Suppose we are planning a drug development program testing the superiority of an experimental treatment over a control treatment. Our drug development program consists of an exploratory phase II trial which is, in case of promising results, followed by a confirmatory phase III trial.
The drugdevelopR package enables us to optimally plan such programs using a utility-maximizing approach. To get a brief introduction, we presented a very basic example on how the package works in Introduction to planning phase II and phase III trials with drugdevelopR. Contrary to the basic setting, where only one phase III trial was planned, we now want to show how to plan several phase III trials using the package.
Suppose we are developing a new tumor treatment, exper. The
patient variable that we want to investigate is how long the patient
survives without further progression of the disease (progression-free
survival). This is a time-to-event outcome variable. Therefore, we will
use the function optimal_multitrial
, which calculates
optimal sample sizes and threshold decisions values for time-to-event
outcomes when several phase III trials are performed.
Within our drug development program, we will compare our experimental treatment exper to the control treatment contro. The treatment effect measure is given by θ = −log (HR), where the hazard ratio HR is the ratio of the hazard rates between the two groups. If we assume that the hazard of experiencing a progression is reduced by 75% in the treatment group compared to the control group, we have a hazard ratio of 0.75.
After installing the package according to the installation instructions, we can load it using the following code:
We insert the same input values as in the example for time-to-event endpoints. As in the basic setting, the treatment effect may be fixed or follow a prior distribution. Furthermore, some options to adapt the program to your specific needs are also available in this setting, however skipping phase II, setting predefined benefit categories and choosing different treatment effects in phase II and III are not possible.
The package implements a framework developed for phase II/III drug development programs where several phase III trials are performed. This is of particular relevance as regulatory agencies often require statistical significance in two or more phase III trials. Different cases, defined by the number of significant trials needed for approval, are possible. For each case, different strategies are possible. They are defined by the number of phase III trials to be conducted in order to reach the goal of the case. For the success of the drug development program, it is necessary that the treatment effects of all phase III trials point in the same direction. For example, if we select case 3 and strategy 4, we require four phase III trials, where three need to be significant at level α and the treatment effect of the fourth must point in the same direction.
The following cases and possible strategies are implemented in the package.
Case | Possible strategies for this case |
---|---|
1 | 1, 2 |
2 | 1 (with significance level of α2)* , 2, 3, 23* |
3 | 1 (with significance level of α3)*, 3, 4 |
Note that setting case = 1
and strategy = 1
would lead to the same results as in the basic setting. There are two
special strategies which we marked with a * in the table:
strategy = 1
in cases 2 and 3 leads to a
situation where one large phase III trial is conducted with adjusted
significance level, i.e. αnew = α2
in case 2 and αnew = α3
in case 3. This feature is implemented as there is discussion that a
larger trial with adjusted significance level may also may serve
evidence on efficacy (see Koch (2005)).So, in addition to the parameters from the basic setting, we provide the following parameters:
case
allows us to chose the number of
trials in phase III that have to show a significant positive treatment
effect for the whole program to be deemed successful. In the following
example we set the parameter case = 3
, indicating that at
least two trials in phase III have to show a significant treatment
effect in phase III.strategy
defines the number of trials
that are conducted in phase III. The strategies 1, 2, 3, and 4 (and 23)
are implemented. Setting strategy = TRUE
returns the
results of the optimization for all implemented strategies for a
specific case. Note that not all strategies are implemented for each
case (see table above). For the following example we set
strategy = TRUE
.Note that for the following example, some input parameters were changed compared to the basic setting in order to reduce computation time.
res <- optimal_multitrial(w = 0.3, # define parameters for prior
hr1 = 0.7, hr2 = 0.8, id1 = 210, id2 = 420, # (https://web.imbi.uni-heidelberg.de/prior/)
d2min = 20, d2max = 200, stepd2 = 5, # define optimization set for d2
hrgomin = 0.7, hrgomax = 0.9, stephrgo = 0.02, # define optimization set for HRgo
alpha = 0.025, beta = 0.1, xi2 = 0.7, xi3 = 0.7, # drug development planning parameters
c2 = 0.75, c3 = 1, c02 = 100, c03 = 150, # define fixed and variable costs
K = Inf, N = Inf, S = -Inf, # set constraints
b1 = 1000, b2 = 2000, b3 = 3000, # define expected benefits
fixed = TRUE, # choose if effects are fixed or random
case = 3, strategy = TRUE # choose case and strategy
num_cl = 3)
After setting all these input parameters and running the function, let’s take a look at the output of the program.
