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AN ANTIVIRAL SUBSTANCE FROM PENICILLIUM FUNICULOSUM : IV. INQUIRY INTO THE MECHANISM BY WHICH HELENINE EXERTS ITS ANTIVIRAL EFFECT

1. Helenine injected intraperitoneally 24 hr prior to a regularly fatal dose of Semliki Forest virus saves most of the mice to which it is administered. 2. Mice saved by helenine develop no viral immunity and regularly succumb when rechallenged 2 wk later with the same dose of virus from which they...

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Autor principal: Shope, Richard E.
Formato: Texto
Lenguaje:English
Publicado: The Rockefeller University Press 1966
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2138137/
https://www.ncbi.nlm.nih.gov/pubmed/5905239
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author Shope, Richard E.
author_facet Shope, Richard E.
author_sort Shope, Richard E.
collection PubMed
description 1. Helenine injected intraperitoneally 24 hr prior to a regularly fatal dose of Semliki Forest virus saves most of the mice to which it is administered. 2. Mice saved by helenine develop no viral immunity and regularly succumb when rechallenged 2 wk later with the same dose of virus from which they were originally saved. 3. The time during which helenine is optimally effective in protecting mice from death by Semliki Forest virus covers a period of approximately 36 hr beginning after about 12 hr and extending to 48 hr before virus infection. When periods of less than 12 hr, or more than 48 hr, elapse between the time of helenine administration and virus inoculation, its protective effectiveness diminishes progressively. 4. Repeated injections of helenine at 2- or 3-day intervals, if continued long enough, exhaust the capacity of a host to respond favorably to helenine administered 24 hr before virus inoculation. 5. Helenine injections at intervals of 4, 3, and 2 wk before its administration 24 hr prior to infection do not decrease the effectiveness of this final dose in protecting mice from fatal infection by the virus. The experimental results here reported indicate that, as suggested by the findings of earlier work, helenine does not act directly as an antiviral substance, but instead exerts its effect through some substance that it induces the host to elaborate. The nature of this induced antiviral substance is as yet unknown though, to judge from the failure of spared mice to acquire viral immunity, it appears to act at a stage in viral replication prior to that at which antigenic viral protein is produced. The findings with helenine and those thus far reported for interferon afford no factual basis for judging the relationship of the two, if any.
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spelling pubmed-21381372008-04-17 AN ANTIVIRAL SUBSTANCE FROM PENICILLIUM FUNICULOSUM : IV. INQUIRY INTO THE MECHANISM BY WHICH HELENINE EXERTS ITS ANTIVIRAL EFFECT Shope, Richard E. J Exp Med Article 1. Helenine injected intraperitoneally 24 hr prior to a regularly fatal dose of Semliki Forest virus saves most of the mice to which it is administered. 2. Mice saved by helenine develop no viral immunity and regularly succumb when rechallenged 2 wk later with the same dose of virus from which they were originally saved. 3. The time during which helenine is optimally effective in protecting mice from death by Semliki Forest virus covers a period of approximately 36 hr beginning after about 12 hr and extending to 48 hr before virus infection. When periods of less than 12 hr, or more than 48 hr, elapse between the time of helenine administration and virus inoculation, its protective effectiveness diminishes progressively. 4. Repeated injections of helenine at 2- or 3-day intervals, if continued long enough, exhaust the capacity of a host to respond favorably to helenine administered 24 hr before virus inoculation. 5. Helenine injections at intervals of 4, 3, and 2 wk before its administration 24 hr prior to infection do not decrease the effectiveness of this final dose in protecting mice from fatal infection by the virus. The experimental results here reported indicate that, as suggested by the findings of earlier work, helenine does not act directly as an antiviral substance, but instead exerts its effect through some substance that it induces the host to elaborate. The nature of this induced antiviral substance is as yet unknown though, to judge from the failure of spared mice to acquire viral immunity, it appears to act at a stage in viral replication prior to that at which antigenic viral protein is produced. The findings with helenine and those thus far reported for interferon afford no factual basis for judging the relationship of the two, if any. The Rockefeller University Press 1966-01-31 /pmc/articles/PMC2138137/ /pubmed/5905239 Text en Copyright © 1966 by The Rockefeller University Press This article is distributed under the terms of an Attribution–Noncommercial–Share Alike–No Mirror Sites license for the first six months after the publication date (see http://www.rupress.org/terms). After six months it is available under a Creative Commons License (Attribution–Noncommercial–Share Alike 4.0 Unported license, as described at http://creativecommons.org/licenses/by-nc-sa/4.0/).
spellingShingle Article
Shope, Richard E.
AN ANTIVIRAL SUBSTANCE FROM PENICILLIUM FUNICULOSUM : IV. INQUIRY INTO THE MECHANISM BY WHICH HELENINE EXERTS ITS ANTIVIRAL EFFECT
title AN ANTIVIRAL SUBSTANCE FROM PENICILLIUM FUNICULOSUM : IV. INQUIRY INTO THE MECHANISM BY WHICH HELENINE EXERTS ITS ANTIVIRAL EFFECT
title_full AN ANTIVIRAL SUBSTANCE FROM PENICILLIUM FUNICULOSUM : IV. INQUIRY INTO THE MECHANISM BY WHICH HELENINE EXERTS ITS ANTIVIRAL EFFECT
title_fullStr AN ANTIVIRAL SUBSTANCE FROM PENICILLIUM FUNICULOSUM : IV. INQUIRY INTO THE MECHANISM BY WHICH HELENINE EXERTS ITS ANTIVIRAL EFFECT
title_full_unstemmed AN ANTIVIRAL SUBSTANCE FROM PENICILLIUM FUNICULOSUM : IV. INQUIRY INTO THE MECHANISM BY WHICH HELENINE EXERTS ITS ANTIVIRAL EFFECT
title_short AN ANTIVIRAL SUBSTANCE FROM PENICILLIUM FUNICULOSUM : IV. INQUIRY INTO THE MECHANISM BY WHICH HELENINE EXERTS ITS ANTIVIRAL EFFECT
title_sort antiviral substance from penicillium funiculosum : iv. inquiry into the mechanism by which helenine exerts its antiviral effect
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2138137/
https://www.ncbi.nlm.nih.gov/pubmed/5905239
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