RNA Replication of Mouse Hepatitis Virus Takes Place at Double-membrane Vesicles

Overview

Journal J Virol

Publisher American Society for Microbiology

Date 2002 Mar 22

PMID 11907209

Citations 293

Authors

Rainer Gosert

Amornrat Kanjanahaluethai

Denise Egger

Kurt Bienz

Susan C Baker

Affiliations

Soon will be listed here.

Abstract

The replication complexes (RCs) of positive-stranded RNA viruses are intimately associated with cellular membranes. To investigate membrane alterations and to characterize the RC of mouse hepatitis virus (MHV), we performed biochemical and ultrastructural studies using MHV-infected cells. Biochemical fractionation showed that all 10 of the MHV gene 1 polyprotein products examined pelleted with the membrane fraction, consistent with membrane association of the RC. Furthermore, MHV gene 1 products p290, p210, and p150 and the p150 cleavage product membrane protein 1 (MP1, also called p44) were resistant to extraction with Triton X-114, indicating that they are integral membrane proteins. The ultrastructural analysis revealed double-membrane vesicles (DMVs) in the cytoplasm of MHV-infected cells. The DMVs were found either as separate entities or as small clusters of vesicles. To determine whether MHV proteins and viral RNA were associated with the DMVs, we performed immunocytochemistry electron microscopy (IEM). We found that the DMVs were labeled using an antiserum directed against proteins derived from open reading frame 1a of MHV. By electron microscopy in situ hybridization (ISH) using MHV-specific RNA probes, DMVs were highly labeled for both gene 1 and gene 7 sequences. By combined ISH and IEM, positive-stranded RNA and viral proteins localized to the same DMVs. Finally, viral RNA synthesis was detected by labeling with 5-bromouridine 5'-triphosphate. Newly synthesized viral RNA was found to be associated with the DMVs. We conclude from these data that the DMVs carry the MHV RNA replication complex and are the site of MHV RNA synthesis.

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References

Chen J, Ahlquist P . Brome mosaic virus polymerase-like protein 2a is directed to the endoplasmic reticulum by helicase-like viral protein 1a. J Virol. 2001; 74(9):4310-8. PMC: 111948. DOI: 10.1128/jvi.74.9.4310-4318.2000. View

Kanjanahaluethai A, Baker S . Identification of mouse hepatitis virus papain-like proteinase 2 activity. J Virol. 2000; 74(17):7911-21. PMC: 112322. DOI: 10.1128/jvi.74.17.7911-7921.2000. View

Molenkamp R, van Tol H, Rozier B, van der Meer Y, Spaan W, Snijder E . The arterivirus replicase is the only viral protein required for genome replication and subgenomic mRNA transcription. J Gen Virol. 2000; 81(Pt 10):2491-2496. DOI: 10.1099/0022-1317-81-10-2491. View

Shen X, Masters P . Evaluation of the role of heterogeneous nuclear ribonucleoprotein A1 as a host factor in murine coronavirus discontinuous transcription and genome replication. Proc Natl Acad Sci U S A. 2001; 98(5):2717-22. PMC: 30205. DOI: 10.1073/pnas.031424298. View

Snijder E, van Tol H, Roos N, Pedersen K . Non-structural proteins 2 and 3 interact to modify host cell membranes during the formation of the arterivirus replication complex. J Gen Virol. 2001; 82(Pt 5):985-994. DOI: 10.1099/0022-1317-82-5-985. View

Thiel V, Herold J, Schelle B, Siddell S . Viral replicase gene products suffice for coronavirus discontinuous transcription. J Virol. 2001; 75(14):6676-81. PMC: 114390. DOI: 10.1128/JVI.75.14.6676-6681.2001. View

Rust R, Landmann L, Gosert R, Tang B, Hong W, Hauri H . Cellular COPII proteins are involved in production of the vesicles that form the poliovirus replication complex. J Virol. 2001; 75(20):9808-18. PMC: 114553. DOI: 10.1128/JVI.75.20.9808-9818.2001. View

Kim J, Spence R, Currier P, Lu X, Denison M . Coronavirus protein processing and RNA synthesis is inhibited by the cysteine proteinase inhibitor E64d. Virology. 1995; 208(1):1-8. PMC: 7131484. DOI: 10.1006/viro.1995.1123. View

Sturman L, Takemoto K . Enhanced growth of a murine coronavirus in transformed mouse cells. Infect Immun. 1972; 6(4):501-7. PMC: 422565. DOI: 10.1128/iai.6.4.501-507.1972. View

10.

Hirano N, Murakami T, Fujiwara K, Matsumoto M . Utility of mouse cell line DBT for propagation and assay of mouse hepatitis virus. Jpn J Exp Med. 1978; 48(1):71-5. View

11.

Bordier C . Phase separation of integral membrane proteins in Triton X-114 solution. J Biol Chem. 1981; 256(4):1604-7. View

12.

Fujiki Y, Hubbard A, Fowler S, Lazarow P . Isolation of intracellular membranes by means of sodium carbonate treatment: application to endoplasmic reticulum. J Cell Biol. 1982; 93(1):97-102. PMC: 2112113. DOI: 10.1083/jcb.93.1.97. View

13.

Skinner M, Siddell S . Coronavirus JHM: nucleotide sequence of the mRNA that encodes nucleocapsid protein. Nucleic Acids Res. 1983; 11(15):5045-54. PMC: 326236. DOI: 10.1093/nar/11.15.5045. View

14.

Cox K, DeLeon D, Angerer L, Angerer R . Detection of mrnas in sea urchin embryos by in situ hybridization using asymmetric RNA probes. Dev Biol. 1984; 101(2):485-502. DOI: 10.1016/0012-1606(84)90162-3. View

15.

Bienz K, Egger D, Pasamontes L . Association of polioviral proteins of the P2 genomic region with the viral replication complex and virus-induced membrane synthesis as visualized by electron microscopic immunocytochemistry and autoradiography. Virology. 1987; 160(1):220-6. DOI: 10.1016/0042-6822(87)90063-8. View

16.

Brierley I, Boursnell M, Binns M, Bilimoria B, Blok V, Brown T . An efficient ribosomal frame-shifting signal in the polymerase-encoding region of the coronavirus IBV. EMBO J. 1987; 6(12):3779-85. PMC: 553849. View

17.

Froshauer S, Kartenbeck J, Helenius A . Alphavirus RNA replicase is located on the cytoplasmic surface of endosomes and lysosomes. J Cell Biol. 1988; 107(6 Pt 1):2075-86. PMC: 2115628. DOI: 10.1083/jcb.107.6.2075. View

18.

Baker S, Shieh C, Soe L, Chang M, Vannier D, Lai M . Identification of a domain required for autoproteolytic cleavage of murine coronavirus gene A polyprotein. J Virol. 1989; 63(9):3693-9. PMC: 250960. DOI: 10.1128/JVI.63.9.3693-3699.1989. View

19.

Lee H, Shieh C, Gorbalenya A, Koonin E, La Monica N, Tuler J . The complete sequence (22 kilobases) of murine coronavirus gene 1 encoding the putative proteases and RNA polymerase. Virology. 1991; 180(2):567-82. PMC: 7131164. DOI: 10.1016/0042-6822(91)90071-i. View

20.

Gorbalenya A, Koonin E, Lai M . Putative papain-related thiol proteases of positive-strand RNA viruses. Identification of rubi- and aphthovirus proteases and delineation of a novel conserved domain associated with proteases of rubi-, alpha- and coronaviruses. FEBS Lett. 1991; 288(1-2):201-5. PMC: 7130274. DOI: 10.1016/0014-5793(91)81034-6. View