Literature DB >> 8024362

Anti-endotoxin therapy in primate bacteremia with HA-1A and BPI.

M A Rogy1, L L Moldawer, H S Oldenburg, W A Thompson, W J Montegut, S A Stackpole, A Kumar, M A Palladino, M N Marra, S F Lowry.   

Abstract

OBJECTIVE: The in vivo neutralizing activities of an anti-lipopolysaccharide (LPS) antibody HA-1A (Centoxin [Centocor, Malvern, PA]), a human immunoglobulin M monoclonal antibody, and of bactericidal/permeability-increasing protein (BPI), an endogenously produced human LPS-neutralizing protein, were studied in a primate model of lethal Escherichia coli bacteremia. SUMMARY BACKGROUND DATA: HA-1A has been used with variable success against LPS activity in some animal models and in a recently reported clinical trial. However, no data assessing the efficacy of this agent in subhuman primates is available. Bactericidal/permeability-increasing protein is a product of polymorphomononuclear cells (PMNs) that is stored in azurophilic granules and exhibits LPS-neutralizing activity in vitro and in some in vivo models.
METHODS: Immediately after E. coli infusion and in a blinded fashion, three baboons were treated with BPI (5 mg/kg bolus infusion and 95 micrograms/kg/min infusion over 4 hr). Three animals received 3 mg/kg BW of HA-1A, whereas another three baboons received a placebo treatment.
RESULTS: The BPI-treated animals demonstrated significantly (p < 0.03) lower circulating LPS-limulus amoebocyte lysate (LAL) activity compared with the control animals, but this reduction in LPS-LAL activity was not associated with improved survival. HA-1A treatment did not reduce LPS-LAL activity. However, both BPI and HA-1A treatment did attenuate the pro-inflammatory cytokine response.
CONCLUSION: The current data suggests that incomplete neutralization of endotoxin activity does not alter mortality from severe bacteremia. Given the diversity of mediator production under such circumstances, a strategy of combination therapy in the form of anti-lipopolysaccharide and anticytokine treatment may be necessary to achieve optimal survival.

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Year:  1994        PMID: 8024362      PMCID: PMC1234290          DOI: 10.1097/00000658-199407000-00011

Source DB:  PubMed          Journal:  Ann Surg        ISSN: 0003-4932            Impact factor:   12.969


  47 in total

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7.  The role of bactericidal/permeability-increasing protein in the treatment of primate bacteremia and septic shock.

Authors:  M A Rogy; H S Oldenburg; S E Calvano; W J Montegut; S A Stackpole; K J Van Zee; M N Marra; R W Scott; J J Seilhammer; L L Moldawer
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Journal:  Eur J Immunol       Date:  1987-10       Impact factor: 5.532

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3.  Antiendotoxin activity of cationic peptide antimicrobial agents.

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4.  Protective effect of bactericidal/permeability-increasing protein (rBPI21) in baboon sepsis is related to its antibacterial, not antiendotoxin, properties.

Authors:  G Schlag; H Redl; J Davies; P Scannon
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5.  Identification of synthetic host defense peptide mimics that exert dual antimicrobial and anti-inflammatory activities.

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Journal:  Toxins (Basel)       Date:  2013-12-18       Impact factor: 4.546

7.  Pilot experience with opebacan/rBPI 21 in myeloablative hematopoietic cell transplantation.

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Review 8.  Chronic Critical Illness and the Persistent Inflammation, Immunosuppression, and Catabolism Syndrome.

Authors:  Russell B Hawkins; Steven L Raymond; Julie A Stortz; Hiroyuki Horiguchi; Scott C Brakenridge; Anna Gardner; Philip A Efron; Azra Bihorac; Mark Segal; Frederick A Moore; Lyle L Moldawer
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Review 9.  Gene therapy in surgery: Part II: Application to septic shock and to organ transplantation.

Authors:  M A Rogy; Julie M Baumhofer; Britta Beinhauer; H Brandmeier; P Eisenburger; U M Losert; Ramila Philip
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