Infectious bronchitis virus (IBV) triggers autophagy to enhance viral replication by activating the VPS34 complex

Autophagy plays an important role in the lifecycle of viruses. However, there is currently a lack of systematic research on the relationship between Infectious Bronchitis Virus (IBV) and Autophagy. This study aims to investigate the impact of IBV on Autophagy and the role of Autophagy in viral replication. We observed that IBV Infection increased the expression of microtubule-associated protein 1 LIGHT chain 3, a marker of Autophagy, decreased the expression of sequestosome 1, and led to elevated intracellular LC3 puncta levels. These findings suggest that IBV Infection activates the autophagic process in cells. To investigate the impact of Autophagy on the replication of IBV, we utilized rapamycin as an Autophagy activator and 3-methyladenine as an Autophagy Inhibitor. Our results indicate that IBV promotes viral replication by inducing Autophagy. Further investigation revealed that IBV induces autophagosome formation by inhibiting the mTOR-ULK1 pathway and activating the activity of vacuolar protein sorting 34 (Vps34), autophagy-related gene 14, and the Beclin-1 complex. Vps34 plays a crucial role in this process, as inhibiting Vps34 protein activity enhances cell proliferation after IBV Infection. Additionally, inhibiting Vps34 significantly improves the survival rate of IBV-infected chicks, suppresses IBV replication in the kidney, and alleviates tracheal, lung, and kidney damage caused by IBV Infection. In summary, IBV Infection can induce Autophagy by modulating the mTOR/ULK1 signaling pathway and activating the Vps34 complex, while Autophagy serves to promote virus replication.

Autophagy; IBV; VPS34; Viral replication; mTOR/ULK1 signaling pathway.