Propranolol in the prevention of the first hemorrhage from esophagogastric varices: A multicenter, randomized clinical trial

Harold O. Conn; Norman D. Grace; Jackie Bosch; Roberto J. Groszmann; Joan Rodés; Steven Charles Wright; Daniel S. Matloff; Guadalupe García–Tsao; Rosemarie L. Fisher; Miguel Navasa; Steven J. Drewniak; Colin E. Atterbury; José M. Bordas; Emanuel Lerner; Christina Bramante

doi:10.1002/hep.1840130517

Propranolol in the prevention of the first hemorrhage from esophagogastric varices: A multicenter, randomized clinical trial

Harold O. Conn(United States Department of Veterans Affairs), Norman D. Grace(Tufts University), Jackie Bosch(Universitat de Barcelona), Roberto J. Groszmann(United States Department of Veterans Affairs), Joan Rodés(Universitat de Barcelona), Steven Charles Wright(Tufts University), Daniel S. Matloff(Tufts University), Guadalupe García–Tsao(United States Department of Veterans Affairs), Rosemarie L. Fisher(United States Department of Veterans Affairs), Miguel Navasa(Universitat de Barcelona), Steven J. Drewniak(Tufts University), Colin E. Atterbury(United States Department of Veterans Affairs), José M. Bordas(Universitat de Barcelona), Emanuel Lerner(United States Department of Veterans Affairs), Christina Bramante(Tufts University)

Hepatology

May 1, 1991

10.1002/hep.1840130517

Cited by 203

Abstract

To assess the effectiveness of propranolol in the prevention of initial variceal hemorrhage, a double-blind, randomized trial was carried out in three centers. Patients with cirrhosis (78% alcoholic), hepatic venous pressure gradients greater than 12 mm Hg and endoscopically proven esophageal varices were randomly assigned to propranolol (51 patients) or placebo (51 patients). Of the 102 patients, 58% were Child's class A, 34% were Child's class B and 8% were Child's class C. Daily dosage was determined by the administration of progressively increasing doses of propranolol with the hepatic vein catheter in place to achieve a 25% decrease in hepatic venous pressure gradient, a decrease in hepatic venous pressure gradient to less than 12 mm Hg or a decrease in resting heart rate to less than 55 beats/min. During a mean follow-up period of 16.3 mo, 11 patients in the placebo group (22%) bled from esophageal varices compared with 2 in the propranolol group (4%) during a mean period of 17.1 mo (p less than 0.01). Three additional patients (6%) in the placebo group bled from portal hypertensive gastropathy compared with none in the propranolol group. Propranolol appeared effective in preventing bleeding from large varices. Eleven deaths (22%) occurred in the placebo group compared with eight deaths (16%) in the propranolol group (NS). The mean dose of propranolol was 132 mg/day, and the median dose was 80 mg/day. Using a compliance index (pill count, clinic attendance, alcohol and propranolol levels and alcohol history), 81% of the propranolol patients and 77% of the placebo patients were considered compliant. Complications severe enough to require cessation of therapy occurred in eight patients (16%) in the propranolol group and four in the placebo group (8%) (NS). We conclude that propranolol effectively prevents the first variceal hemorrhage in patients with alcoholic cirrhosis and large esophageal varices but does not improve survival.

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