Delayed toxicity associated with soluble anthrax toxin receptor decoy-Ig fusion protein treatment.

Delayed toxicity associated with soluble anthrax toxin receptor decoy-Ig fusion protein treatment.

Soluble receptor decoy inhibitors, including receptor-immunogloubulin (Ig) fusion proteins, have shown promise as candidate anthrax toxin therapeutics. These agents act by binding to the receptor-interaction site on the protective antigen (PA) toxin subunit, thereby blocking toxin binding to cell su...

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Main Authors: Diane Thomas, John Naughton, Christopher Cote, Susan Welkos, Marianne Manchester, John A T Young
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2012-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3325282?pdf=render
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spelling doaj-183ad8e9b1124d5e861249568a6dbbb22020-11-24T22:16:34ZengPublic Library of Science (PLoS)PLoS ONE1932-62032012-01-0174e3461110.1371/journal.pone.0034611Delayed toxicity associated with soluble anthrax toxin receptor decoy-Ig fusion protein treatment.Diane ThomasJohn NaughtonChristopher CoteSusan WelkosMarianne ManchesterJohn A T YoungSoluble receptor decoy inhibitors, including receptor-immunogloubulin (Ig) fusion proteins, have shown promise as candidate anthrax toxin therapeutics. These agents act by binding to the receptor-interaction site on the protective antigen (PA) toxin subunit, thereby blocking toxin binding to cell surface receptors. Here we have made the surprising observation that co-administration of receptor decoy-Ig fusion proteins significantly delayed, but did not protect, rats challenged with anthrax lethal toxin. The delayed toxicity was associated with the in vivo assembly of a long-lived complex comprised of anthrax lethal toxin and the receptor decoy-Ig inhibitor. Intoxication in this system presumably results from the slow dissociation of the toxin complex from the inhibitor following their prolonged circulation. We conclude that while receptor decoy-Ig proteins represent promising candidates for the early treatment of B. anthracis infection, they may not be suitable for therapeutic use at later stages when fatal levels of toxin have already accumulated in the bloodstream.http://europepmc.org/articles/PMC3325282?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Diane Thomas
John Naughton
Christopher Cote
Susan Welkos
Marianne Manchester
John A T Young
spellingShingle Diane Thomas
John Naughton
Christopher Cote
Susan Welkos
Marianne Manchester
John A T Young
Delayed toxicity associated with soluble anthrax toxin receptor decoy-Ig fusion protein treatment.
PLoS ONE
author_facet Diane Thomas
John Naughton
Christopher Cote
Susan Welkos
Marianne Manchester
John A T Young
author_sort Diane Thomas
title Delayed toxicity associated with soluble anthrax toxin receptor decoy-Ig fusion protein treatment.
title_short Delayed toxicity associated with soluble anthrax toxin receptor decoy-Ig fusion protein treatment.
title_full Delayed toxicity associated with soluble anthrax toxin receptor decoy-Ig fusion protein treatment.
title_fullStr Delayed toxicity associated with soluble anthrax toxin receptor decoy-Ig fusion protein treatment.
title_full_unstemmed Delayed toxicity associated with soluble anthrax toxin receptor decoy-Ig fusion protein treatment.
title_sort delayed toxicity associated with soluble anthrax toxin receptor decoy-ig fusion protein treatment.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2012-01-01
description Soluble receptor decoy inhibitors, including receptor-immunogloubulin (Ig) fusion proteins, have shown promise as candidate anthrax toxin therapeutics. These agents act by binding to the receptor-interaction site on the protective antigen (PA) toxin subunit, thereby blocking toxin binding to cell surface receptors. Here we have made the surprising observation that co-administration of receptor decoy-Ig fusion proteins significantly delayed, but did not protect, rats challenged with anthrax lethal toxin. The delayed toxicity was associated with the in vivo assembly of a long-lived complex comprised of anthrax lethal toxin and the receptor decoy-Ig inhibitor. Intoxication in this system presumably results from the slow dissociation of the toxin complex from the inhibitor following their prolonged circulation. We conclude that while receptor decoy-Ig proteins represent promising candidates for the early treatment of B. anthracis infection, they may not be suitable for therapeutic use at later stages when fatal levels of toxin have already accumulated in the bloodstream.
url http://europepmc.org/articles/PMC3325282?pdf=render
work_keys_str_mv AT dianethomas delayedtoxicityassociatedwithsolubleanthraxtoxinreceptordecoyigfusionproteintreatment
AT johnnaughton delayedtoxicityassociatedwithsolubleanthraxtoxinreceptordecoyigfusionproteintreatment
AT christophercote delayedtoxicityassociatedwithsolubleanthraxtoxinreceptordecoyigfusionproteintreatment
AT susanwelkos delayedtoxicityassociatedwithsolubleanthraxtoxinreceptordecoyigfusionproteintreatment
AT mariannemanchester delayedtoxicityassociatedwithsolubleanthraxtoxinreceptordecoyigfusionproteintreatment
AT johnatyoung delayedtoxicityassociatedwithsolubleanthraxtoxinreceptordecoyigfusionproteintreatment
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