Comprehensive characterization of toxins during progression of inhalation anthrax in a non-human primate model

Inhalation anthrax has three clinical stages: early-prodromal, intermediate-progressive, and late-fulminant. We report the comprehensive characterization of anthrax toxins, including total protective antigen (PA), total lethal factor (LF), total edema factor (EF), and their toxin complexes, lethal t...

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Autores principales: Boyer, Anne E., Gallegos-Candela, Maribel, Lins, Renato C., Solano, Maria I., Woolfitt, Adrian R., Lee, John S., Sanford, Daniel C., Knostman, Katherine A. B., Quinn, Conrad P., Hoffmaster, Alex R., Pirkle, James L., Barr, John R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2022
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9810172/
https://www.ncbi.nlm.nih.gov/pubmed/36534695
http://dx.doi.org/10.1371/journal.ppat.1010735
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author Boyer, Anne E.
Gallegos-Candela, Maribel
Lins, Renato C.
Solano, Maria I.
Woolfitt, Adrian R.
Lee, John S.
Sanford, Daniel C.
Knostman, Katherine A. B.
Quinn, Conrad P.
Hoffmaster, Alex R.
Pirkle, James L.
Barr, John R.
author_facet Boyer, Anne E.
Gallegos-Candela, Maribel
Lins, Renato C.
Solano, Maria I.
Woolfitt, Adrian R.
Lee, John S.
Sanford, Daniel C.
Knostman, Katherine A. B.
Quinn, Conrad P.
Hoffmaster, Alex R.
Pirkle, James L.
Barr, John R.
author_sort Boyer, Anne E.
collection PubMed
description Inhalation anthrax has three clinical stages: early-prodromal, intermediate-progressive, and late-fulminant. We report the comprehensive characterization of anthrax toxins, including total protective antigen (PA), total lethal factor (LF), total edema factor (EF), and their toxin complexes, lethal toxin and edema toxin in plasma, during the course of inhalation anthrax in 23 cynomolgus macaques. The toxin kinetics were predominantly triphasic with an early rise (phase-1), a plateau/decline (phase-2), and a final rapid rise (phase-3). Eleven animals had shorter survival times, mean±standard deviation of 58.7±7.6 hours (fast progression), 11 animals had longer survival times, 113±34.4 hours (slow progression), and one animal survived. Median (lower–upper quartile) LF levels at the end-of-phase-1 were significantly higher in animals with fast progression [138 (54.9–326) ng/mL], than in those with slow progression [23.8 (15.6–26.3) ng/mL] (p = 0.0002), and the survivor (11.1 ng/mL). The differences were also observed for other toxins and bacteremia. Animals with slow progression had an extended phase-2 plateau, with low variability of LF levels across all time points and animals. Characterization of phase-2 toxin levels defined upper thresholds; critical levels for exiting phase-2 and entering the critical phase-3, 342 ng/mL (PA), 35.8 ng/mL (LF), and 1.10 ng/mL (EF). The thresholds were exceeded earlier in animals with fast progression (38.5±7.4 hours) and later in animals with slow progression (78.7±15.2 hours). Once the threshold was passed, toxin levels rose rapidly in both groups to the terminal stage. The time from threshold to terminal was rapid and similar; 20.8±7.4 hours for fast and 19.9±7.5 hours for slow progression. The three toxemic phases were aligned with the three clinical stages of anthrax for fast and slow progression which showed that anthrax progression is toxin- rather than time-dependent. This first comprehensive evaluation of anthrax toxins provides new insights into disease progression.
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spelling pubmed-98101722023-01-04 Comprehensive characterization of toxins during progression of inhalation anthrax in a non-human primate model Boyer, Anne E. Gallegos-Candela, Maribel Lins, Renato C. Solano, Maria I. Woolfitt, Adrian R. Lee, John S. Sanford, Daniel C. Knostman, Katherine A. B. Quinn, Conrad P. Hoffmaster, Alex R. Pirkle, James L. Barr, John R. PLoS Pathog Research Article Inhalation anthrax has three clinical stages: early-prodromal, intermediate-progressive, and late-fulminant. We report the comprehensive characterization of anthrax toxins, including total protective antigen (PA), total lethal factor (LF), total edema factor (EF), and their toxin complexes, lethal toxin and edema toxin in plasma, during the course of inhalation anthrax in 23 cynomolgus macaques. The toxin kinetics were predominantly triphasic with an early rise (phase-1), a plateau/decline (phase-2), and a final rapid rise (phase-3). Eleven animals had shorter survival times, mean±standard deviation of 58.7±7.6 hours (fast progression), 11 animals had longer survival times, 113±34.4 hours (slow progression), and one animal survived. Median (lower–upper quartile) LF levels at the end-of-phase-1 were significantly higher in animals with fast progression [138 (54.9–326) ng/mL], than in those with slow progression [23.8 (15.6–26.3) ng/mL] (p = 0.0002), and the survivor (11.1 ng/mL). The differences were also observed for other toxins and bacteremia. Animals with slow progression had an extended phase-2 plateau, with low variability of LF levels across all time points and animals. Characterization of phase-2 toxin levels defined upper thresholds; critical levels for exiting phase-2 and entering the critical phase-3, 342 ng/mL (PA), 35.8 ng/mL (LF), and 1.10 ng/mL (EF). The thresholds were exceeded earlier in animals with fast progression (38.5±7.4 hours) and later in animals with slow progression (78.7±15.2 hours). Once the threshold was passed, toxin levels rose rapidly in both groups to the terminal stage. The time from threshold to terminal was rapid and similar; 20.8±7.4 hours for fast and 19.9±7.5 hours for slow progression. The three toxemic phases were aligned with the three clinical stages of anthrax for fast and slow progression which showed that anthrax progression is toxin- rather than time-dependent. This first comprehensive evaluation of anthrax toxins provides new insights into disease progression. Public Library of Science 2022-12-19 /pmc/articles/PMC9810172/ /pubmed/36534695 http://dx.doi.org/10.1371/journal.ppat.1010735 Text en https://creativecommons.org/publicdomain/zero/1.0/This is an open access article, free of all copyright, and may be freely reproduced, distributed, transmitted, modified, built upon, or otherwise used by anyone for any lawful purpose. The work is made available under the Creative Commons CC0 (https://creativecommons.org/publicdomain/zero/1.0/) public domain dedication.
spellingShingle Research Article
Boyer, Anne E.
Gallegos-Candela, Maribel
Lins, Renato C.
Solano, Maria I.
Woolfitt, Adrian R.
Lee, John S.
Sanford, Daniel C.
Knostman, Katherine A. B.
Quinn, Conrad P.
Hoffmaster, Alex R.
Pirkle, James L.
Barr, John R.
Comprehensive characterization of toxins during progression of inhalation anthrax in a non-human primate model
title Comprehensive characterization of toxins during progression of inhalation anthrax in a non-human primate model
title_full Comprehensive characterization of toxins during progression of inhalation anthrax in a non-human primate model
title_fullStr Comprehensive characterization of toxins during progression of inhalation anthrax in a non-human primate model
title_full_unstemmed Comprehensive characterization of toxins during progression of inhalation anthrax in a non-human primate model
title_short Comprehensive characterization of toxins during progression of inhalation anthrax in a non-human primate model
title_sort comprehensive characterization of toxins during progression of inhalation anthrax in a non-human primate model
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9810172/
https://www.ncbi.nlm.nih.gov/pubmed/36534695
http://dx.doi.org/10.1371/journal.ppat.1010735
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