In vivo expression of inducible nitric oxide synthase in experimentally induced neurologic diseases.

Koprowski, Hilary; Zheng, Yun‐Min; Heber‐Katz, Ellen; Fraser, Nigel W.; Rorke, Lucy B.; Fu, Zhen F.; Hanlon, Cathleen A.; Dietzschold, Bernhard

doi:10.1073/pnas.90.7.3024

Cited by 438 publications

(256 citation statements)

References 23 publications

(18 reference statements)

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“…It is possible that cytokine expression may modulate rabies viral production in the central nervous system as suggested by others in animalbased studies, as well as contributing directly to the neuropathogenesis of the infectious process. [7][8][9][10] It follows that inhibition of cytokine expression may have some therapeutic potential in this otherwise fatal disease, as has been demonstrated in a murine model; 9 this clearly awaits further study in humans. To our knowledge, this study is the first to document the histologic relationship of direct infection of rabies virus with expression of TNFa and iNOS in people using an in situ-based assay.…”

Section: Discussionmentioning

confidence: 97%

“…However, despite the relatively paucicellular response in the central nervous system to the infection, there was massive upregulation of both TNFa and iNOS, each of which can damage neurons and supporting tissue. 7,[10][11][12] This suggests a multifactorial pathogenic process for rabies encephalitis that includes widespread viral infection and concomitant increased expression of a variety of cellular factors as well as downregulation of SOCS expression. It is possible that cytokine expression may modulate rabies viral production in the central nervous system as suggested by others in animalbased studies, as well as contributing directly to the neuropathogenesis of the infectious process.…”

Section: Discussionmentioning

confidence: 99%

“…Rabies-induced synthesis of inducible nitric oxide (iNOS) in the central nervous system has been suggested as a pathogenetic step in neuronal cell damage in rabies infections. 6,7 Tumor necrosis factor a (TNFa) expression has also been suggested as an important factor in rabies encephalitis, both in terms of direct toxicity and as modulating viral production. [8][9][10] However, the studies on TNFa and iNOS expression have been done on animal models, and it is not clear if these data can be extrapolated to human rabies.…”

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confidence: 99%

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Molecular detection of rabies encephalitis and correlation with cytokine expression

et al. 2005

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The purposes of this study were to elucidate the role of cytokine upregulation in the pathogenesis of rabies encephalitis and to compare the detection of Negri bodies with that of rabies protein by immunohistochemistry and rabies RNA by reverse transcriptase (RT) in situ PCR for its diagnosis. Negri bodies were evident in 4/7 of the documented rabies cases; viral protein and viral RNA were detected in each case. The average number of rabies-infected cells, determined by counting 150 neurons in serial sections in areas where viral protein was evident, with the three different detection methods was: Negri bodies (o1/150), immunohistochemistry (4/150), and RT in situ PCR (49/150). No rabies protein or RNA was detected in four control brain tissues that were read with the rabies cases in a blinded fashion. The ratio of cells expressing tumor necrosis factor a (TNFa) or inducible nitric oxide synthetase (iNOS) to 1 SSI-1/SOCS-1 (suppressors of cytokine signaling) expression, which is a novel class of negative feedback regulators of cytokine receptor signaling, was markedly increased only in the areas where many viral infected cells were present. Colabeling experiments showed that most of the cells expressing iNOS or TNFa were not virally infected, but rather adjacent to rabies-infected neurons. We conclude that RT in situ PCR for rabies virus is the most accurate test for the determination of viral load in rabies encephalitis. Further, the disease is characterized by massive viral infection of neurons in a markedly focal distribution in conjunction with a concomitant upregulation of cytokine expression in adjacent, noninfected cells that may be due, in part, to SOCS downregulation.

