Your search keyword '"Sawicki, S."' showing total 13 results

1. Coronavirus transcription: a perspective.

Author

Sawicki SG and Sawicki DL

Subjects

Animals, Mice, Open Reading Frames genetics, Genome, Viral, Murine hepatitis virus genetics, Transcription, Genetic

Abstract

At the VIth International Symposium on Corona and Related Viruses held in Quebec, Canada in 1994 we presented a new model for coronavirus transcription to explain how subgenome-length minus strands, which are used as templates for the synthesis of subgenomic mRNAs, might arise by a process involving discontinuous RNA synthesis. The old model explaining subgenomic mRNA synthesis, which was called leader-primed transcription, was based on erroneous evidence that only genome-length negative strands were present in replicative intermediates. To explain the discovery of subgenome-length minus strands, a related model, called the replicon model, was proposed: The subgenomic mRNAs would be produced initially by leader-primed transcription and then replicated into minus-strand templates that would in turn be transcribed into subgenomic mRNAs. We review the experimental evidence that led us to formulate a third model proposing that the discontinuous event in coronavirus RNA synthesis occurs during minus strand synthesis. With our model the genome is copied both continuously to produce minus-strand templates for genome RNA synthesis and discontinuously to produce minus-strand templates for subgenomic mRNA synthesis, and the subgenomic mRNAs do not function as templates for minus strand synthesis, only the genome does.

Published

2005

2. Mouse hepatitis virus minus-strand templates are unstable and turnover during viral replication.

Author

Wang T and Sawicki SG

Subjects

Animals, Cell Line, Genome, Viral, Mice, Murine hepatitis virus genetics, RNA, Messenger metabolism, Transcription, Genetic, Murine hepatitis virus pathogenicity, Murine hepatitis virus physiology, RNA, Viral biosynthesis, Templates, Genetic, Virus Replication

Published

2001

3. Chromatography of mouse hepatitis virus replicative intermediate and replicative form RNA.

Author

Sawicki DL and Sawicki SG

Subjects

Animals, Cell Line, Centrifugation, Density Gradient, Chromatography, Gel, Mice, Murine hepatitis virus genetics, Murine hepatitis virus metabolism, Ribonucleases metabolism, Murine hepatitis virus chemistry, RNA, Viral biosynthesis, RNA, Viral chemistry

Published

2001

4. Identification of the mutations responsible for the phenotype of three MHV RNA-negative ts mutants.

Author

Siddell S, Sawicki D, Meyer Y, Thiel V, and Sawicki S

Subjects

Animals, Genetic Complementation Test, Mice, Murine hepatitis virus growth & development, Phenotype, Temperature, Murine hepatitis virus genetics, Murine hepatitis virus metabolism, Mutation, RNA, Viral metabolism

Published

2001

5. Selection in persistently infected murine cells of an MHV-A59 variant with extended host range.

Author

Schickli JH, Wentworth DE, Zelus BD, Holmes KV, and Sawicki SG

Subjects

Animals, Cats, Cell Line, Cricetinae, Dogs, Genetic Variation, Mice, Murine hepatitis virus pathogenicity, Rats, Selection, Genetic, Murine hepatitis virus physiology, Virus Latency

Abstract

Murine coronavirus MHV-A59 normally infects only murine cells in vitro and causes transmissible infection only in mice. In the 17 C1 1 line of murine cells, the receptor for MHV-A59 is MHVR, a biliary glycoprotein in the carcinoembryonic antigen (CEA) family of glycoproteins. We found that virus released from the 600th passage of 17 C1 1 cells persistently infected with MHV-A59 (MHV/pi600) replicated in hamster (BHK-21) cells. The virus was passaged and plaque-purified in BHK-21 cells, yielding the MHV/BHK strain. Because murine cells persistently infected with MHV-A59 express a markedly reduced level of MHVR (Sawicki, et al., 1995), we tested whether virus with altered receptor interactions was selected in the persistently infected culture. Infection of 17 C1 1 cells by MHV-A59 can be blocked by treating the cells with anti-MHVR MAb-CC1, while infection by MHV/BHK was only partially blocked by MAb-CC1. MHV/BHK virus was also more resistant than wild-type MHV-A59 to neutralization by purified, recombinant, soluble MHVR glycoprotein (sMHVR). Cells in the persistently infected culture may also express reduced levels of and have altered interactions with some of the Bgp-related glycoproteins that can serve as alternative receptors for MHV-A59. Unlike the parental MHV-A59 which only infects murine cells, MHV/BHK virus was able to infect cell lines derived from mice, hamsters, rats, cats, cows, monkeys and humans. However, MHV/BHK was not able to infect all mammalian species, because a pig (ST) cell line and a dog cell line (MDCK I) were not susceptible to infection. MHV/pi600 and MHV/BHK replicated in murine cells more slowly than MHV-A59 and formed smaller plaques. Thus, in the persistently infected murine cells which expressed a markedly reduced level of MHVR, virus variants were selected that have altered interactions with MHVR and an extended host range. In vivo, in mice infected with coronavirus, virus variants with altered receptor recognition and extended host range might be selected in tissues that have low levels of receptors. Depending upon the tissue in which such a virus variant was selected, it might be shed from the infected animal or eaten by a predator, thus presenting a possible means for initiating the transition of a variant virus into a new host as a model for an emerging virus disease.

