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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT00600756
Other study ID # D1443L00039
Secondary ID
Status Completed
Phase Phase 3
First received January 9, 2008
Last updated October 2, 2012
Start date January 2008
Est. completion date October 2009

Study information

Verified date October 2012
Source AstraZeneca
Contact n/a
Is FDA regulated No
Health authority Belgium: The Federal Public Service (FPS) Health, Food Chain Safety and EnvironmentBrazil: Ministry of HealthBulgaria: Ministry of HealthCosta Rica: Ministry of Health Costa RicaDenmark: Ministry of HealthFinland: Ministry of Social Affairs and HealthGermany: Federal Institute for Drugs and Medical DevicesItaly: National Institute of HealthMexico: National Institute of Public Health, Health SecretariatPortugal: National Pharmacy and Medicines InstituteRomania: Ministry of Public HealthRussia: Ministry of Health of the Russian FederationSpain: Ministry of Health and ConsumptionSwitzerland: Federal Office of Public HealthTurkey: Ministry of Health
Study type Interventional

Clinical Trial Summary

The trial is designed to assess the long term subjective well-being in schizophrenic outpatients treated with quetiapine XR (extended release) or oral risperidone at flexible dose in a naturalistic setting over a period of one year. Secondary outcome measures have been selected for helping in the differentiation of the compared atypical antipsychotics. The primary objective of this study is to demonstrate the non-inferiority of quetiapine XR to risperidone assessed at month 6 in terms of responder rate using the self-report instrument SWN-K


Recruitment information / eligibility

Status Completed
Enrollment 798
Est. completion date October 2009
Est. primary completion date October 2009
Accepts healthy volunteers No
Gender Both
Age group 18 Years to 65 Years
Eligibility Inclusion Criteria:

- Treated for symptomatic schizophrenia (DSM-IV-TR codes: 295.10, 295.20, 295.30,295.60, 295.90) or schizoaffective disorder (DSM-IV-TR code:295.70) or schizophreniform disorder (DSM-IV-TR code: 295.40). Patients with co-morbid depressive symptoms may be enrolled

- Patient with first episode of the above mentioned disease (item 3) or patient requiring a medication change for clinical reasons (effectiveness, tolerability, compliance, patient preference), i.e. switch from typical to atypical neuroleptics, switch from other atypical neuroleptics, excluding patients treated with risperidone or quetiapine at the time of enrolment.

Exclusion Criteria:

- Patients with a baseline SWN-K total score of >75

- Patients with previous treatment with risperidone or quetiapine may be enrolled if change of treatment has not been dictated by major lack of tolerability and efficacy and if date of last dose has been at least 3 months prior to enrolment.

Study Design

Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment


Related Conditions & MeSH terms


Intervention

Drug:
Quetiapine XR
Oral, once daily, tablets of 400 mg to 800 mg
Risperidone
Oral, once daily, tablets of 2 mg to 6 mg

