Melatonin reduces oxidative damage in mouse granulosa cells via restraining JNK-dependent autophagy.

Oxidative stress-induced granulosa cell (GCs) injury is believed to be a common trigger for follicular atresia. Emerging evidence indicates that excessive autophagy occurs in mammalian cells with oxidative damage. N-acetyl-5-methoxytrypamine (melatonin) has been shown to prevent GCs from oxidative injury， although the exact mechanism remains to be elucidated. Here， we first demonstrated that the suppression of autophagy through the JNK/BCL-2/BECN1 signaling is engaged in melatonin-mediated GCs protection against oxidative damage. Melatonin inhibited the loss of GCs viability， formation of GFP-MAP1LC3B puncta， accumulation of MAP1LC3B-II blots， degradation of SQSTM1 and the expression of BECN1， which was correlated with impaired activation of JNK during oxidative stress. On the other hand， blocking of autophagy and/or JNK also reduced the level of HO-induced GCs death， but failed to further restore GCs viability in the presence of melatonin. Particularly， the suppression of autophagy provided no additional protective effects when GCs were pretreated with JNK inhibitor and/or melatonin. Importantly， we found that the enhanced interaction between BCL-2 and BECN1 might be a responsive mechanism for autophagy suppression via the melatonin/JNK pathway. Moreover， blocking the downstream antioxidant system of melatonin using specific inhibitors further confirmed a direct role of melatonin/JNK/autophagy axis in preserving GCs survival without scavenging reactive oxygen species (ROS). Taken together， our findings uncover a novel function of melatonin in preventing GCs from oxidative damage by targeting JNK-mediated autophagy， which might contribute to develop therapeutic strategies for patients with ovulation failure-related disorders.