Structural basis for the inhibition of SARS-CoV-2 main protease by antineoplastic drug carmofur.

Zhenming JinYao ZhaoYuan SunBing ZhangHaofeng WangYan WuYan ZhuChen ZhuTianyu HuXiaoyu DuYinkai DuanJing YuXiaobao YangXiuna YangKailin YangXiang LiuLuke W GuddatGengfu XiaoLei-Ke Zhang Haitao YangZihe Rao

Published in: Nature structural & molecular biology (2020)

The antineoplastic drug carmofur is shown to inhibit the SARS-CoV-2 main protease (Mpro). Here, the X-ray crystal structure of Mpro in complex with carmofur reveals that the carbonyl reactive group of carmofur is covalently bound to catalytic Cys145, whereas its fatty acid tail occupies the hydrophobic S2 subsite. Carmofur inhibits viral replication in cells (EC50 = 24.30 μM) and is a promising lead compound to develop new antiviral treatment for COVID-19.

Keyphrases

sars cov
structural basis
respiratory syndrome coronavirus
fatty acid
induced apoptosis
high resolution
cell cycle arrest
coronavirus disease
computed tomography
cell death
drug induced
replacement therapy
crystal structure