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STATISTICS 542 Intro to Clinical Trials SURVIVAL ANALYSIS. Survival Analysis Terminology. Concerned about time to some event Event is often death Event may also be, for example 1. Cause specific death 2. Non-fatal event or death, whichever comes first death or hospitalization
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Survival Analysis Terminology • Concerned about time to some event • Event is often death • Event may also be, for example 1. Cause specific death 2. Non-fatal event or death, whichever comes first death or hospitalization death or MI death or tumor recurrence
Survival Rates at Yearly Intervals • YEARS • At 5 years, survival rates the same • Survival experience in Group A appears more favorable, considering 1 year, 2 year, 3 year and 4 year rates together
Beta-Blocker Heart Attack Trial LIFE-TABLE CUMULATIVE MORTALITY CURVE
Survival Analysis Discuss 1. Estimation of survival curves 2. Comparison of survival curves I. Estimation • Simple Case • All patients entered at the same time and followed for the same length of time • Survival curve is estimated at various time points by (number of deaths)/(number of patients) • As intervals become smaller and number of patients larger, a "smooth" survival curve may be plotted • Typical Clinical Trial Setting
Staggered Entry T years 1 T years 2 Subject T years 3 T years 4 0 T 2T Time Since Start of Trial (T years) • Each patient has T years of follow-up • Time for follow-up taking place may be different for each patient
Subject o Administrative Censoring 1 Failure 2 * • Censoring Loss to Follow-up 3 * 4 T 0 2T Time Since Start of Trial (T years) • Failure time is time from entry until the time of the event • Censoring means vital status of patient is not known beyond that point
Subject Administrative Censoring o 1 Failure 2 * • 3 Censoring Loss to Follow-up 4 * T 0 Follow-up Time (T years)
Clinical Trial with Common Termination Date Subject o 1 2 * • 3 • 4 o • 5 * • • 6 • • 7 • * 8 • 9 o o • 10 o * • 11 o o 0 T 2T Trial Terminated Follow-up Time (T years)
Reduced Sample Estimate (1) Years of Cohort Follow-Up Patients I II Total Entered 100 100 200 1 Died 20 25 45 Entered 80 75 155 2 Died 20 Survived 60
Reduced Sample Estimate (2) • Suppose we estimate the 1 year survival rate a. P(1 yr) = 155/200 = .775 b. P(1 yr, cohort I) = 80/100 = .80 c. P(1 yr, cohort II) = 75/100 = .75 • Now estimate 2 year survival Reduced sample estimate = 60/100 = 0.60 Estimate is based on cohort I only Loss of information
Actuarial Estimate (1) • Ref: Berkson & Gage (1950) Proc of Mayo Clinic • Cutler & Ederer (1958) JCD • Elveback (1958) JASA • Kaplan & Meier (1958) JASA • - Note that we can express P(2 yr survival as • P(2 yrs) = P(2 yrs survival|survived 1st yr) • P(1st yr survival) • = (60/80) (155/200) • = (0.75) (0.775) • = 0.58 • This estimate used all the available data
I1 I2 I3 I4 I5 t0 t1 t2 t3 t4 t5 Actuarial Estimate (2) • In general, divide the follow-up time into a series of intervals • Let pi = prob of surviving Ii given patient alive at beginning of Ii (i.e. survived through Ii -1) • Then prob of surviving through tk, P(tk)
Actuarial Estimate (3) Ii ti-1 ti - Define the following ni = number of subjects alive at beginning of Ii (i.e. at ti-1) di = number of deaths during interval Ii li= number of losses during interval Ii (either administrative or lost to follow-up) - We know only that di deaths and losses occurred in Interval Ii
Estimation of Pi • a. All deaths precede all losses • b. All losses precede all deaths • Deaths and losses uniform, • (1/2 deaths before 1/2 losses) • Actuarial Estimate/Cutler-Ederer • - Problem is that P(t) is a function of the interval choice. • - For some applications, we have no choice, but if we • know the exact date of deaths and losses, the • Kaplan‑Meier method is preferred.
