NS2 is Required for Efficient Translation of Viral MRNA in Minute Virus of Mice-infected Murine Cells

Overview

Journal J Virol

Publisher American Society for Microbiology

Date 1993 Feb 1

PMID 8419637

Citations 31

Authors

L K Naeger

N Salome

D J Pintel

Affiliations

Soon will be listed here.

Abstract

Detailed analysis of five NS2 mutants of the autonomous parvovirus minute virus of mice (MVMp) has revealed the following. At low multiplicities of infection, NS2 mutants killed NB324K cells as well as wild-type (wt) MVM did and grew to high titers, while in contrast they grew poorly and did not readily kill murine A9 cells. Following CaPO4 transfection of murine fibroblasts, NS2 mutant infectious clones generated approximately 10-fold less monomer replicative-form DNA than wt and no detectable progeny single-stranded DNA. On nonmurine semipermissive NB324K cells, however, these mutant plasmid clones generated near wt levels of all replicative DNA forms. After infection of highly synchronized murine fibroblasts by NS2 mutant virus at inputs equivalent to those of the wt, mutant monomer replicative-form DNA was decreased 5- to 10-fold compared with that of the wt, and progeny single-stranded DNA accumulation was decreased to an even greater extent. Both total and cytoplasmic NS2 mutant RNA was decreased, but the amount of total viral mRNA generated, relative to accumulated viral DNA in the same experiments, was similar to that seen in wt infection. The accumulation of virus-generated proteins was also decreased in NS2 mutant infection; however, the magnitude of this decrease, compared with that of wt infections, was significantly greater than the concomitant decrease in mutant-generated levels of accumulated cytoplasmic RNA, and this effect was most dramatic for VP2. There was no such disparity between the relative accumulation of mutant-generated RNA and protein in cells permissive for the growth of these mutants. These results suggest that translation of MVM viral RNA is specifically reduced in NS2 mutant infection of restrictive cells. Because the affected viral proteins are required for the efficient production of viral replicative DNA forms, these results reveal a fundamental, although perhaps not the only, role for NS2 in parvovirus infection.

Citing Articles

Parvovirus nonstructural protein 2 interacts with chromatin-regulating cellular proteins.

Mattola S, Salokas K, Aho V, Mantyla E, Salminen S, Hakanen S PLoS Pathog. 2022; 18(4):e1010353.

PMID: 35395063 PMC: 9020740. DOI: 10.1371/journal.ppat.1010353.

Concepts to Reveal Parvovirus-Nucleus Interactions.

Mattola S, Hakanen S, Salminen S, Aho V, Mantyla E, Ihalainen T Viruses. 2021; 13(7).

PMID: 34372512 PMC: 8310053. DOI: 10.3390/v13071306.

Mutations in the Non-Structural Protein-Coding Sequence of Protoparvovirus H-1PV Enhance the Fitness of the Virus and Show Key Benefits Regarding the Transduction Efficiency of Derived Vectors.

Hashemi H, Condurat A, Stroh-Dege A, Weiss N, Geiss C, Pilet J Viruses. 2018; 10(4).

PMID: 29584637 PMC: 5923444. DOI: 10.3390/v10040150.

Minute Virus of Canines NP1 Protein Governs the Expression of a Subset of Essential Nonstructural Proteins via Its Role in RNA Processing.

Fasina O, Stupps S, Figueroa-Cuilan W, Pintel D J Virol. 2017; 91(12).

PMID: 28356522 PMC: 5446662. DOI: 10.1128/JVI.00260-17.

Complementation for an essential ancillary non-structural protein function across parvovirus genera.

Mihaylov I, Cotmore S, Tattersall P Virology. 2014; 468-470:226-237.

PMID: 25194919 PMC: 4254310. DOI: 10.1016/j.virol.2014.07.043.

References

Reichel P, Merrick W, Siekierka J, Mathews M . Regulation of a protein synthesis initiation factor by adenovirus virus-associated RNA. Nature. 1985; 313(5999):196-200. DOI: 10.1038/313196a0. View

Clemens K, Pintel D . The two transcription units of the autonomous parvovirus minute virus of mice are transcribed in a temporal order. J Virol. 1988; 62(4):1448-51. PMC: 253160. DOI: 10.1128/JVI.62.4.1448-1451.1988. View

Nishioka Y, Silverstein S . Degradation of cellular mRNA during infection by herpes simplex virus. Proc Natl Acad Sci U S A. 1977; 74(6):2370-4. PMC: 432173. DOI: 10.1073/pnas.74.6.2370. View

Hirt B . Selective extraction of polyoma DNA from infected mouse cell cultures. J Mol Biol. 1967; 26(2):365-9. DOI: 10.1016/0022-2836(67)90307-5. View

