Phobic Disorders Clinical Trial
Official title:
Glucocorticoid Treatment for Social Phobia
Social phobia is the third most common psychiatric disorder besides depression and
alcoholism. Several studies have demonstrated the efficacy of cognitive-behavioral therapy
in the treatment of social phobia. Nevertheless, there is no effect in a third of the people
at the existing treatment methods. Pharmacological therapies have similar effects, but there
is a high rate of relapse after discontinuation of medication.
Social phobia is characterized by fear of performance or interaction situations. The strong
fear of negative evaluation by others is usually accompanied by a marked avoidance behavior
and increased physical symptoms such as blushing, sweating, palpitations, or tremors. The
confrontation with a phobic stimulus leads to a retrieval of stimulus-associated aversive
memories, resulting in an immediate anxiety response. Several studies had already shown that
elevated glucocorticoids impair retrieval of declarative memory contents in healthy
subjects. The investigators demonstrated an anxiety-reducing effect after the administration
of cortisone before the confrontation with a phobic stimulus in patients with social and
spider phobia.
Background
Anxiety disorders have major public health significance and social phobia ranks as the third
most common mental health disorder after depression and alcoholism. Even though
cognitive-behavioral therapy (CBT) is the most effective non-pharmacological approach to the
treatment of social phobia, more than one third of the patients do not respond to treatment,
or achieve only partial remission of symptoms. Pharmacotherapy (e.g., SSRIs,
benzodiazepines) has been shown to be effective in the acute treatment of social phobia,
however, with high rates of relapse when medication is discontinued. In addition, the
combination of CBT and medication does not seem to be more beneficial than CBT alone.
Consequently, the development of innovative psychobiological approaches combining effective
psychotherapy methods with synergizing substance administration is a primary challenge in
interdisciplinary research on treatment of social phobia.
In a recent study the investigators found evidence that a pharmacological elevation of
glucocorticoid levels reduces fear in patients with social phobia and spider phobia exposed
to a phobic stimulus. Furthermore, the investigators have shown that repeated administration
of glucocorticoids before exposure to a phobic stimulus leads to an extinction of phobic
fear. Also the low-dose administration of cortisone over a month in patients with
post-traumatic stress disorder reduces cardinal of symptoms the disorder. Based on these
findings, glucocorticoid treatment, in combination with exposure therapy, may help to reduce
fear and promote extinction of phobic fear.
In an interdisciplinary research project involving psychology, behavioral pharmacology
psychiatry, genetics and neuroimaging the investigators propose to investigate the
therapeutic efficacy of combining an exposure-based cognitive-behavioral group therapy
(CBGT) with hydrocortisone treatment. The investigators hypothesize that hydrocortisone
exerts both acute beneficial effects by reducing fear during exposure, and long-term
beneficial effects by facilitating the extinction of phobic fear. Furthermore, the
investigators hypothesize differential treatment responses depending on genetic variations
in glucocorticoid-related genes (substudy 1). These hypotheses will be tested in a clinical
study with 100 patients with mainly speech anxiety who fulfill DSM-IV criteria for a
diagnosis of social phobia and 60 patients with spider phobia.
This is the first study aimed at determining the therapeutic efficacy of combining
hydrocortisone administration and a short-term exposure-based cognitive-behavioral group
therapy for the treatment of social phobic patients with specific speech anxiety and
patients with spider phobia. Considering the large number of patients suffering from social
phobia, the suggested interdisciplinary project will have important clinical implications
for the development of a more effective therapy.
Objective
To determine whether short-term treatment with 20 mg hydrocortisone enhances the efficacy of
exposure-based cognitive-behavioral group therapy (CBGT) in patients with social phobia,
specifically speech anxiety and patients with spider phobia.
A series of studies indicate that elevated glucocorticoid levels inhibit the retrieval of
memory in healthy humans. Further the low-dose administration of glucocorticoids over a
month inhibited the retrieval of traumatic memories in patients with post traumatic stress
disorder. These findings suggest that glucocorticoids might also inhibit retrieval of fear
memory in phobia and social phobia exposed to a phobic stimulus. Additionally, the
investigators found evidence indicating that repeated administration of glucocorticoids
before exposure to a phobic stimulus leads to an extinction of phobic fear. Based on these
findings, glucocorticoid treatment, in combination with exposure therapy, may help to reduce
fear and promote extinction of phobic fear.
Methods
In a placebo-controlled double-blind study design, patients will be randomly assigned to
receive CBGT + hydrocortisone (Social Phobia: N=50 / Spider Phobia: N=30) or CBGT + placebo
(Social Phobia: N=50 / Spider Phobia: N=30). Psychopathological symptoms and stress
reactivity will be assessed by psychometric and endocrine parameters before, during and
after CBGT therapy. The patients have further the possibility to attend to a neuroimaging
study, in which the investigators examine and localize the anxiolytic effect of acute
glucocorticoid administration in the brain (substudy 2). In this substudy 2 the
investigators compare the patients with social phobia with patients with specific spider
phobia and healthy controls as they did in their previous studies (Soravia et al. 2006).
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator), Primary Purpose: Treatment
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