Actuarial Lifetime Method (1) • Used when exact times of death are not known • Vital status is known at the end of an interval period (e.g. 6 months or 1 year) • Assume losses uniform over the interval
Actuarial Lifetime Method (2) Lifetable At Number Number Adjusted Prop Prop. Surv. Up to Interval Risk Died Lost No. At Risk Surviving End of Interval (ni) (di) (li) 0-1 50 9 0 50 41/50-0.82 0.82 1-2 41 6 1 41-1/2=40.5 34.5/40.5=0.852 0.852 x 0.82=0.699 2-3 34 2 4 34-4/2=32 30/32=0.937 0.937 x 0.699=0.655 3-4 28 1 5 28-5/2=25.5 24.5/25.5=0.961 0.961 x 0.655=0.629 4-5 22 2 3 22-3/2=20.5 18.5/20.5=0.902 0.902 x 0.629=0.567
Actuarial Survival Curve 100 80 60 40 20 0 X ___ X___ X___ X___ X___ X___ 1 2 3 4 5
Kaplan-Meier Estimate (1)(JASA, 1958) • Assumptions • 1. "Exact" time of event is known • Failure = uncensored event • Loss = censored event • 2. For a "tie", failure always before loss • 3. Divide follow-up time into intervals such that • a. Each event defines left side of an interval • b. No interval has both deaths & losses
Kaplan-Meier Estimate (2)(JASA, 1958) • Then ni = # at risk just prior to death at ti • Note if interval contains only losses, Pi = 1.0 • Because of this, we may combine intervals with only losses with the previous interval containing only deaths, for convenience X———o—o—o——
Estimate of S(t) or P(t) Suppose that for N patients, there are K distinct failure (death) times. The Kaplan-Meier estimate of survival curves becomes P(t)=P (Survival t) K-M or Product Limit Estimate titi = 1,2,…,k where ni = ni-1 - li-1- di-1 li-1 =# censored events since death at ti-1 di-1 = # deaths at ti-1
Estimate of S(t) or P(t) • Variance of P(t) Greenwood’s Formula
KM Estimate (1) Example (see Table 14-2 in FFD) Suppose we follow 20 patients and observe the event time, either failure (death) or censored (+), as [0.5, 0.6+), [1.5, 1.5, 2.0+), [3.0, 3.5+, 4.0+), [4.8], [6.2, 8.5+, 9.0+), [10.5, 12.0+ (7 pts)] There are 6 distinct failure or death times 0.5, 1.5, 3.0, 4.8, 6.2, 10.5
KM Estimate (2) 1. failure at t1 = 0.5 [.5, 1.5) n1 = 20 d1 = 1 l1 = 1 (i.e. 0.6+) If t d [.5, 1.5), p(t) = p1 = 0.95 V [ P(t1) ] = [.95]2 {1/20(19)} = 0.0024 ^ ^
KM Estimate (4) Data [0.5, 0.6+), [1.5, 1.5, 2.0+), 3.0 etc. 2. failure at t2 = 1.5 n2 = n1 - d1 - R1 [1.5, 3.0) = 20 - 1 - 1 = 18 d2 = 2 R2 = 1 (i.e. 2.0+) If t d [1.5, 3.0), then P(t) = (0.95)(0.89) = 0.84 V [P(t2)] = [0.84]2 { 1/20(19) + 2/18(18-2) } = 0.0068
Life Table 14.2 Kaplan-Meier Life Table for 20 Subjects Followed for One Year Interval Interval Time Number of death nj djRj [.5,1.5) 1 .5 20 1 1 0.95 0.95 0.0024 [1.5,3.0) 2 1.5 18 2 1 0.89 0.84 0.0068 [3.0,4.8) 3 3.0 15 1 2 0.93 0.79 0.0089 [4.8,6.2) 4 4.8 12 1 0 0.92 0.72 0.0114 [6.2,10.5) 5 6.2 11 1 2 0.91 0.66 0.0135 [10.5, ) 6 10.5 8 1 7* 0.88 0.58 0.0164 nj: number of subjects alive at the beginning of the jth interval dj: number of subjects who died during the jth interval Rj : number of subjects who were lost or censored during the jth interval : estimate for pj, the probability of surviving the jth interval given that the subject has survived the previous intervals : estimated survival curve : variance of * Censored due to termination of study
Survival Curve Kaplan-Meier Estimate 1.0 o * 0.9 ^ * o * 0.8 o o * * Estimated Survival Cure [P(t)] 0.7 o o * o o 0.6 o o * o o o 0.5 0 4 6 8 10 12 2 Survival Time t (Months)
Comparison of Two Survival Curves • Assume that we now have a treatment group and a control group and we wish to make a comparison between their survival experience • 20 patients in each group (all patients censored at 12 months) Control 0.5, 0.6+, 1.5, 1.5, 2.0+, 3.0, 3.5+, 4.0+, 4.8, 6.2, 8.5+, 9.0+, 10.5, 12+'s Trt1.0, 1.6+, 2.4+, 4.2+, 4.5, 5.8+, 7.0+, 11.0+, 12+'S
