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CircRNA DICAR as a novel endogenous regulator for diabetic cardiomyopathy and diabetic pyroptosis of cardiomyocytes

Qiong Yuan, Yunwei Sun, Fan Yang, Dan Yan, Mei-Hua Shen, Zhigang Jin, Lin Zhan, Guangqi Liu, Ling Yang, Qianyi Zhou, Zhijun Yu, Xiangyu Zhou, Yang Yu, Yong Xu, Qingming Wu, Jianfang Luo, Xiamin Hu, Chunxiang Zhang

2023Signal Transduction and Targeted Therapy115 citationsDOIOpen Access PDF

Abstract

Abstract In this study, we identified that a conserved circular RNA (circRNA) DICAR, which was downregulated in diabetic mouse hearts. DICAR had an inhibitory effect on diabetic cardiomyopathy (DCM), as the spontaneous cardiac dysfunction, cardiac cell hypertrophy, and cardiac fibrosis occurred in DICAR deficiency ( DICAR +/− ) mice, whereas the DCM was alleviated in DICAR-overexpressed DICAR Tg mice. At the cellular level, we found that overexpression of DICAR inhibited, but knockdown of DICAR enhanced the diabetic cardiomyocyte pyroptosis. At the molecular level, we identified that DICAR-VCP-Med12 degradation could be the underlying molecular mechanism in DICAR-mediated effects. The synthesized DICAR junction part (DICAR-JP) exhibited a similar effect to the entire DICAR. In addition, the expression of DICAR in circulating blood cells and plasma from diabetic patients was lower than that from health controls, which was consistent with the decreased DICAR expression in diabetic hearts. DICAR and the synthesized DICAR-JP may be drug candidates for DCM.

Topics & Concepts

Diabetic cardiomyopathyPyroptosisGene knockdownInternal medicineMedicineRegulatorFibrosisCardiomyopathyEndogenyEndocrinologyCardiac dysfunctionCardiac fibrosisHeart failureApoptosisCell biologyChemistryBiologyInflammasomeGeneInflammationBiochemistryCircular RNAs in diseasesCardiovascular Issues in PregnancyPregnancy-related medical research
CircRNA DICAR as a novel endogenous regulator for diabetic cardiomyopathy and diabetic pyroptosis of cardiomyocytes | Litcius