FoxO3 controls cardiomyocyte proliferation and heart regeneration by regulating Sfrp2 expression in postnatal mice.

FoxO3 通过调节出生后小鼠的 Sfrp2 表达来控制心肌细胞增殖和心脏再生

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作者：Xia Jing-Bo, Liu Kun, Lin Xiao-Lin, Li Hong-Ji, Lin Jin-Hua, Li Li, Liang Chi-Qian, Cao Yan, Wen Na, Liao Zhao-Fu, Zhao Hui, Park Kyu-Sang, Song Guo-Hua, Ye Ze-Bing, Cai Dong-Qing, Ju Zhen-Yu, Qi Xu-Feng

期刊：

Nature Communications

影响因子：

15.700

时间：

2025

起止号：

2025 Mar 14; 16(1):2532

doi：

10.1038/s41467-025-57962-9

研究方向：

细胞生物学

疾病类型：

心肌炎

The Forkhead box O3 (FoxO3) transcription factor is crucial to controlling heart growth in adulthood, but its exact role in cardiac repair and regeneration in postnatal mice remains unclear. Here, we show that FoxO3 deficiency promotes cardiomyocyte proliferation in postnatal mice and improves cardiac function in homeostatic adult mice. Moreover, FoxO3 deficiency accelerates heart regeneration following injury in postnatal mice at the regenerative and non-regenerative stages. We reveal that FoxO3 directly promotes the expression of secreted frizzled-related protein 2 (Sfrp2) and suppresses the activation of canonical Wnt/Î²-catenin signaling during heart regeneration. The increased activation of Î²-catenin in FoxO3-deficient cardiomyocytes can be blocked by Sfrp2 overexpression. In addition, Sfrp2 overexpression suppressed cardiomyocyte proliferation and heart regeneration in FoxO3-deficient mice. These findings suggest that FoxO3 negatively controls cardiomyocyte proliferation and heart regeneration in postnatal mice at least in part by promoting Sfrp2 expression, which leading to the inactivation of canonical Wnt/Î²-catenin signaling.

FoxO3 controls cardiomyocyte proliferation and heart regeneration by regulating Sfrp2 expression in postnatal mice.

FoxO3 通过调节出生后小鼠的 Sfrp2 表达来控制心肌细胞增殖和心脏再生

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