Nature Communications,2022年
Wancang Liu, Liyan Yu, Quanjie Li, Tao Zhang, Zhe Guo, Jing Wang, Xu Pang, Xiaoyu Li, Dongrong Yi, Yongxin Zhang, Xiaomei Fang, Shan Cen, Jianyuan Zhao, Rui Zhou, Tao Deng, Fei Guo, Chen Liang, Zhenlong Liu
LicenseType:CC BY |
| 
| 
[ 浏览:0 
下载:0
] The emergence of new highly pathogenic and drug-resistant influenza strains urges the development of novel therapeutics for influenza A virus (IAV). Here, we report the discovery of an anti-IAV microbial metabolite called APL-16-5 that was originally isolated from the plant endophytic fungus Aspergillus sp. CPCC 400735. APL-16-5 binds to both the E3 ligase TRIM25 and IAV polymerase subunit PA, leading to TRIM25 ubiquitination of PA and subsequent degradation of PA in the proteasome. This mode of action conforms to that of a proteolysis targeting chimera which employs the cellular ubiquitin-proteasome machinery to chemically induce the degradation of target proteins. Importantly, APL-16-5 potently inhibits IAV and protects mice from lethal IAV infection. Therefore, we have identified a natural microbial metabolite with potent in vivo anti-IAV activity and the potential of becoming a new IAV therapeutic. The antiviral mechanism of APL-16-5 opens the possibility of improving its anti-IAV potency and specificity by adjusting its affinity for TRIM25 and viral PA protein through medicinal chemistry.
Nature Communications,2022年
Wancang Liu, Liyan Yu, Quanjie Li, Tao Zhang, Zhe Guo, Jing Wang, Xu Pang, Xiaoyu Li, Dongrong Yi, Yongxin Zhang, Xiaomei Fang, Shan Cen, Jianyuan Zhao, Rui Zhou, Tao Deng, Fei Guo, Chen Liang, Zhenlong Liu
LicenseType:CC BY |
The emergence of new highly pathogenic and drug-resistant influenza strains urges the development of novel therapeutics for influenza A virus (IAV). Here, we report the discovery of an anti-IAV microbial metabolite called APL-16-5 that was originally isolated from the plant endophytic fungus Aspergillus sp. CPCC 400735. APL-16-5 binds to both the E3 ligase TRIM25 and IAV polymerase subunit PA, leading to TRIM25 ubiquitination of PA and subsequent degradation of PA in the proteasome. This mode of action conforms to that of a proteolysis targeting chimera which employs the cellular ubiquitin-proteasome machinery to chemically induce the degradation of target proteins. Importantly, APL-16-5 potently inhibits IAV and protects mice from lethal IAV infection. Therefore, we have identified a natural microbial metabolite with potent in vivo anti-IAV activity and the potential of becoming a new IAV therapeutic. The antiviral mechanism of APL-16-5 opens the possibility of improving its anti-IAV potency and specificity by adjusting its affinity for TRIM25 and viral PA protein through medicinal chemistry.
Signal Transduction and Targeted Therapy,2022年
Peng Du, Xu Yang, Ping Zhu, Huijie Bian, Ke Wang, Zhi-Nan Chen, Ding Wei, Xiuxuan Sun, Ting Guo, Ying Shi, Kun Wang, Jiejie Geng, Tao Zhang, Shirui Chen, Peng Lin, Ruo Chen, Zheng Zhang, Youchun Wang, Chuan Qin, Jiangning Liu, Ke Xu, Guizhen Wu, Qingyi Wang, Liang Chen, Jing Yuan, Hongzhou Lu, Jiuxin Qu, Yingxia Liu, Jin Zou
LicenseType:CC BY |
Signal Transduction and Targeted Therapy,2022年
Peng Du, Xu Yang, Ping Zhu, Huijie Bian, Ke Wang, Zhi-Nan Chen, Ding Wei, Xiuxuan Sun, Ting Guo, Ying Shi, Kun Wang, Jiejie Geng, Tao Zhang, Shirui Chen, Peng Lin, Ruo Chen, Zheng Zhang, Youchun Wang, Chuan Qin, Jiangning Liu, Ke Xu, Guizhen Wu, Qingyi Wang, Liang Chen, Jing Yuan, Hongzhou Lu, Jiuxin Qu, Yingxia Liu, Jin Zou
LicenseType:CC BY |
Journal of Orthopaedic Surgery and Research,2022年
Genxiang Rong, Shuo Zhang, Juehua Jing, Tao Zhang, Yayun Xu
LicenseType:CC BY |
6 Stronger gut microbiome modulatory effects by postbiotics than probiotics in a mouse colitis model [期刊论文]
npj Science of Food,2022年
Lai-Yu Kwok, Qiuwen He, Weiqin Zhang, Tao Zhang, Cuijiao Feng, Zhihong Sun
LicenseType:CC BY |
878987797
028-85220240
