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Protective antigen antibody augments hemodynamic support in anthrax lethal toxin shock in canines.

Authors :
Barochia AV
Cui X
Sun J
Li Y
Solomon SB
Migone TS
Subramanian GM
Bolmer SD
Eichacker PQ
Source :
The Journal of infectious diseases [J Infect Dis] 2012 Mar 01; Vol. 205 (5), pp. 818-29. Date of Electronic Publication: 2012 Jan 05.
Publication Year :
2012

Abstract

Background: Anthrax-associated shock is closely linked to lethal toxin (LT) release and is highly lethal despite conventional hemodynamic support. We investigated whether protective antigen-directed monoclonal antibody (PA-mAb) treatment further augments titrated hemodynamic support.<br />Methods and Results: Forty sedated, mechanically ventilated, instrumented canines challenged with anthrax LT were assigned to no treatment (controls), hemodynamic support alone (protocol-titrated fluids and norepinephrine), PA-mAb alone (administered at start of LT infusion [0 hours] or 9 or 12 hours later), or both, and observed for 96 hours. Although all 8 controls died, 2 of 8 animals receiving hemodynamic support alone survived (median survival times 65 vs 85 hours, respectively; Pā€‰=ā€‰.03). PA-mAb alone at 0 hour improved survival (5 of 5 animals survived), but efficacy decreased progressively with delayed treatment (9 hours, 2 of 3 survived; 12 hours, 0 of 4 survived) (P = .004 comparing survival across treatment times). However, combined treatment increased survival irrespective of PA-mAb administration time (0 hours, 4 of 5 animals; 9 hours, 3 of 3 animals; and 12 hours, 4 of 5 animals survived) (P = .95 comparing treatment times). Compared to hemodynamic support alone, when combined over PA-mAb treatment times (0, 9, and 12 hours), combination therapy produced higher survival (P = .008), central venous pressures, and left ventricular ejection fractions, and lower heart rates, norepinephrine requirements and fluid retention (P ā‰¤ .03).<br />Conclusions: PA-mAb may augment conventional hemodynamic support during anthrax LT-associated shock.

Details

Language :
English
ISSN :
1537-6613
Volume :
205
Issue :
5
Database :
MEDLINE
Journal :
The Journal of infectious diseases
Publication Type :
Academic Journal
Accession number :
22223857
Full Text :
https://doi.org/10.1093/infdis/jir834