TY - JOUR
T1 - Platelet-activating factor receptor antagonist BN 52021 in the treatment of severe sepsis
T2 - A randomized, double-blind, placebo-controlled, multicenter clinical trial
AU - Dhainaut, J. F.A.
AU - Tenaillon, A.
AU - Le Tulzo, Y.
AU - Schlemmer, B.
AU - Solet, J. P.
AU - Wolff, M.
AU - Holzapfel, L.
AU - Zeni, F.
AU - Dreyfuss, D.
AU - Mira, J. P.
AU - De Vathaire, F.
AU - Guinot, P.
AU - Demingeon, D.
AU - Piralla, B.
AU - Ferrand, C.
AU - Zeni, F.
AU - Bertrand, J. C.
AU - Gery, P.
AU - Mier, L.
PY - 1994/1/1
Y1 - 1994/1/1
N2 - Objective: To evaluate the safety and efficacy of a natural platelet- activating factor receptor antagonist, BN 52021 (Ginkgolide B), in the treatment of patients with sepsis syndrome. Design: Prospective, randomized, placebo-controlled, double-blind, phase III, multicenter clinical trial. Setting: Twenty-one academic medical center intensive care units in France. Patients: Two hundred sixty-two patients with sepsis syndrome who received standard supportive care and antimicrobial therapy, in addition to the administration of platelet-activating factor receptor antagonist or placebo. Interventions: Patients received either a 120-mg dose of platelet-activating factor receptor antagonist intravenously every 12 hrs over a 4-day period or placebo. Main Outcome Measurements: All patients were evaluated for 28-day, all-cause mortality. Results: The 28-day mortality rate was 51% for the placebo group and 42% for the platelet-activating factor receptor antagonist group (p = .17). However, the efficacy of platelet-activating factor receptor antagonist was significantly greater in patients with Gram-negative sepsis (test for interaction, p = .03). In a separate analysis of patients with and without Gram-negative sepsis, the 28-day mortality rate was 57% for the patients receiving placebo (30 deaths of 53 patients) and 33% for patients receiving platelet-activating factor receptor antagonist (22 deaths of 67 patients; p = .01). Platelet-activating factor receptor antagonist also significantly (p = .01) reduced the mortality rate among patients with Gram- negative sepsis who were in shock at entry into the study (mortality rate was 65% for placebo vs. 37% for platelet-activating factor receptor antagonist) and among patients >60 yrs of age (mortality rate was 74% for placebo vs. 31% for platelet-activating factor receptor antagonist). A Cox proportional- hazards model identified five independent prognostic factors: a) adequacy of antibiotic therapy; b) severity of illness; c) renal failure; d) hematologic failure; and e) hepatic failure at study entry. When the Gram-negative sepsis population was stratified by age and these five prognostic factors were controlled for, the relative risk of death of the platelet-activating factor receptor antagonist group was 0.61 (0.34 to 1.08, 95% confidence interval; p = .09). This risk corresponds with an adjusted reduction in mortality rate of 39% for patients receiving platelet-activating factor receptor antagonist. No differences in mortality rates were found between the placebo and the platelet-activating factor receptor antagonist groups in the absence of Gram- negative sepsis. There were no differences in adverse events between the placebo and the treated groups. Conclusion: The studied platelet-activating factor receptor antagonist (BN 52021) seems to be a safe and promising treatment for patients with severe Gram-negative sepsis.
AB - Objective: To evaluate the safety and efficacy of a natural platelet- activating factor receptor antagonist, BN 52021 (Ginkgolide B), in the treatment of patients with sepsis syndrome. Design: Prospective, randomized, placebo-controlled, double-blind, phase III, multicenter clinical trial. Setting: Twenty-one academic medical center intensive care units in France. Patients: Two hundred sixty-two patients with sepsis syndrome who received standard supportive care and antimicrobial therapy, in addition to the administration of platelet-activating factor receptor antagonist or placebo. Interventions: Patients received either a 120-mg dose of platelet-activating factor receptor antagonist intravenously every 12 hrs over a 4-day period or placebo. Main Outcome Measurements: All patients were evaluated for 28-day, all-cause mortality. Results: The 28-day mortality rate was 51% for the placebo group and 42% for the platelet-activating factor receptor antagonist group (p = .17). However, the efficacy of platelet-activating factor receptor antagonist was significantly greater in patients with Gram-negative sepsis (test for interaction, p = .03). In a separate analysis of patients with and without Gram-negative sepsis, the 28-day mortality rate was 57% for the patients receiving placebo (30 deaths of 53 patients) and 33% for patients receiving platelet-activating factor receptor antagonist (22 deaths of 67 patients; p = .01). Platelet-activating factor receptor antagonist also significantly (p = .01) reduced the mortality rate among patients with Gram- negative sepsis who were in shock at entry into the study (mortality rate was 65% for placebo vs. 37% for platelet-activating factor receptor antagonist) and among patients >60 yrs of age (mortality rate was 74% for placebo vs. 31% for platelet-activating factor receptor antagonist). A Cox proportional- hazards model identified five independent prognostic factors: a) adequacy of antibiotic therapy; b) severity of illness; c) renal failure; d) hematologic failure; and e) hepatic failure at study entry. When the Gram-negative sepsis population was stratified by age and these five prognostic factors were controlled for, the relative risk of death of the platelet-activating factor receptor antagonist group was 0.61 (0.34 to 1.08, 95% confidence interval; p = .09). This risk corresponds with an adjusted reduction in mortality rate of 39% for patients receiving platelet-activating factor receptor antagonist. No differences in mortality rates were found between the placebo and the platelet-activating factor receptor antagonist groups in the absence of Gram- negative sepsis. There were no differences in adverse events between the placebo and the treated groups. Conclusion: The studied platelet-activating factor receptor antagonist (BN 52021) seems to be a safe and promising treatment for patients with severe Gram-negative sepsis.
KW - Gram-negative bacteria
KW - bacterial infection
KW - critical illness
KW - mortality rate
KW - multiple organ failure
KW - platelet-activating factor
KW - sepsis
KW - septic shock
UR - http://www.scopus.com/inward/record.url?scp=0027945044&partnerID=8YFLogxK
U2 - 10.1097/00003246-199422110-00005
DO - 10.1097/00003246-199422110-00005
M3 - Article
C2 - 7956274
AN - SCOPUS:0027945044
SN - 0090-3493
VL - 22
SP - 1720
EP - 1728
JO - Critical Care Medicine
JF - Critical Care Medicine
IS - 11
ER -