Locations

Country Name City State
Belgium Research Site Assebroek
Belgium Research Site Hasselt
Belgium Research Site Liege
Belgium Research Site Montignies-sur-sambre
Belgium Research Site Roeselare
Belgium Research Site Sint-denijs-westrem
Belgium Research Site Tournai
Brazil Research Site Aparecida de Goiania GO
Brazil Research Site Belo Horizonte Minas Gerais
Brazil Research Site Botucatu
Brazil Research Site Curitiba PR
Brazil Research Site Fortaleza CE
Brazil Research Site Itapira SP
Brazil Research Site Porto Alegre RS
Brazil Research Site Recife PE
Brazil Research Site Ribeirao Preto SP
Brazil Research Site Rio de Janeiro
Brazil Research Site Salvador BA
Brazil Research Site Sao Paulo SP
Brazil Research Site Sorocaba SP
Bulgaria Research Site Cerova Koria Village Veliko Tarnovo
Bulgaria Research Site Pazardjik
Bulgaria Research Site Pleven
Bulgaria Research Site Plovdiv
Bulgaria Research Site Sofia
Bulgaria Research Site Stara Zagora
Bulgaria Research Site Varna
Costa Rica Research Site Barrio Los Yoses San Jose
Costa Rica Research Site Curridabat San Jose
Costa Rica Research Site Guadalupe San Jose
Finland Research Site Helsinki
Finland Research Site Kitee
Finland Research Site Kuopio
Finland Research Site Lapua
Finland Research Site Pori
Finland Research Site Raahe
Finland Research Site Rovaniemi
Finland Research Site Tampere
Finland Research Site Turku
Germany Research Site Bad Saarow
Germany Research Site Berlin
Germany Research Site Bielefeld
Germany Research Site Bochum
Germany Research Site Butzbach
Germany Research Site Darmstadt
Germany Research Site Duisburg
Germany Research Site Gelsenkirchen
Germany Research Site Grevenbroich
Germany Research Site Hamburg
Germany Research Site Hattingen
Germany Research Site Hildesheim
Germany Research Site Koln
Germany Research Site Konigsbruck
Germany Research Site Mittweida
Germany Research Site Munchen
Germany Research Site Oranienburg
Germany Research Site Siegen
Germany Research Site Stralsund
Germany Research Site Wismar
Italy Research Site Ancona
Italy Research Site Andria BA
Italy Research Site Chioggia VE
Italy Research Site Feltre BL
Italy Research Site Fidenza PR
Italy Research Site Genova GE
Italy Research Site Maddaloni CE
Italy Research Site Milano MI
Italy Research Site Palmi RC
Italy Research Site Parma PR
Italy Research Site Perugia PG
Italy Research Site Pompei
Italy Research Site Rimini RN
Italy Research Site Salerno SA
Italy Research Site Sassari SS
Italy Research Site Sora FR
Mexico Research Site Guadalajara Jalisco
Mexico Research Site Mexico
Mexico Research Site Mexico D.f.
Mexico Research Site Mexico D.F
Mexico Research Site Monterrey, Nuevo Leon
Mexico Research Site SLP
Mexico Research Site Yucatan
Portugal Research Site Abraveses
Portugal Research Site Braga
Portugal Research Site Coimbra
Portugal Research Site Lisboa
Portugal Research Site Porto
Portugal Research Site Santarem
Romania Research Site Bucharest
Romania Research Site Craiova
Romania Research Site Galati
Romania Research Site Pitesti Arges
Romania Research Site Sibiu
Russian Federation Research Site Kazan
Russian Federation Research Site Moscow
Russian Federation Research Site Moscow Russia
Russian Federation Research Site St. Petersburg
Spain Research Site Elche (alicante) Comunidad Valenciana
Spain Research Site Jaen Andalucia
Spain Research Site Madrid Comunidad de Madrid
Spain Research Site Malaga Andalucia
Spain Research Site Mataro (barcelona) Cataluna
Spain Research Site Salamanca Castilla Leon
Spain Research Site Sama de Langreo Asturias
Spain Research Site San Juan de Alicante Comunidad Valenciana
Spain Research Site Sevilla Andalucia
Spain Research Site Vigo Galicia
Spain Research Site Zamora Castilla Leon
Spain Research Site Zamudio (vizcaya) Pais Vasco
Switzerland Research Site Prilly Waadt
Switzerland Research Site WIL
Turkey Research Site Ankara
Turkey Research Site Elazig
Turkey Research Site Istanbul
Turkey Research Site Izmir
Turkey Research Site Manisa

Sponsors (1)

Lead Sponsor Collaborator
AstraZeneca

Countries where clinical trial is conducted

Belgium,  Brazil,  Bulgaria,  Costa Rica,  Finland,  Germany,  Italy,  Mexico,  Portugal,  Romania,  Russian Federation,  Spain,  Switzerland,  Turkey, 

