The hardware and bandwidth for this mirror is donated by dogado GmbH, the Webhosting and Full Service-Cloud Provider. Check out our Wordpress Tutorial.
If you wish to report a bug, or if you are interested in having us mirror your free-software or open-source project, please feel free to contact us at mirror[@]dogado.de.
In epidemiologic studies polytomous logistic regression is commonly
used in the study of etiologic heterogeneity when data are from a
case-control study, and the method has good statistical properties.
Although polytomous logistic regression can be implemented using
available software, the additional calculations needed to perform a
thorough analysis of etiologic heterogeneity are cumbersome. To
facilitate use of this method we provide functions
eh_test_subtype()
and eh_test_marker()
to
address two key questions regarding etiologic heterogeneity:
Whether disease subtypes are pre-specified or formed by cross-classification of individual disease markers, the resulting polytomous logistic regression model is the same. Let \(i\) index study subjects, \(i = 1, \ldots, N\), let \(m\) index disease subtypes, \(m = 0, \ldots M\), where \(m=0\) denotes control subjects, and let \(p\) index risk factors, \(p = 1, \ldots, P\). The polytomous logistic regression model is specified as
\[\Pr(Y = m | \mathbf{X}) = \frac{\exp(\mathbf{X}^T \boldsymbol{\beta}_{\boldsymbol{\cdot} m})}{\mathbf{1} + \exp(\mathbf{X}^T \boldsymbol{\beta}) \mathbf{1}}\] where \(\mathbf{X}\) is the \((P+1) \times N\) matrix of risk factor values, with the first row all ones for the intercept, and \(\boldsymbol{\beta}\) is the \((P+1) \times M\) matrix of regression coefficients. \(\boldsymbol{\beta}_{\boldsymbol{\cdot} m}\) indicates the \(m\)th column of the matrix \(\boldsymbol{\beta}\) and \(\mathbf{1}\) represents a vector of ones of length \(M\).
If disease subtypes are pre-specified, either based on clustering
high-dimensional disease marker data or based on a single disease marker
or combinations of disease markers, then statistical tests for etiologic
heterogeneity according to each risk factor can be conducted using the
eh_test_subtype()
function.
Estimates of the parameters of interest related to the question of whether risk factor effects differ across subtypes of disease, \(\hat{\boldsymbol{\beta}}\), and the associated estimated variance-covariance matrix, \(\widehat{cov}(\hat{\boldsymbol{\beta}})\), are obtained directly from the resulting polytomous logistic regression model. Each \(\beta_{pm}\) parameter represents the log odds ratio for a one-unit change in risk factor \(p\) for subtype \(m\) disease versus controls. Hypothesis tests for the question of whether a specific risk factor effect differs across subtypes of disease can be conducted separately for each risk factor \(p\) using a Wald test of the hypothesis
\[H_{0_{\beta_{p.}}}: \beta_{p1} = \dots =
\beta_{pM}\] Using the subtype_data
simulated
dataset, we can examine the influence of risk factors x1
,
x2
, and x3
on the 4 pre-specified disease
subtypes in variable subtype
using the following code:
library(riskclustr)
mod1 <- eh_test_subtype(
label = "subtype",
M = 4,
factors = list("x1", "x2", "x3"),
data = subtype_data)
See the function documentation for details of function arguments.
The resulting estimates \(\hat{\boldsymbol{\beta}}\) can be accessed with
1 | 2 | 3 | 4 | |
---|---|---|---|---|
x1 | 1.5555082 | 0.8232515 | 0.2410591 | 0.1086845 |
x2 | 0.3031594 | 0.4335048 | 0.3518870 | 0.3714092 |
x3 | 0.8000998 | 1.9909315 | 3.0115985 | 1.5594139 |
the associated standard deviation estimates \(\sqrt{\widehat{var}(\hat{\boldsymbol{\beta}})}\) with
1 | 2 | 3 | 4 | |
---|---|---|---|---|
x1 | 0.0875330 | 0.0749353 | 0.0758686 | 0.0693273 |
x2 | 0.0783898 | 0.0732283 | 0.0759600 | 0.0697852 |
x3 | 0.2246070 | 0.1833106 | 0.1783101 | 0.1823138 |
and the heterogeneity p-values with
p_het | |
---|---|
x1 | 0.0000000 |
x2 | 0.4778092 |
x3 | 0.0000000 |
An overall formatted dataframe containing \(\hat{\boldsymbol{\beta}}
\Big(\sqrt{\widehat{var}(\hat{\boldsymbol{\beta}})}\Big)\) and
heterogeneity p-values p_het
to test the null hypotheses
\(H_{0_{\beta_{p.}}}\) can be obtained
as
1 | 2 | 3 | 4 | p_het | |
---|---|---|---|---|---|
x1 | 1.56 (0.09) | 0.82 (0.07) | 0.24 (0.08) | 0.11 (0.07) | <.001 |
x2 | 0.3 (0.08) | 0.43 (0.07) | 0.35 (0.08) | 0.37 (0.07) | 0.478 |
x3 | 0.8 (0.22) | 1.99 (0.18) | 3.01 (0.18) | 1.56 (0.18) | <.001 |
Because it is often of interest to examine associations in a
case-control study on the odds ratio (OR) scale rather than the original
parameter estimate scale, it is also possible to obtain a matrix
containing \(OR=\exp(\hat{\boldsymbol{\beta}})\), along
with 95% confidence intervals and heterogeneity p-values
p_het
to test the null hypotheses \(H_{0_{\beta_{p.}}}\) using
1 | 2 | 3 | 4 | p_het | |
---|---|---|---|---|---|
x1 | 4.74 (3.99-5.62) | 2.28 (1.97-2.64) | 1.27 (1.1-1.48) | 1.11 (0.97-1.28) | <.001 |
x2 | 1.35 (1.16-1.58) | 1.54 (1.34-1.78) | 1.42 (1.23-1.65) | 1.45 (1.26-1.66) | 0.478 |
x3 | 2.23 (1.43-3.46) | 7.32 (5.11-10.49) | 20.32 (14.33-28.82) | 4.76 (3.33-6.8) | <.001 |
If disease subtypes are formed by cross-classifying individual binary
disease markers, then statistical tests for associations between risk
factors and individual disease markers can be conducted using the
eh_test_marker()
funtion.
