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10.3389/fmicb.2020.01105

http://scihub22266oqcxt.onion/10.3389/fmicb.2020.01105
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32595613!7304253!32595613
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suck abstract from ncbi


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pmid32595613      Front+Microbiol 2020 ; 11 (ä): 1105
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  • Remdesivir (GS-5734) Impedes Enterovirus Replication Through Viral RNA Synthesis Inhibition #MMPMID32595613
  • Ye W; Yao M; Dong Y; Ye C; Wang D; Liu H; Ma H; Zhang H; Qi L; Yang Y; Wang Y; Zhang L; Cheng L; Lv X; Xu Z; Lei Y; Zhang F
  • Front Microbiol 2020[]; 11 (ä): 1105 PMID32595613show ga
  • Human enteroviruses are responsible for diverse diseases, from mild respiratory symptoms to fatal neurological complications. Currently, no registered antivirals have been approved for clinical therapy. Thus, a therapeutic agent for the enterovirus-related disease is urgently needed. Remdesivir (GS-5734) is a novel monophosphoramidate adenosine analog prodrug that exhibits potent antiviral activity against diverse RNA virus families, including positive-sense Coronaviridae and Flaviviridae and negative-sense Filoviridae, Paramyxoviridae, and Pneumoviridae. Currently, remdesivir is under phase 3 clinical development for disease COVID-19 treatment. Here, we found that remdesivir impeded both EV71 viral RNA (vRNA) and complementary (cRNA) synthesis, indicating that EV71 replication is inhibited by the triphosphate (TP) form of remdesivir. Moreover, remdesivir showed potent antiviral activity against diverse enteroviruses. These data extend the remdesivir antiviral activity to enteroviruses and indicate that remdesivir is a promising antiviral treatment for EV71 and other enterovirus infections.
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