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Section: Discussionmentioning

confidence: 97%

Section: Discussionmentioning

confidence: 99%

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confidence: 99%

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Molecular detection of rabies encephalitis and correlation with cytokine expression

et al. 2005

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“…In addition to MBP-specific lymphocytes, activated monocytes expressing iNOS have been implicated in the development of EAE in conventional models (eg., 3,5,8,11) where disease pathogenesis has been associated with CNS inflammation and nitrotyrosine formation (eg., 3, 5). Therefore, we have assessed the effects of UA treatment on the distribution of iNOS-positive cells in PLSJL mice immunized with MBP.…”

Section: Effects Of Ua On the Immune Response To Mbpmentioning

confidence: 99%

The Peroxynitrite Scavenger Uric Acid Prevents Inflammatory Cell Invasion into the Central Nervous System in Experimental Allergic Encephalomyelitis through Maintenance of Blood-Central Nervous System Barrier Integrity

Kean

Spitsin

Mikheeva

et al. 2000

The Journal of Immunology

143

113

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Uric acid (UA), a product of purine metabolism, is a known scavenger of peroxynitrite (ONOO−), which has been implicated in the pathogenesis of multiple sclerosis and experimental allergic encephalomyelitis (EAE). To determine whether the known therapeutic action of UA in EAE is mediated through its capacity to inactivate ONOO− or some other immunoregulatory phenomenon, the effects of UA on Ag presentation, T cell reactivity, Ab production, and evidence of CNS inflammation were assessed. The inclusion of physiological levels of UA in culture effectively inhibited ONOO−-mediated oxidation as well as tyrosine nitration, which has been associated with damage in EAE and multiple sclerosis, but had no inhibitory effect on the T cell-proliferative response to myelin basic protein (MBP) or on APC function. In addition, UA treatment was found to have no notable effect on the development of the immune response to MBP in vivo, as measured by the production of MBP-specific Ab and the induction of MBP-specific T cells. The appearance of cells expressing mRNA for inducible NO synthase in the circulation of MBP-immunized mice was also unaffected by UA treatment. However, in UA-treated animals, the blood-CNS barrier breakdown normally associated with EAE did not occur, and inducible NO synthase-positive cells most often failed to reach CNS tissue. These findings are consistent with the notion that UA is therapeutic in EAE by inactivating ONOO−, or a related molecule, which is produced by activated monocytes and contributes to both enhanced blood-CNS barrier permeability as well as CNS tissue pathology.

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“…Others have demonstrated dysfunction of ion channels in infected cell culture [97], and defective cholinergic neurotransmission [98]. Induction of inducible nitric oxide synthase mRNA and increased levels of nitric oxide have been demonstrated in rodents inoculated with the virus [96,97,99,100]. The role of these in natural rabies infection in humans is uncertain.…”

Section: Bat Rabiesmentioning

confidence: 99%

Perspectives in Diagnosis and Treatment of Rabies Viral Encephalitis: Insights from Pathogenesis

et al. 2016

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Rabies viral encephalitis, though one of the oldest recognized infectious disease of humans, remains an incurable, fatal encephalomyelitis, despite advances in understanding of its pathobiology. Advances in science have led us on the trail of the virus in the host, but the sanctuaries in which the virus remains hidden for its survival are unknown. Insights into host-pathogen interactions have facilitated evolving immunologic therapeutic strategies, though we are far from a cure. Most of the present-day knowledge has evolved from in vitro studies using fixed (attenuated) laboratory strains that may not be applicable in the clinical setting. Much remains to be unraveled about this elusive virus. This review attempts to re-examine the current advances in understanding of the pathobiology of the rabies virus that modulate the diagnosis, treatment, and prevention of this fatal disease.

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In vivo expression of inducible nitric oxide synthase in experimentally induced neurologic diseases.

Cited by 438 publications

References 23 publications

Molecular detection of rabies encephalitis and correlation with cytokine expression

Molecular detection of rabies encephalitis and correlation with cytokine expression

The Peroxynitrite Scavenger Uric Acid Prevents Inflammatory Cell Invasion into the Central Nervous System in Experimental Allergic Encephalomyelitis through Maintenance of Blood-Central Nervous System Barrier Integrity

Perspectives in Diagnosis and Treatment of Rabies Viral Encephalitis: Insights from Pathogenesis

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