Etchison D, Milburn S, Edery I, Sonenberg N, Hershey J . Inhibition of HeLa cell protein synthesis following poliovirus infection correlates with the proteolysis of a 220,000-dalton polypeptide associated with eucaryotic initiation factor 3 and a cap binding protein complex. J Biol Chem. 1982; 257(24):14806-10. View

Cater J, Pintel D . The small non-structural protein NS2 of the autonomous parvovirus minute virus of mice is required for virus growth in murine cells. J Gen Virol. 1992; 73 ( Pt 7):1839-43. DOI: 10.1099/0022-1317-73-7-1839. View

Naeger L, Schoborg R, Zhao Q, Tullis G, Pintel D . Nonsense mutations inhibit splicing of MVM RNA in cis when they interrupt the reading frame of either exon of the final spliced product. Genes Dev. 1992; 6(6):1107-19. DOI: 10.1101/gad.6.6.1107. View

BOUCK N, DI MAYORCA G . Somatic mutation as the basis for malignant transformation of BHK cells by chemical carcinogens. Nature. 1976; 264(5588):722-7. DOI: 10.1038/264722a0. View

Lloyd R, Toyoda H, Etchison D, Wimmer E, EHRENFELD E . Cleavage of the cap binding protein complex polypeptide p220 is not effected by the second poliovirus protease 2A. Virology. 1986; 150(1):299-303. DOI: 10.1016/0042-6822(86)90291-6. View

10.

Naeger L, Cater J, Pintel D . The small nonstructural protein (NS2) of the parvovirus minute virus of mice is required for efficient DNA replication and infectious virus production in a cell-type-specific manner. J Virol. 1990; 64(12):6166-75. PMC: 248791. DOI: 10.1128/JVI.64.12.6166-6175.1990. View

11.

Caillet-Fauquet P, Perros M, Brandenburger A, Spegelaere P, Rommelaere J . Programmed killing of human cells by means of an inducible clone of parvoviral genes encoding non-structural proteins. EMBO J. 1990; 9(9):2989-95. PMC: 552016. DOI: 10.1002/j.1460-2075.1990.tb07491.x. View

12.

Rice A, Roberts B . Vaccinia virus induces cellular mRNA degradation. J Virol. 1983; 47(3):529-39. PMC: 255294. DOI: 10.1128/JVI.47.3.529-539.1983. View

13.

Bernstein H, Sonenberg N, Baltimore D . Poliovirus mutant that does not selectively inhibit host cell protein synthesis. Mol Cell Biol. 1985; 5(11):2913-23. PMC: 369102. DOI: 10.1128/mcb.5.11.2913-2923.1985. View

14.

Fenwick M, McMenamin M . Early virion-associated suppression of cellular protein synthesis by herpes simplex virus is accompanied by inactivation of mRNA. J Gen Virol. 1984; 65 ( Pt 7):1225-8. DOI: 10.1099/0022-1317-65-7-1225. View

15.

Cotmore S, Tattersall P . Organization of nonstructural genes of the autonomous parvovirus minute virus of mice. J Virol. 1986; 58(3):724-32. PMC: 252977. DOI: 10.1128/JVI.58.3.724-732.1986. View

16.

Cotmore S, Tattersall P . The autonomously replicating parvoviruses of vertebrates. Adv Virus Res. 1987; 33:91-174. DOI: 10.1016/s0065-3527(08)60317-6. View

17.

Siekierka J, Mariano T, Reichel P, Mathews M . Translational control by adenovirus: lack of virus-associated RNAI during adenovirus infection results in phosphorylation of initiation factor eIF-2 and inhibition of protein synthesis. Proc Natl Acad Sci U S A. 1985; 82(7):1959-63. PMC: 397459. DOI: 10.1073/pnas.82.7.1959. View

18.

Schneider R, Shenk T . Impact of virus infection on host cell protein synthesis. Annu Rev Biochem. 1987; 56:317-32. DOI: 10.1146/annurev.bi.56.070187.001533. View

19.

Pedrali-Noy G, Spadari S, Miller-Faures A, Miller A, Kruppa J, Koch G . Synchronization of HeLa cell cultures by inhibition of DNA polymerase alpha with aphidicolin. Nucleic Acids Res. 1980; 8(2):377-87. PMC: 327273. DOI: 10.1093/nar/8.2.377. View

20.

MARTIN P, Henry C, Ferre F, Duterque-Coquillaud M, Lagrou C, Ghysdael J . Transformation of quail embryo fibroblasts by a retrovirus carrying a normal human c-myc gene. EMBO J. 1986; 5(7):1529-33. PMC: 1166976. DOI: 10.1002/j.1460-2075.1986.tb04393.x. View