Providing Tools for Effective Care and Treatment of Anxiety Disorders

Providing Tools for Effective Care and Treatment of Anxiety Disorders (AD): Outcomes, Mediators and Moderators of Enhanced Extinction

Status

Completed

Phases

Study type

Interventional

Source

ClinicalTrials.gov

Registry ID

NCT02605668

Acronym

PROTECT-AD

Enrollment

726

Registered

2015-11-16

Start date

2015-12-12

Completion date

2019-07-24

Last updated

2019-09-16

For informational purposes only — not medical advice. Sourced from public registries and may not reflect the latest updates. Terms

Conditions

Panic Disorder, Agoraphobia, Specific Phobias, Social Anxiety Disorder

Keywords

Anxiety Disorders, Extinction Learning, Optimized Extinction, Behavioral Therapy, Massed Confrontation, Social Anxiety Disorder, Specific Phobia, Panic Disorder, Agoraphobia

Brief summary

PROTECT-AD is a cognitive behavioral treatment study involving highly qualified psychotherapeutic centers at seven German universities. It is our goal to further investigate and optimize existing effective treatments of anxiety disorders. In order to achieve this, the investigators want to investigate the effect of extinction learning in an intensified psychological intervention on treatment outcome in adults and children with anxiety disorders. The intensified psychological intervention is characterized by a higher number of exposure trials over a short time period. In the control condition the exposure trials take place in a weekly interval, analog to standard care.

Detailed description

Novel preclinical research evidence suggests extinction learning as the core mechanism of action of exposure-based therapies and provides according strategies to improve the effectiveness of treatment by optimized extinction. A translational research agenda is suggested to examine whether enhanced extinction learning components derived from preclinical research, applied within an intensified exposure-based treatment, improves outcomes. In a multicenter randomized clinical trial, linked to mechanistic subprojects, the investigators test in n=620 patients with primary AD allowing for comorbidity whether intensified psychological interventions based on augmented extinction learning (IPI) result in faster, stronger and more persistent outcomes on subjective, clinical, behavioral, physiological and neural indices as compared to an, otherwise identical, standard research treatment without explicit enhanced extinction (TAU). The investigators hypothesize that (a) enhanced extinction elements (IPI) will result in higher effect sizes, faster recovery, (b) more pronounced changes in an array of systems, including elements of extinction learning and in objective behavioral measures assessed in intersession exposure trials. The investigators also examine moderators of outcome (i.e. type of diagnosis, comorbidity) and explore whether IPI is associated with lower health care costs.

Interventions

BEHAVIORALIntensified psychological intervention

12 sessions of Cognitive Behavioral Therapy a 100 minutes, over the course of 6 weeks (2 sessions per week/week 1 and 2, 3 sessions per week/week 3 und 4, 1 session per week/week 5 and 6)

BEHAVIORALStandard intervention

12 sessions of Cognitive Behavioral Therapy a 100 minutes, over the course of 10 weeks (2 sessions per week/week 1 and 2, 1 session per week/week 3 to 10)

Study design

Allocation

RANDOMIZED

Intervention model

PARALLEL

Primary purpose

TREATMENT

Masking

NONE

Eligibility

Sex/Gender

ALL

Age

15 Years to 70 Years

Healthy volunteers

Inclusion criteria

* age 15 - 70 years * one or more of the following DSM-IV/5 anxiety disorders: Panic Disorder, Agoraphobia, Social Anxiety Disorder, Specific Phobia * HAMA - Score \> 18 * CGI - Score \> 3 * Can attend therapy regularly (with or without support) * Informed Consent

Exclusion criteria

* Every reason the protocol may not be upheld (e.g. planned hospitalization within study time frame, planning to move away, etc.) * Current suicidal tendency * DSM-5 Bipolar Disorder * DSM-5 Psychotic Disorder * DSM-5 Borderline Personality Disorder * Current treatment of other mental disorder (drugs, psychotherapy) * Current Alcohol, Benzodiazepine or other Substance Use Disorders * Severe medical illness/condition (every serious physical illness, including cardiovascular, kidney, endocrinological and neurological conditions, Hepatitis or other clinical findings that suggest a severe illness and may affect participation in the study)

Design outcomes

Primary

Measure	Time frame	Description
change in somatic and psychic anxiety symptoms	assessed three times: Baseline, Post (1 week after end of therapy) and Follow up (6 months after end of therapy)	Anxiety symptoms are assessed using the clinician-rated Structured Interview Guide for the Hamilton Anxiety Scale (SIGH-A for the HAMA). Stronger, faster and more persistent reduction of anxiety symptoms in the IPI group than in the TAU group is expected.

