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An Aurora Kinase B–Based Mouse System to Efficiently Identify and Analyze Proliferating Cardiomyocytes

Wenbin Fu, Qiao Liao, Liangpeng Li, Yu Shi, Andi Zeng, Chunyu Zeng, Wei Eric Wang

2020Frontiers in Cell and Developmental Biology13 citationsDOIOpen Access PDF

Abstract

To identify and analyze the live proliferating cardiomyocytes is crucial for deciphering the mechanisms controlling endogenous cardiac regeneration. Traditional methods confuse cell division with multinucleation in postnatal cardiomyocytes. Recent efforts have achieved significant progress on discerning cytokinesis from only nuclear division. However, those methods were either designed to label post-cytokinesis progeny or challenging to sort the live proliferating cardiomyocytes. In this study, we highlighted an Aurkb-reporter based mouse system with a tdTomato fluorescence labeling. It could efficiently identify proliferating cardiomyocytes in neonates. The analysis of sorting tdTomato+ cardiomyocytes with different ploidy indicated that mononucleated cardiomyocytes might not possess significantly higher proliferating potential than other cardiomyocytes when most cardiomyocytes have become post-mitotic. Moreover, tdTomato+ cardiomyocytes were significantly increased and enriched at injury border zone after apex resection in neonates, while there were no increased tdTomato+ cardiomyocytes after myocardial infarction in adults.

Topics & Concepts

CytokinesisMitosisBiologyCell biologyMyocyteCell divisionCell sortingRegeneration (biology)Developmental biologyCellGeneticsCongenital heart defects researchTissue Engineering and Regenerative MedicineCardiac Fibrosis and Remodeling