Probing the SAM Binding Site of SARS-CoV-2 Nsp14 In Vitro Using SAM Competitive Inhibitors Guides Developing Selective Bisubstrate Inhibitors

被引:0
作者
Devkota, Kanchan [1 ]
Schapira, Matthieu [1 ,2 ]
Perveen, Sumera [1 ]
Yazdi, Aliakbar Khalili [1 ]
Li, Fengling [1 ]
Chau, Irene [1 ]
Ghiabi, Pegah [1 ]
Hajian, Taraneh [1 ]
Loppnau, Peter [1 ]
Bolotokova, Albina [1 ]
Satchell, Karla J. F. [3 ]
Wang, Ke [4 ,5 ]
Li, Deyao [4 ,5 ]
Liu, Jing [6 ,7 ]
Smil, David [1 ]
Luo, Minkui [4 ,5 ]
Jin, Jian [6 ,7 ]
Fish, Paul, V [8 ]
Brown, Peter J. [1 ]
Vedadi, Masoud [1 ,2 ]
机构
[1] Univ Toronto, Struct Genom Consortium, 101 Coll St 7 Floor,Room 714, Toronto, ON M5G 1L7, Canada
[2] Univ Toronto, Dept Pharmacol & Toxicol, Toronto, ON, Canada
[3] Northwestern Univ, Dept Microbiol Immunol, Ctr Struct Genom Infect Dis, Feinberg Sch Med, Chicago, IL 60611 USA
[4] Mem Sloan Kettering Canc Ctr, Chem Biol Program, 1275 York Ave, New York, NY 10021 USA
[5] Cornell Univ, Weill Cornell Med Coll, Program Pharmacol, New York, NY 10021 USA
[6] Icahn Sch Med Mt Sinai, Mt Sinai Ctr Therapeut Discovery, Dept Pharmacol Sci, Tisch Canc Inst, New York, NY 10029 USA
[7] Icahn Sch Med Mt Sinai, Mt Sinai Ctr Therapeut Discovery, Dept Oncol Sci, Tisch Canc Inst, New York, NY 10029 USA
[8] UCL, Alzheimers Res UK UCL Drug Discovery Inst, London, England
基金
英国工程与自然科学研究理事会; 美国国家卫生研究院; 加拿大创新基金会;
关键词
nsp14; SARS-CoV-2; COVID-19; coronavirus; MASS-SPECTROMETRY; CORONAVIRUS; SARS; PNEUMONIA; DISCOVERY; DOT1L;
D O I
10.1177/24725552211026261
中图分类号
Q5 [生物化学];
学科分类号
071010 ; 081704 ;
摘要
The COVID-19 pandemic has clearly brought the healthcare systems worldwide to a breaking point, along with devastating socioeconomic consequences. The SARS-CoV-2 virus, which causes the disease, uses RNA capping to evade the human immune system. Nonstructural protein (nsp) 14 is one of the 16 nsps in SARS-CoV-2 and catalyzes the methylation of the viral RNA at N7-guanosine in the cap formation process. To discover small-molecule inhibitors of nsp14 methyltransferase (MTase) activity, we developed and employed a radiometric MTase assay to screen a library of 161 in-house synthesized S-adenosylmethionine (SAM) competitive MTase inhibitors and SAM analogs. Among six identified screening hits, SS148 inhibited nsp14 MTase activity with an IC50 value of 70 +/- 6 nM and was selective against 20 human protein lysine MTases, indicating significant differences in SAM binding sites. Interestingly, DS0464 with an IC50 value of 1.1 +/- 0.2 mu M showed a bisubstrate competitive inhibitor mechanism of action. DS0464 was also selective against 28 out of 33 RNA, DNA, and protein MTases. The structure-activity relationship provided by these compounds should guide the optimization of selective bisubstrate nsp14 inhibitors and may provide a path toward a novel class of antivirals against COVID-19, and possibly other coronaviruses.
引用
收藏
页码:1200 / 1211
页数:12
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