Convergent use of phosphatidic acid for hepatitis C virus and SARS-CoV-2 replication organelle formation

被引:44
|
作者
Tabata, Keisuke [1 ,12 ,13 ]
Prasad, Vibhu [1 ]
Paul, David [1 ,14 ]
Lee, Ji-Young [1 ]
Minh-Tu Pham [1 ]
Twu, Woan-Ing [1 ]
Neufeldt, Christopher J. [1 ]
Cortese, Mirko [1 ]
Cerikan, Berati [1 ]
Stahl, Yannick [2 ]
Joecks, Sebastian [1 ,15 ]
Tran, Cong Si [1 ]
Luechtenborg, Christian [2 ]
V'kovski, Philip [3 ,4 ]
Hoermann, Katrin [5 ]
Mueller, Andre C. [5 ]
Zitzmann, Carolin [6 ,7 ,16 ]
Haselmann, Uta [1 ]
Beneke, Juergen [8 ]
Kaderali, Lars [6 ,7 ]
Erfle, Holger [8 ]
Thiel, Volker [3 ,4 ]
Lohmann, Volker [1 ]
Superti-Furga, Giulio [5 ,9 ]
Bruegger, Britta [2 ]
Bartenschlager, Ralf [1 ,10 ,11 ]
机构
[1] Heidelberg Univ, Dept Infect Dis, Mol Virol, Heidelberg, Germany
[2] Heidelberg Univ, Biochem Ctr Heidelberg, Heidelberg, Germany
[3] Inst Virol & Immunol IVI, Bern, Switzerland
[4] Univ Bern, Vetsuisse Fac, Dept Infect Dis & Pathobiol, Bern, Switzerland
[5] Austrian Acad Sci, CeMM Res Ctr Mol Med, Vienna, Austria
[6] Univ Med Greifswald, Inst Bioinformat, Greifswald, Germany
[7] Univ Med Greifswald, Ctr Funct Genom Microbes, Greifswald, Germany
[8] Heidelberg Univ, BioQuant, Heidelberg, Germany
[9] Med Univ Vienna, Ctr Physiol & Pharmacol, Vienna, Austria
[10] German Canc Res Ctr, Div Virus Associated Carcinogenesis, Heidelberg, Germany
[11] German Ctr Infect Res, Heidelberg Partner Site, Heidelberg, Germany
[12] Osaka Univ, Grad Sch Med, Dept Genet, Osaka, Japan
[13] Osaka Univ, Grad Sch Frontier Biosci, Lab Intracellular Membrane Dynam, Osaka, Japan
[14] MRC Lab Mol Biol, Francis Crick Ave, Cambridge CB2 0QH, England
[15] LI COR Biosci GmbH, Siemensstr 25A, Bad Homburg, Germany
[16] Los Alamos Natl Lab, Theoret Biol & Biophys, Los Alamos, NM USA
基金
欧洲研究理事会; 瑞士国家科学基金会;
关键词
MODULATION; AUTOPHAGY; TARGET; AGPAT2; CYCLE;
D O I
10.1038/s41467-021-27511-1
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
Double membrane vesicles (DMVs) serve as replication organelles of plus-strand RNA viruses such as hepatitis C virus (HCV) and SARS-CoV-2. Viral DMVs are morphologically analogous to DMVs formed during autophagy, but lipids driving their biogenesis are largely unknown. Here we show that production of the lipid phosphatidic acid (PA) by acylglycerolphosphate acyltransferase (AGPAT) 1 and 2 in the ER is important for DMV biogenesis in viral replication and autophagy. Using DMVs in HCV-replicating cells as model, we found that AGPATs are recruited to and critically contribute to HCV and SARS-CoV-2 replication and proper DMV formation. An intracellular PA sensor accumulated at viral DMV formation sites, consistent with elevated levels of PA in fractions of purified DMVs analyzed by lipidomics. Apart from AGPATs, PA is generated by alternative pathways and their pharmacological inhibition also impaired HCV and SARS-CoV-2 replication as well as formation of autophagosome-like DMVs. These data identify PA as host cell lipid involved in proper replication organelle formation by HCV and SARS-CoV-2, two phylogenetically disparate viruses causing very different diseases, i.e. chronic liver disease and COVID-19, respectively. Host-targeting therapy aiming at PA synthesis pathways might be suitable to attenuate replication of these viruses. Double membrane vesicles (DMV) are used as replication organelles by several RNA viruses. Applying proteomics and lipidomics, Tabata and Prasad et al. find that two cellular acyltransferases (AGPAT1/2), responsible for synthesis of phosphatidic acid, play a role in the DMV-biogenesis of HCV and SARS-CoV-2, highlighting a common biogenesis mechanism for evolutionary distant positive-strand RNA viruses.
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页数:15
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