Protective role of interferon against cytotoxcicity induced by rabies virus in mice

Tohamy, Amany A.; Fahmy, Ali; Dkhil, Mohamed A.; Diab, Mohammad

doi:10.5897/ajb09.1568

Cited by 4 publications

(4 citation statements)

References 37 publications

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“…The increased survival rate and reduced cytogenetic changes suggest that protection induced by interferon against rabies virus activity could be, at least partially, attributable to blockage of the replication of CVS strain of rabies virus. [12] Similar observation was reported from study involving monkeys infected with rabies virus when administered by repeated intramuscular administration of human leukocyte interferon beginning 24 h after infection. [7] Bosko Postic et al, showed simultaneous inoculation of interferon and street rabies in rabbit in opposite hind limbs decreased the mortality but interferon in vitro failed to neutralise rabies virus.…”

Section: Discussionsupporting

confidence: 83%

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A preliminary study of recombinant human interferon-α-2a activity against rabies virus in murine model

Roy

Patil

Ghadigaonkar

et al. 2015

Indian Journal of Medical Microbiology

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Rabies remains an important public health problem in the world due to uncontrolled enzootic rabies. Although rabies associated fatalities may be prevented with timely immunoprophylaxis, but till date a therapeutic molecule has remained elusive. We investigated the role of rhuIFN α-2a in murine model challenged with rabies virus. Titre of 10(4.25) LD50/0.03 ml of 10% w/v RV CVS stock suspension were obtained. Based on 1LD50 titre, challenge dose of 50 LD 50 was administered along with rhuIFN α-2a with pre-exposure (primed) and post-exposure with the rabies virus. Both showed increased survival time as compared with the virus controls. These findings suggest that the rhuIFN α-2a might have some anti-viral activity, which can be used for the treatment of rabies infection. Further research on the efficacy of interferon along with anti-viral drugs for the treatment will be helpful in designing combination therapy against the disease.

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Section: Discussionsupporting

confidence: 83%

“…The infected Swiss albino mice were observed for mortality upto 21 days. [12] The pre-exposure and post-exposure treatments of rhuIFN α-2a challenged with RV CVS were repeated in triplicate. All the infectious work was carried out in Biosafety level-2 cabinet.…”

Section: Pre-exposure and Post-exposure Treatmentsmentioning

confidence: 99%

A preliminary study of recombinant human interferon-α-2a activity against rabies virus in murine model

Roy

Patil

Ghadigaonkar

et al. 2015

Indian Journal of Medical Microbiology

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“…Our results were similar to that reported by Tohamy et al, where pre treatment of mice with IFN, 24 h before infection delayed the onset of specific rabies signs [31]. Therefore, based on development of characteristic signs of illness in the pre-exposure and post-exposure groups, we speculated that priming with interferon in the pre-exposure group can lead to local production of cytokines and recruitment of lymphocytes.…”

Section: Discussionsupporting

confidence: 81%

“…However, the mechanism behind the reported protective activity of exogenous interferon is not clear. Recently Tohamy et al, demonstrated that pretreating rabies infected mice with interferon significantly reduced cytogenetic changes [31]. These reports formed the basis of the present study which is an attempt to investigate the role of recombinant human interferon alpha (rhIFN a-2A) on prognosis and expression of innate immunity cytokines during rabies infection.…”

Section: Introductionmentioning

confidence: 95%

Exogenous interferon prolongs survival of rabies infected mice

et al. 2015

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Rabies is an acute viral infection that causes encephalomyelitis in almost all warm blooded animals and is invariably fatal once the clinical signs appear. The present study was carried out to assess the effect of recombinant human interferon alpha (rhIFN a-2A) treatment on the survival of rabies infected mice and its correlation with cytokines expression. The gene expression of TNF-a and IL-6 was measured by SYBR Green Real Time PCR for two groups-''Pre-exposure'' (mice were inoculated with rhIFN a-2A prior to rabies infection) and ''Post-exposure'' (mice were inoculated with rhIFN a-2A post rabies virus infection). Delayed mortality was observed in interferon treated infected groups. In addition, statistically significant decrease (P \ 0.0001) in the expression of TNF-a and IL-6 was observed, both in the pre-exposure and post-exposure groups. These findings indicate that modulation of cytokine secretion using exogenous biologicals such as rhIFN may offer novel therapeutic approaches to treat diseases such as rabies.

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