Published

1998

6. Negative strand RNA synthesis by temperature-sensitive mutants of mouse hepatitis virus.

Author

Younker DR and Sawicki SG

Subjects

Animals, Mice, Mutation, Temperature, Murine hepatitis virus genetics, RNA, Viral biosynthesis

Abstract

Mutants of the A59 strain of mouse hepatitis virus (MHV) were studied to determine the effects of temperature shift on negative and positive strand RNA synthesis. Mutant LA 9 was originally reported to have a selective temperature sensitive defect in negative strand synthesis. We found that this mutant continued to synthesize negative strands for at least one hour after temperature shift. LA 6 was found to possess a temperature sensitive defect in negative strand synthesis. Following temperature shift, negative strand synthesis rapidly declined. The effect of temperature shift on negative strand synthesis by LA 6 was similar to the effect of cycloheximide treatment of the parental A59 virus. Temperature shift of Alb 16 infected cells did not stop negative strand synthesis but did prevent a corresponding rise in the rate of positive strand synthesis. Therefore, we suggest that Alb 16 is a conversion mutant because it cannot convert newly synthesized negative strands into templates for positive strand synthesis at the nonpermissive temperature.

Published

1998

7. The murine coronavirus mouse hepatitis virus strain A59 from persistently infected murine cells exhibits an extended host range.

Author

Schickli JH, Zelus BD, Wentworth DE, Sawicki SG, and Holmes KV

Subjects

Animals, Antibodies, Monoclonal metabolism, Antibodies, Viral metabolism, Antigens, CD, Cats, Cattle, Cell Adhesion Molecules, Cell Line, Cell Line, Transformed, Chlorocebus aethiops, Cricetinae, Dogs, Glycoproteins metabolism, HeLa Cells, Hemagglutinins, Viral biosynthesis, Humans, Mice, Murine hepatitis virus isolation & purification, Murine hepatitis virus metabolism, Murine hepatitis virus physiology, Neutralization Tests, Nucleocapsid biosynthesis, RNA, Viral biosynthesis, Rats, Recombinant Proteins metabolism, Solubility, Swine, Time Factors, Vero Cells, Viral Proteins biosynthesis, Murine hepatitis virus pathogenicity, Viral Fusion Proteins, Virus Latency

Abstract

In murine 17 Cl 1 cells persistently infected with murine coronavirus mouse hepatitis virus strain A59 (MHV-A59), expression of the virus receptor glycoprotein MHVR was markedly reduced (S. G. Sawicki, J. H. Lu, and K. V. Holmes, J. Virol. 69:5535-5543, 1995). Virus isolated from passage 600 of the persistently infected cells made smaller plaques on 17 Cl 1 cells than did MHV-A59. Unlike the parental MHV-A59, this variant virus also infected the BHK-21 (BHK) line of hamster cells. Virus plaque purified on BHK cells (MHV/BHK) grew more slowly in murine cells than did MHV-A59, and the rate of viral RNA synthesis was lower and the development of the viral nucleocapsid (N) protein was slower than those of MHV-A59. MHV/BHK was 100-fold more resistant to neutralization with the purified soluble recombinant MHV receptor glycoprotein (sMHVR) than was MHV-A59. Pretreatment of 17 Cl 1 cells with anti-MHVR monoclonal antibody CC1 protected the cells from infection with MHV-A59 but only partially protected them from infection with MHV/BHK. Thus, although MHV/BHK could still utilize MHVR as a receptor, its interactions with the receptor were significantly different from those of MHV-A59. To determine whether a hemagglutinin esterase (HE) glycoprotein that could bind the virions to 9-O-acetylated neuraminic acid moieties on the cell surface was expressed by MHV/BHK, an in situ esterase assay was used. No expression of HE activity was detected in 17 Cl 1 cells infected with MHV/BHK, suggesting that this virus, like MHV-A59, bound to cell membranes via its S glycoprotein. MHV/BHK was able to infect cell lines from many mammalian species, including murine (17 Cl 1), hamster (BHK), feline (Fcwf), bovine (MDBK), rat (RIE), monkey (Vero), and human (L132 and HeLa) cell lines. MHV/BHK could not infect dog kidney (MDCK I) or swine testis (ST) cell lines. Thus, in persistently infected murine cell lines that express very low levels of virus receptor MHVR and which also have and may express alternative virus receptors of lesser efficiency, there is a strong selective advantage for virus with altered interactions with receptor (D. S. Chen, M. Asanaka, F. S. Chen, J. E. Shively, and M. M. C. Lai, J. Virol. 71:1688-1691, 1997; D. S. Chen, M. Asanaka, K. Yokomori, F.-I. Wang, S. B. Hwang, H.-P. Li, and M. M. C. Lai, Proc. Natl. Acad. Sci. USA 92:12095-12099, 1995; P. Nedellec, G. S. Dveksler, E. Daniels, C. Turbide, B. Chow, A. A. Basile, K. V. Holmes, and N. Beauchemin, J. Virol. 68:4525-4537, 1994). Possibly, in coronavirus-infected animals, replication of the virus in tissues that express low levels of receptor might also select viruses with altered receptor recognition and extended host range.

