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Rescue of rhesus macaques from the lethality of aerosolized ricin toxin
Chad J. Roy, Dylan J. Ehrbar, Natasha Bohorova, Ognian Bohorov, Do Kim, Michael Pauly, Kevin Whaley, Yinghui Rong, Fernando J. Torres-Velez, Ellen S. Vitetta, Peter J. Didier, Lara Doyle-Meyers, Larry Zeitlin, Nicholas J. Mantis
Chad J. Roy, Dylan J. Ehrbar, Natasha Bohorova, Ognian Bohorov, Do Kim, Michael Pauly, Kevin Whaley, Yinghui Rong, Fernando J. Torres-Velez, Ellen S. Vitetta, Peter J. Didier, Lara Doyle-Meyers, Larry Zeitlin, Nicholas J. Mantis
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Research Article Immunology Pulmonology

Rescue of rhesus macaques from the lethality of aerosolized ricin toxin

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Abstract

Ricin toxin (RT) ranks at the top of the list of bioweapons of concern to civilian and military personnel alike, due to its high potential for morbidity and mortality after inhalation. In nonhuman primates, aerosolized ricin triggers severe acute respiratory distress characterized by perivascular and alveolar edema, neutrophilic infiltration, and severe necrotizing bronchiolitis and alveolitis. There are currently no approved countermeasures for ricin intoxication. Here, we report the therapeutic potential of a humanized mAb against an immunodominant epitope on ricin’s enzymatic A chain (RTA). Rhesus macaques that received i.v. huPB10 4 hours after a lethal dose of ricin aerosol exposure survived toxin challenge, whereas control animals succumbed to ricin intoxication within 30 hours. Antibody intervention at 12 hours resulted in the survival of 1 of 5 monkeys. Changes in proinflammatory cytokine, chemokine, and growth factor profiles in bronchial alveolar lavage fluids before and after toxin challenge successfully clustered animals by treatment group and survival, indicating a relationship between local tissue damage and experimental outcome. This study represents the first demonstration, to our knowledge, in nonhuman primates that the lethal effects of inhalational ricin exposure can be negated by a drug candidate, and it opens up a path forward for product development.

Authors

Chad J. Roy, Dylan J. Ehrbar, Natasha Bohorova, Ognian Bohorov, Do Kim, Michael Pauly, Kevin Whaley, Yinghui Rong, Fernando J. Torres-Velez, Ellen S. Vitetta, Peter J. Didier, Lara Doyle-Meyers, Larry Zeitlin, Nicholas J. Mantis

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Figure 6

Principal component analysis of cytokine, chemokine, and growth factor fold changes following RT challenge.

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Principal component analysis of cytokine, chemokine, and growth factor f...
Scatter plots of the first 2 principal components of log2-transformed cytokine fold changes in (A–C) serum and (D–F) BAL from all animals included in the study, calculated using singular value decomposition. Each dot represents an individual monkey; red was used for those in the 4-hour group, black for the 12-hour group, and white for the control group. The 95% confidence ellipses of the group means are color-coded by group. Eigenvectors (C and F) are colored to show the percent contribution of each cytokine to the principal components.

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