EXPANDED CLINICAL-EVALUATION OF LOVASTATIN (EXCEL) STUDY RESULTS .4. ADDITIONAL PERSPECTIVES ON THE TOLERABILITY OF LOVASTATIN

被引:92
作者
DUJOVNE, CA
CHREMOS, AN
POOL, JL
SCHNAPER, H
BRADFORD, RH
SHEAR, CL
HIGGINS, J
DOWNTON, M
FRANKLIN, FA
NASH, DT
GOULD, AL
LANGENDORFER, A
机构
[1] MERCK SHARP & DOHME LTD,W POINT,PA 19486
[2] BAYLOR COLL MED,DEPT MED,HOUSTON,TX 77030
[3] UNIV ALABAMA,CTR AGING,BIRMINGHAM,AL 35294
[4] OKLAHOMA MED RES FDN,LIPID RES CLIN,OKLAHOMA CITY,OK 73104
[5] CLIN RES INT INC,RES TRIANGLE PK,NC
[6] UNIV ALABAMA,DEPT GASTROENTEROL & NUTR,BIRMINGHAM,AL 35294
[7] SUNY HLTH SCI CTR,SYRACUSE,NY
来源
AMERICAN JOURNAL OF MEDICINE | 1991年 / 91卷
关键词
D O I
10.1016/0002-9343(91)90053-Z
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
This randomized, double-blind, multicenter, diet-and-placebo-controlled study was designed to clarify the dose-response relationship of lovastatin therapy to lipid-modifying efficacy and drug-related adverse events. Exclusion criteria were minimized so that study patients were representative of the majority of patients with moderate hypercholesterolemia seen in medical practice. After 6 weeks on the American Heart Association Step 1 Diet, a total of 8,215 patients were randomly assigned to 48 weeks of treatment with diet and placebo or lovastatin at dosages of 20 or 40 mg once a day or 20 or 40 mg twice a day. All adverse events were monitored, with particular attention to evaluation of liver and muscle. Liver transaminase elevations suggestive of possible hepatotoxicity, defined as successive elevations in either aspartate transaminase or alanine aminotransferase > 3 times the upper limit of normal, occurred in equal numbers of placebo and lovastatin 20 mg/day treated patients (0.1%). The frequencies were higher in lovastatin 40 mg/day and 80 mg/day patient groups (0.9 and 1.5%, respectively). No patient was diagnosed as having clinically symptomatic hepatic dysfunction. Creatine kinase (CK) elevations above the upper limit of normal occurred frequently in placebo- (29%), as well as lovastatin-treated patients (29-35%), and muscle symptoms were reported with similar frequency in all groups (7-9%). The combination of muscle symptoms with marked CK elevations (> 10 times the upper limit of normal) was seen in only five patients: one in a 40 mg/day dose group and four in the 80 mg/day dose group. No patient developed rhabdomyolysis. The incidence of clinical and laboratory adverse events requiring discontinuation was 6% for the placebo group and from 7% (20 mg/day) to 9% (80 mg/day) for lovastatin treatment groups. No new types of adverse experiences related to lovastatin treatment were reported. lovastatin, as an adjunct to diet for the reduction of elevated LDL cholesterol. was generally very well tolerated.
引用
收藏
页码:S25 / S30
页数:6
相关论文
共 16 条
[1]  
ALBERTS AW, 1989, CARDIOVASC DRUG REV, V7, P88
[2]  
BILHEIMER DW, 1983, T ASSOC AM PHYSICIAN, V96, P1
[3]   EXPANDED CLINICAL-EVALUATION OF LOVASTATIN (EXCEL) STUDY RESULTS .1. EFFICACY IN MODIFYING PLASMA-LIPOPROTEINS AND ADVERSE EVENT PROFILE IN 8245 PATIENTS WITH MODERATE HYPERCHOLESTEROLEMIA [J].
BRADFORD, RH ;
SHEAR, CL ;
CHREMOS, AN ;
DUJOVNE, C ;
DOWNTON, M ;
FRANKLIN, FA ;
GOULD, AL ;
HESNEY, M ;
HIGGINS, J ;
HURLEY, DP ;
LANGENDORFER, A ;
NASH, DT ;
POOL, JL ;
SCHNAPER, H .
ARCHIVES OF INTERNAL MEDICINE, 1991, 151 (01) :43-49
[4]   EXPANDED CLINICAL-EVALUATION OF LOVASTATIN (EXCEL) STUDY - DESIGN AND PATIENT CHARACTERISTICS OF A DOUBLE-BLIND, PLACEBO-CONTROLLED STUDY IN PATIENTS WITH MODERATE HYPERCHOLESTEROLEMIA [J].
BRADFORD, RH ;
SHEAR, CL ;
CHREMOS, AN ;
DUJOVNE, C ;
FRANKLIN, FA ;
HESNEY, M ;
HIGGINS, J ;
LANGENDORFER, A ;
POOL, JL ;
SCHNAPER, H ;
STEPHENSON, WP .
AMERICAN JOURNAL OF CARDIOLOGY, 1990, 66 (08) :B44-B55
[5]  
BRADFORD RH, 1991, AM J MED, V91, P18
[6]  
DAVIDSON CS, 1979, NIH79313 US DHEW PUB, P108
[7]  
GRUNDY SM, 1988, NEW ENGL J MED, V319, P24
[8]   LOVASTATIN (MEVINOLIN) IN THE TREATMENT OF HETEROZYGOUS FAMILIAL HYPERCHOLESTEROLEMIA - A MULTICENTER STUDY [J].
HAVEL, RJ ;
HUNNINGHAKE, DB ;
ILLINGWORTH, DR ;
LEES, RS ;
STEIN, EA ;
TOBERT, JA ;
BACON, SR ;
BOLOGNESE, JA ;
FROST, PH ;
LAMKIN, GE ;
LEES, AM ;
LEON, AS ;
GARDNER, K ;
JOHNSON, G ;
MELLIES, MJ ;
RHYMER, PA ;
TUN, P .
ANNALS OF INTERNAL MEDICINE, 1987, 107 (05) :609-615
[9]   3-HYDROXY-3-METHYLGLUTARYL - COENZYME-A REDUCTASE INHIBITORS IN THE TREATMENT OF HYPERCHOLESTEROLEMIA [J].
HOEG, JM ;
BREWER, HB .
JAMA-JOURNAL OF THE AMERICAN MEDICAL ASSOCIATION, 1987, 258 (24) :3532-3536
[10]  
LATIES AM, 1991, AM J CARDIOL, V66, P447
12