Kielin/chordin-like protein deficiency aggravates pressure overload-induced cardiac dysfunction and remodeling via P53/P21/CCNB1 signaling in mice.
Yao XuZihui ZhengHeng PanMengmeng ZhaoJishou ZhangShanshan PengJianfang LiuWei PanZheng YinShuwan XuCheng WeiJuan-Juan QinYingzhong LinJun WanMenglong WangPublished in: FASEB journal : official publication of the Federation of American Societies for Experimental Biology (2024)
Targeting cardiac remodeling is regarded as a key therapeutic strategy for heart failure. Kielin/chordin-like protein (KCP) is a secretory protein with 18 cysteine-rich domains and associated with kidney and liver fibrosis. However, the relationship between KCP and cardiac remodeling remains unclear. Here, we aimed to investigate the role of KCP in cardiac remodeling induced by pressure overload and explore its potential mechanisms. Left ventricular (LV) KCP expression was measured with real-time quantitative PCR, western blotting, and immunofluorescence staining in pressure overload-induced cardiac remodeling in mice. Cardiac function and remodeling were evaluated in wide-type (WT) mice and KCP knockout (KO) mice by echocardiography, which were further confirmed by histological analysis with hematoxylin and eosin and Masson staining. RNA sequence was performed with LV tissue from WT and KO mice to identify differentially expressed genes and related signaling pathways. Primary cardiac fibroblasts (CFs) were used to validate the regulatory role and potential mechanisms of KCP during fibrosis. KCP was down-regulated in the progression of cardiac remodeling induced by pressure overload, and was mainly expressed in fibroblasts. KCP deficiency significantly aggravated pressure overload-induced cardiac dysfunction and remodeling. RNA sequence revealed that the role of KCP deficiency in cardiac remodeling was associated with cell division, cell cycle, and P53 signaling pathway, while cyclin B1 (CCNB1) was the most significantly up-regulated gene. Further investigation in vivo and in vitro suggested that KCP deficiency promoted the proliferation of CFs via P53/P21/CCNB1 pathway. Taken together, these results suggested that KCP deficiency aggravates cardiac dysfunction and remodeling induced by pressure overload via P53/P21/CCNB1 signaling in mice.
Keyphrases
- left ventricular
- heart failure
- signaling pathway
- cell cycle
- high fat diet induced
- oxidative stress
- hypertrophic cardiomyopathy
- computed tomography
- single cell
- diabetic rats
- poor prognosis
- acute myocardial infarction
- type diabetes
- genome wide
- mitral valve
- metabolic syndrome
- pulmonary hypertension
- coronary artery disease
- cell proliferation
- atrial fibrillation
- adipose tissue
- mesenchymal stem cells
- bone marrow
- endothelial cells
- pi k akt
- percutaneous coronary intervention
- risk assessment
- insulin resistance
- amino acid
- drug induced
- left atrial
- acute coronary syndrome
- human health
- induced apoptosis
- aortic valve
- acute heart failure