Author: Yan, Haiyan; Sun, Jing; Wang, Kun; Wang, Huiqiang; Wu, Shuo; Bao, Linlin; He, Weiqing; Wang, Dong; Zhu, Airu; Zhang, Tian; Gao, Rongmei; Dong, Biao; Li, Jianrui; Yang, Lu; Zhong, Ming; Lv, Qi; Qin, Feifei; Zhuang, Zhen; Huang, Xiaofang; Yang, Xinyi; Li, Yuhuan; Che, Yongsheng; Jiang, Jiandong
Title: Repurposing CFDA-approved drug carrimycin as an antiviral agent against human coronaviruses, including the currently pandemic SARS-CoV-2 Cord-id: zp9qn3wv Document date: 2021_3_11
ID: zp9qn3wv
Snippet: COVID-19 pandemic caused by SARS-CoV-2 infection severely threatens global health and economic development. No effective antiviral drug is currently available to treat COVID-19 and any other human coronavirus infections. We report herein that a CFDA-approved macrolide antibiotic, carrimycin, potently inhibited the cytopathic effects (CPE) and reduced the levels of viral protein and RNA in multiple cell types infected by human coronavirus 229E, OC43, and SARS-CoV-2. Time-of-addition and pseudotyp
Document: COVID-19 pandemic caused by SARS-CoV-2 infection severely threatens global health and economic development. No effective antiviral drug is currently available to treat COVID-19 and any other human coronavirus infections. We report herein that a CFDA-approved macrolide antibiotic, carrimycin, potently inhibited the cytopathic effects (CPE) and reduced the levels of viral protein and RNA in multiple cell types infected by human coronavirus 229E, OC43, and SARS-CoV-2. Time-of-addition and pseudotype virus infection studies indicated that carrimycin inhibited one or multiple post-entry replication events of human coronavirus infection. In support of this notion, metabolic labelling studies showed that carrimycin significantly inhibited the synthesis of viral RNA. Our studies thus strongly suggest that carrimycin is an antiviral agent against a broad-spectrum of human coronaviruses and its therapeutic efficacy to COVID-19 is currently under clinical investigation.
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