Secondary

Measure	Time frame	Description
change in categorial diagnosis according to the Diagnostic and Statistical Manual of Mental Disorders (DSM-IV/5)	assessed three times: Baseline, Post (1 week after end of therapy) and Follow Up (6 months after end of therapy)	categorical diagnoses are assessed using a German version of the Composite International Diagnostic Interview (CIDI).
change in screened anxiety symptoms	assessed fivetimes: Baseline, therapy session 4 (week 2 of therapy), therapy session 11 (week 5 to week 9 of therapy), Post (1 week after end of therapy) and Follow Up (6 months after end of therapy)	The DSM-5 cross-cutting symptom measure for anxiety disorders (Cross-D) is used as a brief screener for anxiety symptoms.
change in depressive symptoms	assessed fivetimes: Baseline, therapy session 4 (week 2 of therapy), therapy session 11 (week 5 to week 9 of therapy), Post (1 week after end of therapy) and Follow Up (6 months after end of therapy)	depressive symptoms are assessed using the Beck Depression Inventory (BDI-II)
change in anxiety sensitivity	assessed three times: Baseline, Post (1 week after end of therapy) and Follow Up (6 months after end of therapy)	anxiety sensitivity is assessed using the Anxiety sensitivity inventory (ASI)
change in panic and agoraphobic symptoms	assessed three times: Baseline, Post (1 week after end of therapy) and Follow Up (6 months after end of therapy)	panic and agoraphobic symptoms are assessed using the Panic and agoraphobia scale (PAS)
change in agoraphobic avoidance	assessed three times: Baseline, Post (1 week after end of therapy) and Follow Up (6 months after end of therapy)	agoraphobic avoidance is assessed using the Mobility Inventory (MI)
change in symptoms of Generalized Anxiety Disorder	assessed three times: Baseline, Post (1 week after end of therapy) and Follow Up (6 months after end of therapy)	symptoms of generalized anxiety disorder (GAD)are assessed using the GAD-7
change in severity of the anxiety disorder	assessed five times: Baseline, therapy session 4 (week 2 of therapy), therapy session 11 (week 5 to week 9 of therapy), Post (1 week after end of therapy) and Follow Up (6 months after end of therapy)	Severity of the anxiety disorder is assessed by the clinician-rated Clinical Global Impression Scale (CGI). It is anchored for anxiety disorders.
change in Specific Phobia symptoms	assessed three times: Baseline, Post (1 week after end of therapy) and Follow Up (6 months after end of therapy)	symptoms of specific phobia are assessed using an adapted version of the DSM-5 dimensional scale for specific phobias
change in disability	assessed three times: Baseline, Post (1 week after end of therapy) and Follow Up (6 months after end of therapy)	Disability is assessed using the 12-item version of the World Health Organization Disability Schedule (WHODAS 2.0)
change in quality of life	assessed three times: Baseline, Post (1 week after end of therapy) and Follow Up (6 months after end of therapy)	Quality of life is assessed using the EuroQol five-dimensional measure for quality of life (EQ5D)
change in psychopathological symptoms	assessed seven times: Baseline, therapy sessions 2 (week 1 of therapy), 4 (week 2), 7 (week 3 to 5), 10 (week 4 to 8), 11 (week 5 to 9), 12 (week 6 to 10) Post (1 week after end of therapy) and Follow Up (6 months after end of therapy)	psychopathological symptoms are assessed using the Brief Symptom Inventory (BSI), a short form of the Symptom Checklist 90 (SCL-90). At Baseline, Post and Follow Up, the 53 item Version is used, during therapy the 18 item version is used
change in agoraphobic cognitions	assessed three times: Baseline, Post (1 week after end of therapy) and Follow Up (6 months after end of therapy)	agoraphobic cognitions are assessed using the Agoraphobic Cognitions Questionnaire (ACQ)
fear of body sensations	assessed three times: Baseline, Post (1 week after end of therapy) and Follow Up (6 months after end of therapy)	fear of body sensations is assessed using the Body Sensations Questionnaire (BSQ)
change in social anxiety	assessed three times: Baseline, Post (1 week after end of therapy) and Follow Up (6 months after end of therapy)	social anxiety is assessed using the Liebowitz Social Anxiety Scale (LSAS)

Countries

Germany

Outcome results

None listed

Source: ClinicalTrials.gov · Data processed: Feb 4, 2026