Article

The PIWI-interacting RNA CRAPIR alleviates myocardial ischemia‒reperfusion injury by reducing p53-mediated apoptosis via binding to SRSF1

Hong Yan1,2, Han Li1,3, Dao-hong Yin1,3, Zi-zhen Zhang1,3, Qian-yun Zhang1,3, Zhong-yu Ren1,3, Yu Hu1,3, Gui-yang Zheng1,3, Yu Liu4, Wen-ya Ma1,3, Yi-ning Liu1,3, Xiu-xiu Wang1,3, Ben-zhi Cai1,3,5, Hong-yang Chen1,6
1 Department of Pharmacy at the Second Affiliated Hospital (National Key Laboratory of Frigid Zone Cardiovascular Diseases), Harbin Medical University, Harbin 150086, China
2 Department of Pharmacy at the Fourth Affiliated Hospital of Harbin Medical University, Harbin 150086, China
3 Institute of Clinical Pharmacology (The Heilongjiang Key Laboratory of Drug Research), Harbin Medical University, Harbin 150001, China
4 Department of Clinical Laboratory at the Fourth Affiliated Hospital of Harbin Medical University, Harbin 150001, China
5 NHC Key Laboratory of Cell Transplantation, The Heilongjiang Key Laboratory of Drug Research, Harbin Medical University, Harbin 150001, China
6 College of Pharmacy, Harbin Medical University (Daqing), Daqing 163319, China
Correspondence to: Yi-ning Liu: 18846456454@163.com, Xiu-xiu Wang: wangxiuxiu2017@126.com, Ben-zhi Cai: caibz@ems.hrbmu.edu.cn, Hong-yang Chen: chenhongyang@hmudq.edu.cn,
DOI: 10.1038/s41401-025-01534-6
Received: 18 October 2024
Accepted: 6 March 2025
Advance online: 3 April 2025

Abstract

Ischemia-reperfusion (I/R) injury refers to the secondary damage that occurs when blood flow is restored to heart tissues and organs following a period of prolonged ischemia. This damage is exacerbated primarily through mechanisms such as oxidative stress, inflammatory responses and apoptosis, all of which can severely impact patient prognosis. PIWI-interacting RNAs (piRNAs) represent a novel class of small noncoding RNAs that play pivotal roles in regulating gene expression and cellular functions. However, the precise role and underlying mechanisms of piRNAs in I/R injury remain poorly understood. In this study, we investigated the role and molecular mechanisms of a cardiac regeneration-associated PIWI-interacting RNA (CRAPIR), previously identified by our team, in I/R injury. An I/R injury model was established in adult male mice. The protein levels of cleaved caspase-3, Bax, Bcl2 and p53 were assessed using Western blotting, and cardiomyocyte apoptosis was detected via TUNEL staining. Our study revealed that, in I/R-damaged heart tissues and hypoxia‒reoxygenation (H/R)-induced cardiomyocyte models, CRAPIR was upregulated 24 h after I/R and H/R but was markedly downregulated at 72 h after I/R injury and 48 h after H/R injury. In the I/R mouse model, agomir-mediated overexpression of CRAPIR alleviated heart dysfunction and reduced cardiomyocyte apoptosis caused by I/R injury. Conversely, CRAPIR knockdown via an antagomir exacerbated I/R-induced cardiac dysfunction and increased the number of apoptotic cardiomyocytes. Mechanistically, CRAPIR interacts with serine/arginine-rich splicing factor 1 (SRSF1), triggering the upregulation of murine double minute 2 (MDM2) expression. The increased MDM2 promoted p53 ubiquitination, leading to reduced p53 levels. Furthermore, silencing SRSF1 or MDM2 attenuated the protective effect of CRAPIR against cardiomyocyte apoptosis following H/R injury. These findings suggest that CRAPIR serves as a critical regulator of I/R injury via the SRSF1/MDM2/p53 signaling pathway.
Keywords: PIWI-interacting RNA; apoptosis; ischemia/reperfusion injury; SRSF1; p53

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