res
#> Optimization result with 3 significant trial(s) needed, strategy 1:
#> Utility: -231.07
#> Sample size:
#> phase II: 30, phase III: 368, total: 398
#> Expected number of events:
#> phase II: 20, phase III: 258, total: 278
#> Assumed event rate:
#> phase II: 0.7, phase III: 0.7
#> Probability to go to phase III: 0.57
#> Total cost:
#> phase II: 122, phase III: 454, cost constraint: Inf
#> Fixed cost:
#> phase II: 100, phase III: 150
#> Variable cost per patient:
#> phase II: 0.75, phase III: 1
#> Effect size categories (expected gains):
#> small: 1 (1000), medium: 0.95 (2000), large: 0.85 (3000)
#> Success probability: 0.19
#> Joint probability of success and observed effect of size ... in phase III:
#> small: 0.06, medium: 0.11, large: 0.02
#> Significance level: 1.5625e-05
#> Targeted power: 0.9
#> Decision rule threshold: 0.76 [HRgo]
#> Assumed true effect: 0.7 [hr]
#> Treatment effect offset between phase II and III: 0 [gamma]
#>
#> Optimization result with 3 significant trial(s) needed, strategy 3:
#> Utility: -411.1
#> Sample size:
#> phase II: 30, phase III: 258, total: 288
#> Expected number of events:
#> phase II: 20, phase III: 180, total: 200
#> Assumed event rate:
#> phase II: 0.7, phase III: 0.7
#> Probability to go to phase III: 0.5
#> Total cost:
#> phase II: 122, phase III: 483, cost constraint: Inf
#> Fixed cost:
#> phase II: 100, phase III: 150
#> Variable cost per patient:
#> phase II: 0.75, phase III: 1
#> Effect size categories (expected gains):
#> small: 1 (1000), medium: 0.95 (2000), large: 0.85 (3000)
#> Success probability: 0.08
#> Joint probability of success and observed effect of size ... in phase III:
#> small: 0, medium: 0.05, large: 0.03
#> Significance level: 0.025
#> Targeted power: 0.9
#> Decision rule threshold: 0.7 [HRgo]
#> Assumed true effect: 0.7 [hr]
#> Treatment effect offset between phase II and III: 0 [gamma]
#>
#> Optimization result with 3 significant trial(s) needed, strategy 4:
#> Utility: -436.79
#> Sample size:
#> phase II: 58, phase III: 416, total: 474
#> Expected number of events:
#> phase II: 40, phase III: 292, total: 332
#> Assumed event rate:
#> phase II: 0.7, phase III: 0.7
#> Probability to go to phase III: 0.5
#> Total cost:
#> phase II: 144, phase III: 716, cost constraint: Inf
#> Fixed cost:
#> phase II: 100, phase III: 150
#> Variable cost per patient:
#> phase II: 0.75, phase III: 1
#> Effect size categories (expected gains):
#> small: 1 (1000), medium: 0.95 (2000), large: 0.85 (3000)
#> Success probability: 0.2
#> Joint probability of success and observed effect of size ... in phase III:
#> small: 0, medium: 0.17, large: 0.02
#> Significance level: 0.025
#> Targeted power: 0.9
#> Decision rule threshold: 0.7 [HRgo]
#> Assumed true effect: 0.7 [hr]
#> Treatment effect offset between phase II and III: 0 [gamma]
The program returns a data frame where the output for all implemented strategies is listed.
For strategy 1 we get:
res[1,]$d2
is the optimal number of events for phase II
and res[1,]$d3
the resulting number of events for phase
III. We see that the optimal scenario requires 20 events in phase II and
258 events in phase III, which correspond to 30 participants in phase II
and 368 in phase III.res[1,]$HRgo
is the optimal threshold value for the
go/no-go decision rule. We see that we need a hazard ratio of less than
0.76 in phase II in order to proceed to phase III.res[1,]$u
is the expected utility of the program for
the optimal sample size and threshold value. In our case it amounts to
-231.07, i.e. we have an expected utility of -23 107 000$.alpha
is returned having
a value of 0.000016, which corresponds to the adjusted significance
level α3.The results for strategy 3 are:
res[2,]$d2
is the optimal number of events for phase II
and res[2,]$d3
the resulting number of events for phase
III. We see that the optimal scenario requires 20 events in phase II and
180 events in phase III, which leads to 30 participants in phase II and
258 in phase III. This corresponds to three trials in phase III with
each trial having 86 participants.res[2,]$HRgo
is the optimal threshold value for the
go/no-go decision rule. We see that we need a hazard ratio of less than
0.7 in phase II in order to proceed to phase III.res[2,]$u
is the expected utility of the program for
the optimal sample size and threshold value. In our case it amounts to
-411.1, i.e. we have an expected utility of -41 110 000$.Strategy 4 yields the following results:
res[3,]$d2
is the optimal number of events for phase II
and res[3,]$d3
the resulting number of events for phase
III. We see that the optimal scenario requires 40 events in phase II and
292 events in phase III, which leads to 58 participants in phase II and
416 in phase III. This corresponds to four trials in phase III with each
trial having 104 participants.res[3,]$HRgo
is the optimal threshold value for the
go/no-go decision rule. We see that we need a hazard ratio of less than
0.70 in phase II in order to proceed to phase III.res[3,]$u
is the expected utility of the program for
the optimal sample size and threshold value. In our case it amounts to
-436.79, i.e. we have an expected utility of -43 679 000$.In this article we presented an example where several phase III
trials are conducted. Note that this example is not restricted to
time-to-event endpoints but can also be applied to binary and normally
distributed endpoints by using the functions
optimal_multitrial_binary
and
optimal_multitrial_normal
. For more information on how to
use the package, see:
Koch, G. G. (2005). Statistical consideration of the strategy for demonstrating clinical evidence of effectiveness one larger vs two smaller pivotal studies by z. shun, e. chi, s. durrleman and l. fisher, statistics in medicine 2005; 24: 1619–1637. Statistics in Medicine, 24(11):1639–1646.