Occlusal disharmony is known to affect not only oral cavity area but also autonomic nervous system in the heart. Since renin-angiotensin system (RAS) inhibitor captopril (Cap) is one of the first-line drugs for preventing cardiac remodeling in patients with heart failure, we hypothesized that Cpt might prevent cardiac dysfunction induced by occlusal disharmony. To test this hypothesis, we used a bite-opening (BO) mouse model, which was developed by cementing a suitable appliance onto the mandibular incisor. Mice (16-week, male C57BL/6) were divided into four groups: 1) Control, 2) BO, 3) Cap (via drinking water containing 0.1g/L), and 4) Cap + BO. After 2 weeks, cardiac function was significantly decreased with increased cardiac fibrosis and myocyte apoptosis in the BO group, compared to the control, and these changes were suppressed by Cap. We examined the mechanism and confirmed that cardiac dysfunction induced by BO was associated with dual phosphorylation on PKCδ (Tyr-311/Thr-505), leading to activation of CaMKII with increased phosphorylation of RyR2 and phospholamban. These results suggest that activation of RAS might play an important role for the development of cardiac diseases induced by occlusal anomalies.