Published

1997

8. Persistent infection of cultured cells with mouse hepatitis virus (MHV) results from the epigenetic expression of the MHV receptor.

Author

Sawicki SG, Lu JH, and Holmes KV

Subjects

3T3 Cells, Animals, Antibodies, Monoclonal pharmacology, Cell Adhesion Molecules, Clone Cells, Disease Susceptibility, Flow Cytometry, Glycoproteins biosynthesis, Mice, Mice, Inbred BALB C, Murine hepatitis virus pathogenicity, Receptors, Virus biosynthesis, Semliki forest virus physiology, Species Specificity, Vesicular stomatitis Indiana virus physiology, Glycoproteins physiology, Murine hepatitis virus physiology, Receptors, Virus physiology, Virus Replication

Abstract

The A59 strain of murine coronavirus mouse hepatitis virus (MHV) can cause persistent infection of 17C1-1 cells and other murine cell lines. Persistently infected cultures released large amounts of virus (10(7) to 10(8) PFU/ml) and were resistant to superinfection with MHV but not to infection with unrelated Semliki Forest and vesicular stomatitis viruses. The culture medium from persistently infected cultures did not contain a soluble inhibitor such as interferon that protected uninfected cells from infection by MHV or vesicular stomatitis virus. The persistent infection was cured if fewer than 100 cells were transferred during subculturing, and such cured cultures were susceptible to reinfection and the reestablishment of persistent infection. Cultures of 17C1-1 cells that had been newly cloned from single cells consisted of a mixture of MHV-resistant and -susceptible cells. 17C1-1/#97 cells, which were cured by subcloning after 97 passages of a persistently infected culture over a 1-year period, contained 5 to 10% of their population as susceptible cells, while 17C1-1/#402 cells, which were cured by subcloning after 402 passages over a 3-year period, had less than 1% susceptible cells. Susceptibility to infection correlated with the expression of MHV receptor glycoprotein (MHVR [Bgp1a]). Fluorescence-activated cell sorter analysis with antibody to MHVR showed that 17C1-1/#97 cells contained a small fraction of MHVR-expressing cells. These MHVR-expressing cells were selectively eliminated within 24 h after challenge with MHV-A59, and pretreatment of 17C1-1/#97 cells with monoclonal antibody CC1, which binds to the N-terminal domain of MHVR, blocked infection. We conclude that the subpopulation of MHVR-expressing cells were infected and killed in acutely or persistently infected cultures, while the subpopulation of MHVR-nonexpressing cells survived and proliferated. The subpopulation of MHVR-negative cells produced a small proportion of progeny cells that expressed MHVR and became infected, thereby maintaining the persistent infection as a steady-state carrier culture. Thus, in 17C1-1 cell cultures, the unstable or epigenetic expression of MHVR permitted the establishment of a persistent, chronic infection.

Published

1995

9. Coronavirus transcription: subgenomic mouse hepatitis virus replicative intermediates function in RNA synthesis.

Author

Sawicki SG and Sawicki DL

Subjects

Animals, Cell Line, Clone Cells, Kinetics, Mice, RNA, Viral biosynthesis, RNA, Viral isolation & purification, Genes, Viral, Murine hepatitis virus genetics, RNA, Viral genetics, Transcription, Genetic

