The continuous evolution of coronaviruses compromises the efficacy of existing therapeutic antibodies and replication inhibitors, necessitating antiviral strategies that are resilient to viral escape. Distinct from conventional antibody cocktails that remain vulnerable to spike protein mutations, we evaluated a multi-mechanistic therapy targeting three discrete stages of the viral life cycle: receptor binding, membrane fusion, and viral replication. Using pseudotyped and authentic human coronavi
Potent in vitro synergistic antiviral effects of the pan-coronavirus fusion inhibitor EK1 in combination with RBD-specific antibodies or M pro inhibitors
Ruixue Xiu·Wei Xu·Wenbo Cai·Qi Wang·Minxiang Xie·Yingdan Wang·Chang Li·Qiao Wang·Jinghe Huang·Tianlei Ying·Chuanjun Song·Li Lu·Shi Jiang·Yuanzhou Wang