Anxiety Disorders Clinical Trial
Official title:
Initial Severity and Antidepressant Efficacy for Anxiety Disorders: an Individual Patient Data Meta-analysis
Anxiety disorders are common disorders, which pose a major burden to society and the individual. An anxiety disorder may be treated with medication, in particular with antidepressants such as the selective serotonin reuptake inhibitors (SSRIs). However, much of what is known about antidepressants is derived from research in depression rather than anxiety. In recent years, researchers have found that antidepressants are more effective for severely depressed patients than they are for patients with milder symptoms. It is possible that a similar relationship between symptom severity and antidepressant efficacy exists for anxiety disorders, but there is currently little evidence available to answer this question. As antidepressants are frequently prescribed to patients with mild or moderate anxiety, a clear understanding of their effectiveness across the severity range is vital to inform treatment decisions. Therefore, the purpose of this meta-analysis is to examine whether initial symptom severity affects antidepressant efficacy for anxiety disorders.
Study design:
The proposed project is an individual patient data meta-analysis. The investigators will
collate data from 29 randomized controlled trials of second-generation antidepressants
(specifically: paroxetine, paroxetine controlled release (CR), duloxetine, and fluoxetine)
for the short-term treatment of an anxiety disorder, including a total of approximately
8,800 participants. The anxiety disorders that are included in the proposed project are
generalized anxiety disorder (GAD), social anxiety disorder (SAD), obsessive-compulsive
disorder (OCD), post-traumatic stress disorder (PTSD), and panic disorder (PD). Generalized
linear mixed models will be used to investigate whether initial symptom severity is related
to antidepressant efficacy.
Statistical analysis plan:
A separate longitudinal analysis will be conducted for each disorder. For GAD, SAD, OCD, and
PTSD, linear mixed models will be used; for PD, a generalized linear mixed model (multilevel
negative binomial regression) will be used, as the dependent variable for this disorder
(number of panic attacks) is a discrete count variable. Maximum likelihood estimation will
be used as the estimation method for the linear mixed models, while Laplace approximation
will be used as the estimation method for the multilevel negative binomial regression for
PD. In all models, measurement occasion represents level 1, participants represent level 2,
and trial represents level 3. The effect measure of interest is the change in symptoms from
baseline, except for PD, for which the effect measure of interest is the total number of
panic attacks per two weeks.
The initial model will be built by including all the fixed effects of interest, regardless
of significance. These include initial severity, treatment group and covariates (see below).
Linear and quadratic terms for time (in days since baseline) will be included. For each
participant, the actual visit dates will be used (if available) rather than the intended
weekly visit date. The following two- and three-way interactions will also be included:
severity x group, severity x linear time, group x linear time, severity x group x linear
time, severity x quadratic time, group x quadratic time, severity x group x quadratic time.
Using this first model, the variance-covariance structure of the nested data will be modeled
by including random effects. Random effects for study, subject and (linear and quadratic)
time, as well as various covariance structures (unstructured, autocorrelated errors,
Toeplitz, etc.) will be considered. Restricted maximum likelihood (REML) will be used for
estimation, and the best-fitting model will be selected based upon the Akaike Information
Criterion (AICc).
In this best-fitting model, backward selection with maximum likelihood (ML) will be used to
select the significant fixed effects. Non-significant interaction terms will be removed from
the model (unless the three-way interaction of group x severity x (linear or quadratic) time
is significant, in which case all two-way interactions and main effects that use these
variables will be retained). The best-fitting model will again be selected based upon the
Akaike Information Criterion (AICc).
Covariates: Models with and without the following covariates will be tested: age, gender,
and duration of illness (if available). Only the main effect of these covariates will be
included; no interactions with other variables will be included.
Missing data: Baseline variables (such as initial severity) are likely to be essentially
complete, but some change scores are likely to be missing due to dropout or missed
measurement occasions. The assumption is made that these data are missing at random (MAR),
that is: missingness of the dependent variable may depend upon observed variables (such as
previous symptom scores or covariates), but it does not depend upon the value of the
unobserved (missing) variable. When MAR holds, the mixed model yields unbiased estimates of
coefficients and standard errors even when some data is missing, and no other methods for
handling missing data are required.
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