Abstract

Both genomic and subgenomic replicative intermediates (RIs) and replicative-form (RF) structures were found in 17CL1 mouse cells that had been infected with the A59 strain of mouse hepatitis virus (MHV), a prototypic coronavirus. Seven species of RNase-resistant RF RNAs, whose sizes were consistent with the fact that each was derived from an RI that was engaged in the synthesis of one of the seven MHV positive-strand RNAs, were produced by treatment with RNase A. Because the radiolabeling of the seven RF RNAs was proportional to that of the corresponding seven positive-strand RNAs, the relative rate of synthesis of each of the MHV positive-strand RNAs may be controlled by the relative number of each of the size classes of RIs that are produced. In contrast to alphavirus, which produced its subgenome-length RF RNAs from genome-length RIs, MHV RF RNAs were derived from genome- and subgenome-length RIs. Only the three largest MHV RF RNAs (RFI, RFII, and RFIII) were derived from the RIs that migrated slowest on agarose gels. The four smallest RF RNAs (RFIV, RFV, RFVI, and RFVII) were derived from RIs that migrated in a broad region of the gel that extended from the position of 28S rRNA to the position of the viral single-stranded MHV mRNA-3. Because all seven RIs were labeled during very short pulses with [3H]uridine, we concluded that the subgenome-length RIs are transcriptionally active. These findings, with the recent report of the presence of subgenome-length negative-strand RNAs in cells infected with porcine transmissible gastroenteritis virus (P. B. Sethna, S.-L. Hung, and D. A. Brian, Proc. Natl. Acad. Sci. USA 86: 5626-5630, 1989), strongly suggest that coronaviruses utilize a novel replication strategy that employs the synthesis of subgenomic negative strands to produce subgenomic mRNAs.

Published

1990

10. Characterization of a small plaque mutant of the A59 strain of mouse hepatitis virus defective in cell fusion.

Author

Sawicki SG

Subjects

Animals, Binding Sites, Cell Fusion, Cell Line, Genes, Viral, Molecular Weight, Murine hepatitis virus metabolism, Mutation, RNA, Viral biosynthesis, RNA, Viral genetics, Trypsin, Viral Fusion Proteins isolation & purification, Viral Fusion Proteins metabolism, Murine hepatitis virus genetics, Viral Fusion Proteins genetics

Published

1987

11. Coronavirus minus-strand RNA synthesis and effect of cycloheximide on coronavirus RNA synthesis.

Author

Sawicki SG and Sawicki DL

Subjects

Animals, Cell Fusion, Cell Line, Depression, Chemical, Hydrogen-Ion Concentration, Mice, Murine hepatitis virus drug effects, Murine hepatitis virus physiology, RNA-Dependent RNA Polymerase metabolism, RNA-Dependent RNA Polymerase physiology, Time Factors, Viral Proteins metabolism, Viral Proteins physiology, Virus Replication, Cycloheximide pharmacology, Murine hepatitis virus metabolism, Poly A biosynthesis, RNA, Messenger biosynthesis, RNA, Viral biosynthesis

Abstract

The temporal sequence of coronavirus plus-strand and minus-strand RNA synthesis was determined in 17CL1 cells infected with the A59 strain of mouse hepatitis virus (MHV). MHV-induced fusion was prevented by keeping the pH of the medium below pH 6.8. This had no effect on the MHV replication cycle, but gave 5- to 10-fold-greater titers of infectious virus and delayed the detachment of cells from the monolayer which permitted viral RNA synthesis to be studied conveniently until at least 10 h postinfection. Seven species of poly(A)-containing viral RNAs were synthesized at early and late times after infection, in nonequal but constant ratios. MHV minus-strand RNA synthesis was first detected at about 3 h after infection and was found exclusively in the viral replicative intermediates and was not detected in 60S single-stranded form in infected cells. Early in the replication cycle, from 45 to 65% of the [3H]uridine pulse-labeled RF core of purified MHV replicative intermediates was in minus-strand RNA. The rate of minus-strand synthesis peaked at 5 to 6 h postinfection and then declined to about 20% of the maximum rate. The addition of cycloheximide before 3 h postinfection prevented viral RNA synthesis, whereas the addition of cycloheximide after viral RNA synthesis had begun resulted in the inhibition of viral RNA synthesis. The synthesis of both genome and subgenomic mRNAs and of viral minus strands required continued protein synthesis, and minus-strand RNA synthesis was three- to fourfold more sensitive to inhibition by cycloheximide than was plus-strand synthesis.

Published

1986

12. Temperature-sensitive mutants of MHV-A59.

Author

Sturman LS, Eastwood C, Frana MF, Duchala C, Baker F, Ricard CS, Sawicki SG, and Holmes KV

Subjects

Animals, Cell Line, Genes, Viral, Mutation, Phenotype, Temperature, Viral Proteins genetics, Viral Structural Proteins, Virus Replication, Murine hepatitis virus genetics

Published

1987

13. Identification of the mutations responsible for the phenotype of three MHV RNA-negative ts mutants

Author

Siddell S, Sawicki D, Meyer Y, Volker Thiel, and Sawicki S

Subjects

Mice, Murine hepatitis virus, Phenotype, Genetic Complementation Test, Mutation, Temperature, Animals, RNA, Viral