Attenuation of SARS-CoV-2 replication and associated inflammation by concomitant targeting of viral and host cap 2'-O-ribose methyltransferases

被引:23
|
作者
Bergant, Valter [1 ]
Yamada, Shintaro [2 ]
Grass, Vincent [1 ]
Tsukamoto, Yuta [2 ]
Lavacca, Teresa [1 ]
Krey, Karsten [1 ]
Muhlhofer, Maria-Teresa [1 ]
Wittmann, Sabine [3 ]
Ensser, Armin [3 ]
Herrmann, Alexandra [3 ]
Vom Hemdt, Anja [4 ]
Tomita, Yuriko [5 ]
Matsuyama, Shutoku [5 ]
Hirokawa, Takatsugu [6 ,7 ,8 ]
Huang, Yiqi [1 ]
Piras, Antonio [1 ]
Jakwerth, Constanze A. [9 ,10 ,11 ]
Oelsner, Madlen [9 ,10 ,11 ]
Thieme, Susanne [12 ]
Graf, Alexander [12 ]
Krebs, Stefan [12 ]
Blum, Helmut [12 ]
Kuemmerer, Beate M. [4 ,13 ]
Stukalov, Alexey [1 ]
Schmidt-Weber, Carsten B. [9 ,10 ,11 ]
Igarashi, Manabu [14 ,15 ]
Gramberg, Thomas [3 ]
Pichlmair, Andreas [1 ,16 ]
Kato, Hiroki [2 ]
机构
[1] Tech Univ Munich TUM, Sch Med, Inst Virol, Munich, Germany
[2] Univ Hosp Bonn UKB, Med Fac, Inst Cardiovasc Immunol, Bonn, Germany
[3] Friedrich Alexander Univ Erlangen Nurnberg, Inst Clin & Mol Virol, Erlangen, Germany
[4] Univ Bonn, Med Fac, Inst Virol, Bonn, Germany
[5] Natl Inst Infect Dis NIID, Dept Virol 3, Tokyo, Japan
[6] Univ Tsukuba, Transborder Med Res Ctr, Tsukuba, Ibaraki, Japan
[7] Univ Tsukuba, Div Biomed Sci, Tsukuba, Ibaraki, Japan
[8] Natl Inst Adv Ind Sci & Technol, Cellular & Mol Biotechnol Res Inst, Tokyo, Japan
[9] Tech Univ Munich TUM, Ctr Allergy & Environm ZAUM, Munich, Germany
[10] German Res Ctr Environm Hlth, Helmholtz Ctr Munich, Munich, Germany
[11] German Ctr Lung Res DZL, CPC M, Munich, Germany
[12] Ludwig Maximilian Univ Munich LMU, Gene Ctr, Lab Funct Genome Anal LAFUGA, Munich, Germany
[13] German Ctr Infect Res DZIF, Bonn Cologne Partner Site, Bonn, Germany
[14] Hokkaido Univ, Int Inst Zoonosis Control, Int Collaborat Unit, Sapporo, Hokkaido, Japan
[15] Hokkaido Univ, Int Inst Zoonosis Control, Div Global Epidemiol, Sapporo, Hokkaido, Japan
[16] German Ctr Infect Res DZIF, Munich Partner Site, Munich, Germany
基金
欧洲研究理事会;
关键词
antivirals; COVID-19; host-directed; methyltransferase; SARS-CoV-2; S-ADENOSYLHOMOCYSTEINE HYDROLASE; BROAD-SPECTRUM; CAUSES HYPERHOMOCYSTEINEMIA; ACCURATE DOCKING; L-HOMOCYSTEINE; IN-VITRO; CORONAVIRUS; INHIBITOR; POTENT; RNA;
D O I
10.15252/embj.2022111608
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
The SARS-CoV-2 infection cycle is a multistage process that relies on functional interactions between the host and the pathogen. Here, we repurposed antiviral drugs against both viral and host enzymes to pharmaceutically block methylation of the viral RNA 2'-O-ribose cap needed for viral immune escape. We find that the host cap 2'-O-ribose methyltransferase MTr1 can compensate for loss of viral NSP16 methyltransferase in facilitating virus replication. Concomitant inhibition of MTr1 and NSP16 efficiently suppresses SARS-CoV-2 replication. Using in silico target-based drug screening, we identify a bispecific MTr1/NSP16 inhibitor with anti-SARS-CoV-2 activity in vitro and in vivo but with unfavorable side effects. We further show antiviral activity of inhibitors that target independent stages of the host SAM cycle providing the methyltransferase co-substrate. In particular, the adenosylhomocysteinase (AHCY) inhibitor DZNep is antiviral in in vitro, in ex vivo, and in a mouse infection model and synergizes with existing COVID-19 treatments. Moreover, DZNep exhibits a strong immunomodulatory effect curbing infection-induced hyperinflammation and reduces lung fibrosis markers ex vivo. Thus, multispecific and metabolic MTase inhibitors constitute yet unexplored treatment options against COVID-19.
引用
收藏
页数:23
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