细胞 RNA 测序分析为分离的第一和第二心前体细胞心肌细胞以及类似节点的细胞提供了独特的分子特征的证据。广泛的电生理分析揭示了第一和第二心场中占主导地位的心房动作电位表型,与我们在单细胞 RNA 测序中的发现一致。最后,我们确定了两个新的表面标记物,POPDC2 和 CORIN,它们分别能够纯化心肌细胞和第一心前体细胞心肌细胞。

结论

我们描述了一种从人类胚胎干细胞中分离和鉴定心前体细胞特异性和类似节点的心肌细胞的高产量方法。获得这些不同心肌细胞亚型的富集群体增加了早期心脏发生过程中基因表达谱分析的分辨率、心律失常建模和药物筛选。这为开发有效的干细胞疗法治疗影响心脏特定区域或腔室特定先天性心脏缺陷的疾病铺平了道路。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/99c7/9020202/908148403450/cvab102f7.jpg

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