Subgroup treatment effect pattern (STEP) fit for survival outcome
Source:R/fit_survival_step.R
fit_survival_step.Rd![[Stable]](figures/lifecycle-stable.svg)
This fits the subgroup treatment effect pattern (STEP) models for a survival outcome. The treatment arm variable must have exactly 2 levels, where the first one is taken as reference and the estimated hazard ratios are for the comparison of the second level vs. the first one.
The model which is fit is:
Surv(time, event) ~ arm * poly(biomarker, degree) + covariates + strata(strata)
where degree is specified by control_step().
fit_survival_step(
variables,
data,
control = c(control_step(), control_coxph())
)Arguments
- variables
(named
listofcharacter)
list of analysis variables: needstime,event,arm,biomarker, and optionalcovariatesandstrata.- data
(
data.frame)
the dataset containing the variables to summarize.- control
(named
list)
combined control list fromcontrol_step()andcontrol_coxph().
Value
A matrix of class step. The first part of the columns describe the subgroup intervals used
for the biomarker variable, including where the center of the intervals are and their bounds. The
second part of the columns contain the estimates for the treatment arm comparison.
Note
For the default degree 0 the biomarker variable is not included in the model.
See also
control_step() and control_coxph() for the available customization options.
Examples
# Testing dataset with just two treatment arms.
library(dplyr)
adtte_f <- tern_ex_adtte %>%
filter(
PARAMCD == "OS",
ARM %in% c("B: Placebo", "A: Drug X")
) %>%
mutate(
# Reorder levels of ARM to display reference arm before treatment arm.
ARM = droplevels(forcats::fct_relevel(ARM, "B: Placebo")),
is_event = CNSR == 0
)
labels <- c("ARM" = "Treatment Arm", "is_event" = "Event Flag")
formatters::var_labels(adtte_f)[names(labels)] <- labels
variables <- list(
arm = "ARM",
biomarker = "BMRKR1",
covariates = c("AGE", "BMRKR2"),
event = "is_event",
time = "AVAL"
)
# Fit default STEP models: Here a constant treatment effect is estimated in each subgroup.
step_matrix <- fit_survival_step(
variables = variables,
data = adtte_f
)
dim(step_matrix)
#> [1] 39 12
head(step_matrix)
#> Percentile Center Percentile Lower Percentile Upper Interval Center
#> [1,] 0.025 0 0.275 1.472755
#> [2,] 0.050 0 0.300 2.028546
#> [3,] 0.075 0 0.325 2.204086
#> [4,] 0.100 0 0.350 2.799776
#> [5,] 0.125 0 0.375 2.969998
#> [6,] 0.150 0 0.400 3.149068
#> Interval Lower Interval Upper n events loghr se ci_lower
#> [1,] 0.4459546 4.182444 39 29 0.03729601 0.4243013 -0.7943192
#> [2,] 0.4459546 4.349471 43 31 0.23246622 0.3881347 -0.5282639
#> [3,] 0.4459546 4.626913 46 32 0.07952492 0.3813113 -0.6678314
#> [4,] 0.4459546 4.805767 50 35 0.09020455 0.3638368 -0.6229026
#> [5,] 0.4459546 4.929816 53 37 0.15522702 0.3477999 -0.5264483
#> [6,] 0.4459546 5.020539 57 41 0.11135760 0.3332843 -0.5418676
#> ci_upper
#> [1,] 0.8689112
#> [2,] 0.9931963
#> [3,] 0.8268813
#> [4,] 0.8033117
#> [5,] 0.8369023
#> [6,] 0.7645828
# Specify different polynomial degree for the biomarker interaction to use more flexible local
# models. Or specify different Cox regression options.
step_matrix2 <- fit_survival_step(
variables = variables,
data = adtte_f,
control = c(control_coxph(conf_level = 0.9), control_step(degree = 2))
)
# Use a global model with cubic interaction and only 5 points.
step_matrix3 <- fit_survival_step(
variables = variables,
data = adtte_f,
control = c(control_coxph(), control_step(bandwidth = NULL, degree = 3, num_points = 5L))
)