学术探索
学术期刊
新闻热点
数据分析
智能评审

FIXING THE NUMBER OF EVENTS IN LARGE COMPARATIVE TRIALS WITH LOW EVENT RATES - A BINOMIAL APPROACH

被引:16
作者
SHUSTER, JJ
机构
[1] University of Statistics, University of Florida, Gainesville, FL
来源
CONTROLLED CLINICAL TRIALS | 1993年 / 14卷 / 03期
关键词
BINOMIAL DISTRIBUTION; CENSORED SURVIVAL DATA; FISHERS EXACT TEST; GROUP SEQUENTIAL METHODS; MINIMAL DETECTABLE DIFFERENCE; POWER; SAMPLE SIZE;
D O I
10.1016/0197-2456(93)90003-V
中图分类号
R-3 [医学研究方法]; R3 [基础医学];
学科分类号
1001 ;
摘要
In designing large clinical trials where the event rates are low, capabilities can be improved if one fixes the number of events rather than the number of patients. The dependent variable, the number of events in the treatment group, has essentially an unconditional binomial distribution. Simple tables giving the minimum detectable difference are provided for common type I error values and power. Implications for sequential monitoring are also presented. The methods can be applied to large randomized, stratified trials utilizing censored survival data, planned under proportional hazards and equal target population competing losses, provided that event rates are low.
引用
收藏
页码:198 / 208
页数:11
相关论文
共 19 条
[1]  
Bernstein D., 1978, Journal of Statistical Computation and Simulation, V8, P65, DOI 10.1080/00949657808810249
[2]   POWER COMPUTATIONS FOR DESIGNING COMPARATIVE POISSON TRIALS [J].
GAIL, M .
BIOMETRICS, 1974, 30 (02) :231-237
[3]   PLANNING SIZE AND DURATION OF A CLINICAL TRIAL STUDYING TIME TO SOME CRITICAL EVENT [J].
GEORGE, SL ;
DESU, MM .
JOURNAL OF CHRONIC DISEASES, 1974, 27 (1-2) :15-24
[4]  
Gordon Lan KK., 1982, SEQUENTIAL ANAL, V1, P207, DOI [DOI 10.1080/07474948208836014, 10.1080/07474948208836014]
[5]   DESIGNING CLINICAL-TRIALS WITH ARBITRARY SPECIFICATION OF SURVIVAL FUNCTIONS AND FOR THE LOG RANK OR GENERALIZED WILCOXON TEST [J].
HALPERN, J ;
BROWN, BW .
CONTROLLED CLINICAL TRIALS, 1987, 8 (03) :177-189
[6]   INTRODUCTION TO SAMPLE-SIZE DETERMINATION AND POWER ANALYSIS FOR CLINICAL-TRIALS [J].
LACHIN, JM .
CONTROLLED CLINICAL TRIALS, 1981, 2 (02) :93-113
[7]   MULTIPLE TESTING PROCEDURE FOR CLINICAL-TRIALS [J].
OBRIEN, PC ;
FLEMING, TR .
BIOMETRICS, 1979, 35 (03) :549-556
[8]   CONSERVATISM OF APPROXIMATION SIGMA (O - E)2/E IN LOGRANK TEST FOR SURVIVAL DATA OR TUMOR INCIDENCE DATA [J].
PETO, R ;
PIKE, MC .
BIOMETRICS, 1973, 29 (03) :579-584
[9]   PLANNING THE DURATION OF A COMPARATIVE CLINICAL-TRIAL WITH LOSS TO FOLLOW-UP AND A PERIOD OF CONTINUED OBSERVATION [J].
RUBINSTEIN, LV ;
GAIL, MH ;
SANTNER, TJ .
JOURNAL OF CHRONIC DISEASES, 1981, 34 (9-10) :469-479
[10]   MONITORING RULES FOR STOPPING ACCRUAL IN COMPARATIVE SURVIVAL STUDIES [J].
RUBINSTEIN, LV ;
GAIL, MH .
CONTROLLED CLINICAL TRIALS, 1982, 3 (04) :325-343
12