Let \(k\) index disease markers, \(k = 1, \ldots, K\). Here the \(M\) disease subtypes are formed by cross-classification of the \(K\) binary disease markers, so that we have \(M = 2^K\) disease subtypes.
To evaluate the independent influences of individual disease markers, it is convenient to transform the parameters in \(\boldsymbol{\beta}\) using the one-to-one linear transformation
\[\hat{\boldsymbol{\gamma}} = \frac{\hat{\boldsymbol{\beta}} \mathbf{L}}{M/2}.\] Here \(\mathbf{L}\) is an \(M \times K\) contrast matrix such that the entries are -1 if disease marker \(k\) is absent for disease subtype \(m\) and 1 if disease marker \(k\) is present for disease subtype \(m\). \(\boldsymbol{\gamma}\) is then the \((P+1) \times K\) matrix of parameters that reflect the independent effects of distinct disease markers. Each element of the \(\boldsymbol{\gamma}\) parameters represents the average of differences in log odds ratios between disease subtypes defined by different levels of the \(k\)th disease marker with respect to the \(p\)th risk factor when the other disease markers are held constant. Variance estimates corresponding to each \(\hat{\gamma}_{pk}\) are obtained using
\[\widehat{var}(\hat{\gamma}_{pk}) = \left(\frac{M}{2}\right)^{-2} \mathbf{L}_{\boldsymbol{\cdot} k}^T \widehat{cov}(\hat{\boldsymbol{\beta}}_{p \boldsymbol{\cdot}}^T) \mathbf{L}_{\boldsymbol{\cdot} k}\] where \(\mathbf{L}_{\boldsymbol{\cdot} k}\) is the \(k\)th column of the \(\mathbf{L}\) matrix and the estimated variance-covariance matrix \(\widehat{cov}(\hat{\boldsymbol{\beta}}_{p \boldsymbol{\cdot}})\) for each risk factor \(p\) is obtained directly from the polytomous logistic regression model.
Hypothesis tests for the question of whether a risk factor effect differs across levels of each individual disease marker of which the disease subtypes are comprised can be conducted separately for each combination of risk factor \(p\) and disease marker \(k\) using a Wald test of the hypothesis
\[H_{0_{{\gamma_{pk}}}}: \gamma_{pk} =
0.\] Using the subtype_data
simulated dataset, we
can examine the influence of risk factors x1
,
x2
, and x3
on the two individual disease
markers marker1
and marker2
. These two binary
disease markers will be cross-classified to form four disease subtypes
that will be used as the outcome in the polytomous logistic regression
model to obtain the \(\hat{\boldsymbol{\beta}}\) estimates, which
are then transformed in order to obtain estimates and hypothesis tests
related to the individual disease markers.
library(riskclustr)
mod2 <- eh_test_marker(
markers = list("marker1", "marker2"),
factors = list("x1", "x2", "x3"),
case = "case",
data = subtype_data)
See the function documentation for details of function arguments.
The resulting estimates \(\hat{\boldsymbol{\gamma}}\) can be accessed with
marker1 | marker2 | |
---|---|---|
x1 | -1.0145081 | -0.4323157 |
x2 | -0.0066840 | 0.0749338 |
x3 | 0.8899905 | -0.1306765 |
the associated standard deviation estimates \(\sqrt{\widehat{var}(\hat{\boldsymbol{\gamma}})}\) with
marker1 | marker2 | |
---|---|---|
x1 | 0.0681025 | 0.0601803 |
x2 | 0.0631465 | 0.0588423 |
x3 | 0.1450606 | 0.1348479 |
and the associated p-values with
marker1 | marker2 | |
---|---|---|
x1 | 0.0000000 | 0.0000000 |
x2 | 0.9157016 | 0.2028521 |
x3 | 0.0000000 | 0.3325126 |
An overall formatted dataframe containing the \(\hat{\boldsymbol{\gamma}} \Big(\sqrt{\widehat{var}(\hat{\boldsymbol{\gamma}})}\Big)\) and p-values to test the null hypotheses \(H_{0_{\gamma_{pk}}}\) can be obtained as
marker1 est | marker1 pval | marker2 est | marker2 pval | |
---|---|---|---|---|
x1 | -1.01 (0.07) | <.001 | -0.43 (0.06) | <.001 |
x2 | -0.01 (0.06) | 0.916 | 0.07 (0.06) | 0.203 |
x3 | 0.89 (0.15) | <.001 | -0.13 (0.13) | 0.333 |
The estimates and heterogeneity p-values for disease subtypes formed
by cross-classifying these individual disease markers can also be
accessed in objects beta_se_p
and or_ci_p
, as
described in the section on Pre-specified
subtypes.
These binaries (installable software) and packages are in development.
They may not be fully stable and should be used with caution. We make no claims about them.
Health stats visible at Monitor.