TY - JOUR
T1 - Randomized, placebo-controlled trial of lisofylline for early treatment of acute lung injury and acute respiratory distress syndrome
AU - The ARDS Clinical Trials Network
AU - National Heart, Lung, and Blood Institute
AU - National Institutes of Health
AU - Wiedemann, Herbert P.
AU - Arroliga, Alejandro C.
AU - Komara, John B.A.
AU - Welsh, Carolyn
AU - Fulkerson, William J.
AU - MacIntyre, Neil
AU - Mallatratt, Lee
AU - Sebastian, Mark
AU - Sladen, Robert
AU - Wilcox, Carroll
AU - Brower, Roy G.
AU - Thompson, David
AU - Morris, Alan H.
AU - Clemmer, Terry
AU - Davis, Robin
AU - Orme, James
AU - Lawton, Charles B.
AU - d'Hulst, Janice
AU - Smith, Carolyn
AU - Gottlieb, Jonathan
AU - Girod, Aimee
AU - Matthay, Michael A.
AU - Daniel, Brian
AU - Kallet, Richard
AU - Luce, John M.
AU - Gryzner, Michael A.
AU - Abraham, Edward
AU - Piedalue, Fran
AU - Kalous, Dawn
AU - Walberg, Christine
AU - Lockrem, John
AU - McIntyre, Robert
AU - Parsons, Polly
AU - Stevens, Chris
AU - Silverman, Henry J.
AU - Corral, Wanda
AU - Toews, Galen B.
AU - Arnoldi, Deborah
AU - Bartlett, Robert H.
AU - Dechert, Ron
AU - Watts, Charles
AU - Lanken, Paul N.
AU - Anderson, Harry
AU - Finkel, Barbara
AU - Hanson, C. William
AU - Hudson, Leonard D.
AU - Lee, Claudette
AU - Maier, Ronald V.
AU - Steinberg, Kenneth P.
AU - Garcia, Joe G.N.
N1 - Publisher Copyright:
Copyright © 2002 by Lippincott Williams & Wilkins
PY - 2002
Y1 - 2002
N2 - Objective: To determine whether the administration of lisofylline (1-[5R-hydroxyhexyl]-3,7-dimethylxanthine) would decrease mortality in patients with acute lung injury (ALI) or acute respiratory distress syndrome (ARDS). Design: A prospective, randomized, double-blind, placebo-controlled, multicenter study. Setting: Intensive care units at 21 hospitals at the ten centers constituting the ARDS Clinical Trials Network. Patients: A total of 235 patients who met eligibility criteria were enrolled in the study (116 into the lisofylline group, 119 into the placebo group). Interventions: Patients were randomized to receive either lisofylline or placebo. The dose of lisofylline was 3 mg/kg with a maximum dose of 300 mg intravenously every 6 hrs. The intravenous solution of study drug was administered over 10 mins every 6 hrs. Dosing was continued for 20 days or until the patient achieved 48 hrs of unassisted breathing. Measurements and Main Results: The trial was stopped by the Data Safety Monitoring Board for futility at the first scheduled interim analysis. The patient groups had similar characteristics at enrollment. No significant safety concerns were associated with lisofylline therapy. There was no significant difference between groups in the number of patients who had died at 28 days (31.9% lisofylline vs. 24.7% placebo, p = .215). There was no significant difference between the lisofylline and placebo groups in terms of resolution of organ failures, ventilator-free days, infection-related deaths, or development of serious infection during the 28-day study period. The median number of organ failure-free days for the five nonpulmonary organ failures examined (cardiovascular, central nervous system, coagulation, hepatic, and renal) was not different between the lisofylline and placebo groups. Although lisofylline has been reported to decrease circulating free fatty acid levels, we did not find any such treatment effect compared with placebo. Conclusions: In this study, there was no evidence that lisofylline had beneficial effects in the treatment of established ALI/ ARDS.
AB - Objective: To determine whether the administration of lisofylline (1-[5R-hydroxyhexyl]-3,7-dimethylxanthine) would decrease mortality in patients with acute lung injury (ALI) or acute respiratory distress syndrome (ARDS). Design: A prospective, randomized, double-blind, placebo-controlled, multicenter study. Setting: Intensive care units at 21 hospitals at the ten centers constituting the ARDS Clinical Trials Network. Patients: A total of 235 patients who met eligibility criteria were enrolled in the study (116 into the lisofylline group, 119 into the placebo group). Interventions: Patients were randomized to receive either lisofylline or placebo. The dose of lisofylline was 3 mg/kg with a maximum dose of 300 mg intravenously every 6 hrs. The intravenous solution of study drug was administered over 10 mins every 6 hrs. Dosing was continued for 20 days or until the patient achieved 48 hrs of unassisted breathing. Measurements and Main Results: The trial was stopped by the Data Safety Monitoring Board for futility at the first scheduled interim analysis. The patient groups had similar characteristics at enrollment. No significant safety concerns were associated with lisofylline therapy. There was no significant difference between groups in the number of patients who had died at 28 days (31.9% lisofylline vs. 24.7% placebo, p = .215). There was no significant difference between the lisofylline and placebo groups in terms of resolution of organ failures, ventilator-free days, infection-related deaths, or development of serious infection during the 28-day study period. The median number of organ failure-free days for the five nonpulmonary organ failures examined (cardiovascular, central nervous system, coagulation, hepatic, and renal) was not different between the lisofylline and placebo groups. Although lisofylline has been reported to decrease circulating free fatty acid levels, we did not find any such treatment effect compared with placebo. Conclusions: In this study, there was no evidence that lisofylline had beneficial effects in the treatment of established ALI/ ARDS.
KW - Acute lung injury
KW - Acute respiratory distress syndrome
KW - Lisotylline
KW - Oxidant
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UR - http://www.scopus.com/inward/citedby.url?scp=0036152894&partnerID=8YFLogxK
U2 - 10.1097/00003246-200201000-00001
DO - 10.1097/00003246-200201000-00001
M3 - Article
C2 - 11902249
AN - SCOPUS:0036152894
SN - 0090-3493
VL - 30
SP - 1
EP - 6
JO - Critical care medicine
JF - Critical care medicine
IS - 1
ER -