关键词: CRISPR / Cas9, OGA, O-GlcNAcylation, AAV9, 心肌细胞

Abstract: Objective Constructing an adult cardiomyocyte-specific Oga knockout mouse model to study the function of endogenous OGA in the maintenance of adult cardiac homeostasis. Method Firstly, Screening the effective sgRNAs targeting the Oga coding region and and constructed them in AAV9 virus. Then AAV9 was injected into cardiomyocyte specific SpCas9 knockin mice ( α-MHC^Cas9) by intraperitoneal injection. qPCR and Western blot were performed to confirm whether Oga was successfully knockout. Finally, to study the function of Oga in cardiac homeostasis maintenance, the cardiac structure was analyzed by histology and the cardiac function was analyzed by transthoracic echocardiography. Result Two effective sgRNAs targeting Oga were identified and delivered by AAV9 to disrupt Oga gene successfully in cardiomyocytes. Consistently, O-GlcNAcylation level was significantly increased by Oga deletion. There were no significant differences in overall structure and function indicated by the histological and echocardiographic analyses. Conclusion By using the AAV9-mediated delivery of CRISPR / Cas9 system, we successfully constructed the adult cardiomyocyte- specific Oga knockout mouse model, which would be provided as an effective mouse model for studying the function and mechanism of OGA-mediated O-GlcNAcylation clearance in the maintenance of cardiac homeostasis.

Key words: CRISPR / Cas9, OGA, O-GlcNAcylation, AAV9, cardiomyocyte