Kaplan-Meier Estimate for Treatment 1. t1 = 1.0 n1 = 20 p1 = 20 - 1 = 0.95 d1 = 1 20 l1 = 3 p(t) = .95 2. t2 = 4.5 n2 = 20 - 1 - 3 p2 = 16 - 1 =0 .94 = 16 16 d2 = 1 ^
Kaplan-Meier Estimate 1.0 o * TRT 0.9 * ^ * o * 0.8 o o * * Estimated Survival Cure [P(t)] 0.7 CONTROL o o * 0.6 o * o o o o 0.5 0 4 6 8 10 12 2 Survival Time t (Months)
Comparison of Two Survival Curves • Comparison of Point Estimates • Suppose at some time t* we want to compare PC(t*) for the control and PT(t*) for treatment • The statistic has approximately, a normal distribution under H0 • Example:
Comparison of Overall Survival Curve • H0: Pc(t) = PT(t) • A. Mantel-Haenszel Test • Ref: Mantel & Haenszel (1959) J Natl Cancer Inst • Mantel (1966) Cancer Chemotherapy Reports • - Mantel and Haenszel (1959) showed that a series of 2 x 2 • tables could be combined into a summary statistic • (Note also: Cochran (1954) Biometrics) • - Mantel (1966) applied this procedure to the comparison of • two survival curves • - Basic idea is to form a 2 x 2 table at each distinct death • time, determining the number in each group who were at • risk and number who died
Comparison of Two Survival Curves (1) • Suppose we have K distinct times for a death occurring • ti i = 1,2, .., K. For each death time, • Died At Risk • at ti Alive (prior to ti) • Treatment ai bi ai + bi • Control ci di ci + di • ai + ci bi + di Ni • Consider ai, the observed number of • deaths in the TRT group, under H0
Comparison of Two Survival Curves(2) E(ai) = (ai + bi)(ai + ci)/Ni CMantel-Haenszel Statistic
Table 14.3Comparison of Survival Data for a Control Group and an Intervention Group Using the Mantel-Haenszel Procedure Rank Event Intervention Control Total Times j tj aj + bj ajj cj + dj cjj aj + cj bj + dj 1 0.5 20 0 0 20 1 1 1 39 2 1.0 20 1 0 18 0 0 1 37 3 1.5 19 0 2 18 2 1 2 35 4 3.0 17 0 1 15 1 2 1 31 5 4.5 16 1 0 12 0 0 1 27 6 4.8 15 0 1 12 1 0 1 26 7 6.2 14 0 1 11 1 2 1 24 8 10.5 13 0 1 8 1 1 20 • aj + bj = number of subjects at risk in the intervention group prior to the death at time tj • cj + cj = number of subjects at risk in the control group prior to the death at time tj • aj = number of subjects in the intervention group who died at time tj • cj = number of subjects in the control group who died at time tj • j = number of subjects who were lost or censored between time tj and time tj+1 • aj + cj = number of subjects in both groups who died at time tj • bj + dj = number of subjects in both groups who are at risk minus the number who died at time tj
Mantel-Haenszel Test • Operationally • 1. Rank event times for both groups combined • 2. For each failure, form the 2 x 2 table • a. Number at risk (ai + bi, ci + di) • b. Number of deaths (ai, ci) • c. Losses (lTi, lCi) • Example (See table 14-3 FFD) - Use previous data set • Trt: 1.0, 1.6+, 2.4+, 4.2+, 4.5, 5.8+, 7.0+, 11.0+, 12.0+'s • Control: 0.5, 0.6+, 1.5, 1.5, 2.0+, 3.0, 3.5+, 4.0+, 4.8, 6.2, • 8.5+, 9.0+, 10.5, 12.0+'s
1. Ranked Failure Times - Both groups combined 0.5, 1.0, 1.5, 3.0, 4.5, 4.8, 6.2, 10.5 C T C C T C C C 8 distinct times for death (k = 8) 2. At t1 = 0.5 (k = 1) [.5, .6+, 1.0) T: a1 + b1 = 20 a1 = 0 lT1 = 0 c1 + d1 = 20 c1 = 1 lC1 = 1 1 loss @ .6+ D A R T 0 20 20 C 1 19 20 1 39 40 E(a1)= 1•20/40 = 0.5 V(a1) = 1•39 • 20 • 20 402 •39
E(a2)= 1•20 38 V(a2) = 1•37 • 20 • 18 382 •37 3. At t2 = 1.0 (k = 2) [1.0, 1.5) T: a2 + b2 = (a1 + b1) - a1 - lT1 a2 = 1.0 = 20 - 0 - 0 = 20 lT2 = 0 C. c2 + d2 = (c1 + d1) - c1 - lC1 c2 = 0 = 20 - 1 - 1 = 18 lC2 = 0 so D A R T 1 19 20 C 0 18 18 1 37 38
