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斑马鱼发育和再生过程中心肌细胞的异质性。

Cardiomyocyte heterogeneity during zebrafish development and regeneration.

机构信息

Department of Developmental Genetics, Max Planck Institute for Heart and Lung Research, Bad Nauheim, Germany.

Bioinformatics and Deep Sequencing Platform, Max Planck Institute for Heart and Lung Research, Bad Nauheim, Germany.

出版信息

Dev Biol. 2021 Aug;476:259-271. doi: 10.1016/j.ydbio.2021.03.014. Epub 2021 Apr 12.

Abstract

Contrary to adult mammals, zebrafish are able to regenerate their heart after cardiac injury. This regenerative response relies, in part, on the endogenous ability of cardiomyocytes (CMs) to dedifferentiate and proliferate to replenish the lost muscle. However, CM heterogeneity and population dynamics during development and regeneration require further investigation. Through comparative transcriptomic analyses of the developing and adult zebrafish heart, we identified tnnc2 and tnni4b.3 expression as markers for CMs at early and late developmental stages, respectively. Using newly developed reporter lines for these genes, we investigated their expression dynamics during heart development and regeneration. tnnc2 reporter lines label most CMs at embryonic stages, and this labeling declines rapidly during larval stages; in adult hearts, tnnc2 reporter expression is only detectable in a small subset of CMs. Conversely, expression of a tnni4b.3 reporter is initially visible in CMs in the outer curvature of the ventricle at larval stages, and it is subsequently present in a vast majority of the CMs in adult hearts. To further characterize the adult CMs labeled by the tnnc2 (i.e., embryonic) reporter, we performed transcriptomic analyses and found that they express markers of immature CMs as well as genes encoding components of the Notch signaling pathway. In support of this finding, we observed, using two different reporters, that these CMs display higher levels of Notch signaling. Moreover, during adult heart regeneration, CMs in the injured area activate the embryonic CM reporter and downregulate the tnni4b.3 reporter, further highlighting the molecular changes in regenerating CMs. Overall, our findings provide additional evidence for CM heterogeneity in adult zebrafish.

摘要

与成年哺乳动物不同,斑马鱼在心脏损伤后能够再生心脏。这种再生反应部分依赖于心肌细胞(CMs)去分化和增殖的内在能力,以补充丢失的肌肉。然而,CM 的异质性和发育及再生过程中的群体动态仍需要进一步研究。通过对发育中和成年斑马鱼心脏的比较转录组分析,我们鉴定出 tnnc2 和 tnni4b.3 的表达可分别作为早期和晚期发育阶段 CMs 的标志物。利用新开发的这些基因的报告线,我们研究了它们在心脏发育和再生过程中的表达动态。tnnc2 报告线在胚胎阶段标记大多数 CMs,而在幼体阶段标记迅速减少;在成年心脏中,tnnc2 报告线的表达仅在一小部分 CMs 中可检测到。相反,tnni4b.3 报告线的表达在幼体阶段首先在心室外弯曲处的 CMs 中可见,随后在成年心脏中的绝大多数 CMs 中存在。为了进一步表征由 tnnc2(即胚胎)报告线标记的成年 CMs,我们进行了转录组分析,发现它们表达未成熟 CMs 的标志物以及 Notch 信号通路组成部分的基因。支持这一发现,我们使用两种不同的报告线观察到,这些 CMs 表现出更高水平的 Notch 信号。此外,在成年心脏再生过程中,损伤区域的 CMs 激活胚胎期 CM 报告线并下调 tnni4b.3 报告线,这进一步强调了再生 CMs 中的分子变化。总的来说,我们的研究结果为成年斑马鱼 CMs 的异质性提供了更多证据。

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