Murine Coronavirus Spike Protein Determines the Ability of the Virus To Replicate in the Liver and Cause Hepatitis

Navas, Sonia; Seo, Su-Hun; Chua, Ming Ming; Sarma, Jayasri Das; Lavi, Ehud; Hingley, Susan T.; Weiss, Susan R.

doi:10.1128/jvi.75.5.2452-2457.2001

Cited by 77 publications

(103 citation statements)

References 45 publications

(46 reference statements)

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“…Infection of un-injured C57BL/6 female mice with 5 × 10 5 PFU MHV leads to acute hepatitis infection, but all mice survive and recover and this is associated with clearance of virus from the liver to below levels detectable by plaque assay (~200PFU/g tissue) (Eriksson et al, 2008; Navas et al, 2001). In contrast, all mice that received 5 × 10 5 PFU of MHV 1 week following a complete bilateral crush SCI at thoracic level-T3 died by 6 days post-infection (p.i.)…”

Section: Resultsmentioning

confidence: 99%

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Impaired immune responses following spinal cord injury lead to reduced ability to control viral infection

Held

Steward

Blanc

et al. 2010

Experimental Neurology

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Spinal cord injuries disrupt central autonomic pathways that regulate immune function, and increasing evidence suggests that this may cause deficiencies in immune responses in people with spinal cord injuries. Here we analyze the consequences of spinal cord injury (SCI) on immune responses following experimental viral infection of mice. Female C57BL/6 mice received complete crush injuries at either thoracic level 3 (T3) or 9 (T9), and 1 week post-injury, injured mice and un-injured controls were infected with different dosages of mouse hepatitis virus (MHV, a positive-strand RNA virus). Following MHV infection, T3- and T9-injured mice exhibited increased mortality in comparison to un-injured and laminectomy controls. Infection at all dosages resulted in significantly higher viral titer in both T3- and T9-injured mice compared to un-injured controls. Investigation of anti-viral immune responses revealed impairment of cellular infiltration and effector functions in mice with SCI. Specifically, cell-mediated responses were diminished in T3-injured mice, as seen by reduction in virus-specific CD4+ T lymphocyte proliferation and IFN-γ production and decreased numbers of activated antigen presenting cells compared to infected un-injured mice. Collectively, these data indicate that the inability to control viral replication following SCI is not level dependent and that increased susceptibility to infection is due to suppression of both innate and adaptive immune responses.

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Section: Resultsmentioning

confidence: 99%

“…MHV-A59 replicates within the liver, without central nervous system infection, following intraperitoneal (i.p.) injection of C57BL/6 mice (Navas et al, 2001). Age-matched 5- to 7-week-old female C57BL/6 mice (H-2 b background) were purchased from the National Cancer Institute, Bethesda, Maryland, and used for all experiments.…”

Section: Methodsmentioning

confidence: 99%

Impaired immune responses following spinal cord injury lead to reduced ability to control viral infection

Held

Steward

Blanc

et al. 2010

Experimental Neurology

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“…demonstrated that MHV-infected mice contained numerous lesions characteristic of MHV-induced hepatitis, consisting of large confluent areas of hepatocyte necrosis with a dense, mixed acute and chronic inflammatory infiltrate, primarily involving portal tracts (Fig. 6, E and F, arrows) (43,44). Numerous portal venules showed severe endothelialitis with infiltrating lymphocytes.…”

Section: Liver Pathologymentioning

confidence: 99%

Expression of CXC Chemokine Ligand 10 from the Mouse Hepatitis Virus Genome Results in Protection from Viral-Induced Neurological and Liver Disease

Walsh

Edwards

Romero

et al. 2007

The Journal of Immunology

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Using the recombinant murine coronavirus mouse hepatitis virus (MHV) expressing the T cell-chemoattractant CXCL10 (MHV-CXCL10), we demonstrate a potent antiviral role for CXCL10 in host defense. Instillation of MHV-CXCL10 into the CNS of CXCL10-deficient (CXCL10−/−) mice resulted in viral infection and replication in both brain and liver. Expression of virally encoded CXCL10 within the brain protected mice from death and correlated with increased infiltration of T lymphocytes, enhanced IFN-γ secretion, and accelerated viral clearance when compared with mice infected with an isogenic control virus, MHV. Similarly, viral clearance from the livers of MHV-CXCL10-infected mice was accelerated in comparison to MHV-infected mice, yet was independent of enhanced infiltration of T lymphocytes and NK cells. Moreover, CXCL10−/− mice infected with MHV-CXCL10 were protected from severe hepatitis as evidenced by reduced pathology and serum alanine aminotransferase levels compared with MHV-infected mice. CXCL10-mediated protection within the liver was not dependent on CXC-chemokine receptor 2 (CXCR2) signaling as anti-CXCR2 treatment of MHV-CXCL10-infected mice did not modulate viral clearance or liver pathology. In contrast, treatment of MHV-CXCL10-infected CXCL10−/− mice with anti-CXCL10 Ab resulted in increased clinical disease correlating with enhanced viral recovery from the brain and liver as well as increased serum alanine aminotransferase levels. These studies highlight that CXCL10 expression promotes protection from coronavirus-induced neurological and liver disease.

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“…Differences in the S protein, sometimes as few as one or two amino acids, of porcine transmissible gastroenteritis (TGEV) determine whether the virus is enteropathogenic or essentially nonpathogenic in pigs [3,59]. Genetically manipulated MHVs, with different tropisms with regard to disease in the liver and nerve tissue, have tropisms reflective of the strain from the S gene was derived [75,76]. We have shown that the S protein is an important factor with regard to the host cell range of IBV, at least in vitro.…”

Section: Coronavirus Spike Protein As a Determinant Of Pathogenicitymentioning

confidence: 99%

Coronavirus avian infectious bronchitis virus

2007

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-Infectious bronchitis virus (IBV), the coronavirus of the chicken (Gallus gallus), is one of the foremost causes of economic loss within the poultry industry, affecting the performance of both meat-type and egg-laying birds. The virus replicates not only in the epithelium of upper and lower respiratory tract tissues, but also in many tissues along the alimentary tract and elsewhere e.g. kidney, oviduct and testes. It can be detected in both respiratory and faecal material. There is increasing evidence that IBV can infect species of bird other than the chicken. Interestingly breeds of chicken vary with respect to the severity of infection with IBV, which may be related to the immune response. Probably the major reason for the high profile of IBV is the existence of a very large number of serotypes. Both live and inactivated IB vaccines are used extensively, the latter requiring priming by the former. Their effectiveness is diminished by poor cross-protection. The nature of the protective immune response to IBV is poorly understood. What is known is that the surface spike protein, indeed the amino-terminal S1 half, is sufficient to induce good protective immunity. There is increasing evidence that only a few amino acid differences amongst S proteins are sufficient to have a detrimental impact on cross-protection. Experimental vector IB vaccines and genetically manipulated IBVs -with heterologous spike protein genes -have produced promising results, including in the context of in ovo vaccination.

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Murine Coronavirus Spike Protein Determines the Ability of the Virus To Replicate in the Liver and Cause Hepatitis

Cited by 77 publications

References 45 publications

Impaired immune responses following spinal cord injury lead to reduced ability to control viral infection

Impaired immune responses following spinal cord injury lead to reduced ability to control viral infection

Expression of CXC Chemokine Ligand 10 from the Mouse Hepatitis Virus Genome Results in Protection from Viral-Induced Neurological and Liver Disease

Coronavirus avian infectious bronchitis virus

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