Eight 2x2 Tables Corresponding to the Event TimesUsed in the Mantel-Haenszel Statistic in Survival Comparison of Treatment (T) and Control (C) Groups 1. (0.5 mo.)* D† A‡ R§ 5. (4.5 mo.)* D A R T 0 20 20 T 1 15 16 C 1 19 20 C 0 12 12 1 39 40 1 27 28 2. (1.0 mo) D A R 6. (4.8 mo.) D A R T 1 19 20 T 0 15 15 C 0 18 18 C 1 11 12 1 37 38 1 26 27 3. (1.5 mo.) D A R 7. (6.2 mo.) D A R T 0 19 19 T 0 14 14 C 2 16 18 C 1 10 11 2 35 37 1 24 25 4. (3.0 mo.) D A R 8. (10.5 mo.) D A R T 0 17 17 T 0 13 13 C 1 14 15 C 1 7 8 1 31 32 1 20 21 * Number in parentheses indicates time, tj, of a death in either group † Number of subjects who died at time tj ‡ Number of subjects who are alive between time tj and time tj+1 § Number of subjects who were at risk before the death at time tj R=D+A)
Compute MH Statistics Recall K = 1 K = 2 K = 3 t1 = 0.5 t2 = 1.0 t3 = 1.5 D A 0 20 20 1 19 20 1 39 40 D A 1 19 20 0 18 18 1 37 38 D A 0 19 19 2 16 18 2 35 37 a. ai = 2 (only two treatment deaths) b. E(ai ) = 20(1)/40 + 20(1)/38 + 19(2)/37 + . . . = 4.89 c. V(ai) = = 2.22 d. MH = (2 - 4.89)2/2.22 = 3.76 or ZMH =
B. Gehan Test (Wilcoxon) Ref: Gehan, Biometrika (1965) Mantel, Biometrics (1966) Gehan (1965) first proposed a modified Wilcoxon rank statistic for survival data with censoring. Mantel (1967) showed a simpler computational version of Gehan’s proposed test. 1. Combine all observations XT’s and XC’s into a single sample Y1, Y2, . . ., YNC + NT 2. Define Uijwhere i = 1, NC + NT j = 1, NC + NT -1 Yi < Yj and death at Yi Uij = 1 Yi > Yj and death at Yj 0 elsewhere 3. Define Ui i = 1, … , NC + NT
Gehan Test • Note: • Ui = {number of observed times definitely less than i} • {number of observed times definitely greater} • 4. Define W = S Ui (controls) • 5. V[W] = NCNT • Variance due to Mantel • 6. • Example (Table 14-5 FFD) • Using previous data set, rank all observations
The Gehan Statistics, Gi involves the scores Ui and is defined as G = W2/V(W) where W = Ui (Uis in control group only) and
Example of Gehan Statistics Scores Ui for Intervention and Control (C) Groups Observation Ranked Definitely Definitely = Ui i Observed Time Group Less More 1 0.5 C 0 39 -39 2 (0.6)* C 1 0 1 3 1.0 I 1 37 -36 4 1.5 C 2 35 -33 5 1.5 C 2 35 -33 6 (1.6) I 4 0 4 7 (2.0) C 4 0 4 8 (2.4) I 4 0 4 9 3.0 C 4 31 -27 10 (3.5) C 5 0 5 11 (4.0) C 5 0 5 12 (4.2) I 5 0 5 13 4.5 I 5 27 -22 14 4.8 C 6 26 -20 15 (5.8) I 7 0 7 16 6.2 C 7 24 -17 17 (7.0) I 8 0 8 18 (8.5) C 8 0 8 19 (9.0) C 8 0 8 20 10.5 C 8 20 -12 21 (11.0) I 9 0 9 22-40 (12.0) 12I, 7C 9 0 9 *Censored observations
Gehan Test • Thus W = (-39) + (1) + (-36) + (-33) + (4) + . . . . • = -87 • and V[W] = (20)(20) {(-39)2 +12 + (-36)2 + . . . } • (40)(39) • = 2314.35 • so • Note MH and Gehan not equal
Cox Proportional Hazards Model Ref: Cox (1972) Journal of the Royal Statistical Association • Recall simple exponential S(t) = e-lt • More complicated If l(s) = l, get simple model • Adjust for covariates • Cox PHM l(t,x) =l0(t) ebx
Cox Proportional Hazards Model • So • S(t1,X) = • = • = • Estimate regression coefficients (non-linear estimation) b, SE(b) • Example • x1 = 1 Trt • 2 Control • x2 = Covariate 1 • indicator of treatment effect, adjusted for x2, x3 , . . . • If no covariates, except for treatment group (x1), • PHM = logrank
Homework Problem 1. Kaplan-Meier 2. Gehan-Wilcoxon 3. Mantel-Haenszel a D = drug; P = placebo b In weeks c A = alive; D = dead Source: P.B. Gregory (1974)
Survival Analysis Summary • Time to event methodology very useful in multiple settings • Can estimate time to event probabilities or survival curves • Methods can compare survival curves • Can stratify for subgroups • Can adjust for baseline covariates using regression model • Need to plan for this in sample size estimation & overall design