Outcome

Type Measure Description Time frame Safety issue
Primary Responder Rate at Month 6 in the Per Protocol Population Using the Subjective Well-being Under Neuroleptics Scale, Short Version (SWN-K) Total Score The SWN-K is comprised of 20 questions, rated on a 6-point scale from 1 (not at all) to 6 (very much). Scores range from 20 to 120, with higher scores implying higher subjective well-being. A responder is defined as a subject with an increase of 10 points or 20% from baseline in SWN-K total score (non-inferiority limit of -9.7% in responder rate) 6 months No
Secondary Change From Baseline in Mean Subjective Well-Being Under Neuroleptic Treatment Scale (SWN-K) Total Score at Month 12 in the Per Protocol Population The SWN-K is comprised of 20 questions, each of which is rated using a 6-point scale ranging from 1 (not at all) to 6 (very much). Possible scores range from 20 to 120, with higher scores implying higher subjective well-being. Baseline and Month 12 No
Secondary Change From Baseline in Mean Subjective Well-Being Under Neuroleptic Treatment Scale (SWN-K) Total Score at Month 12 in the Intent-to-Treat (ITT) Population The SWN-K is comprised of 20 questions, each of which is rated using a 6-point scale ranging from 1 (not at all) to 6 (very much). Possible scores range from 20 to 120, with higher scores implying higher subjective well-being. Baseline and Month 12 No
Secondary Change From Baseline in the Subjective Well-Being Under Neuroleptic Treatment Scale (SWN-K) Subscale Score: Physical Functioning at Month 12 in the ITT Population. The SWN-K total score is the sum of 5 subscores (4 questions each): physical functioning, social integration, mental functioning, self-control, and emotional regulation. The subscores are rated using a 6-point scale (the higher the grade, the better the response). Possible subscores range from 4 to 24. Baseline and 12 months No
Secondary Change From Baseline in the Subjective Well-Being Under Neuroleptic Treatment Scale (SWN-K) Subscale Score: Social Integration at Month 12 in the ITT Population. The SWN-K total score is the sum of 5 subscores (4 questions each): physical functioning, social integration, mental functioning, self-control, and emotional regulation. The subscores are rated using a 6-point scale (the higher the grade, the better the response). Possible subscores range from 4 to 24. Baseline and 12 months No
Secondary Change From Baseline in the Subjective Well-Being Under Neuroleptic Treatment Scale (SWN-K) Subscale Score: Mental Functioning at Month 12 in the ITT Population. The SWN-K total score is the sum of 5 subscores (4 questions each): physical functioning, social integration, mental functioning, self-control, and emotional regulation. The subscores are rated using a 6-point scale (the higher the grade, the better the response). Possible subscores range from 4 to 24. Baseline and 12 months No
Secondary Change From Baseline in the Subjective Well-Being Under Neuroleptic Treatment Scale (SWN-K) Subscale Score: Self-control at Month 12 in the ITT Population. The SWN-K total score is the sum of 5 subscores (4 questions each): physical functioning, social integration, mental functioning, self-control, and emotional regulation. The subscores are rated using a 6-point scale (the higher the grade, the better the response). Possible subscores range from 4 to 24. Baseline and 12 months No
Secondary Change From Baseline in the Subjective Well-Being Under Neuroleptic Treatment Scale (SWN-K) Subscale Score: Emotional Regulation at Month 12 in the ITT Population. The SWN-K total score is the sum of 5 subscores (4 questions each): physical functioning, social integration, mental functioning, self-control, and emotional regulation. The subscores are rated using a 6-point scale (the higher the grade, the better the response). Possible subscores range from 4 to 24. Baseline and 12 months No
Secondary The Remission Rate in Both the Quetiapine XR Group and the Risperidone Group at Month 12 in the ITT Population Remission was defined as a SWN-K total score greater than or equal to 80. The reported population is participants who showed remission over, time from baseline to Month 12 12 months No
Secondary The Effect of Quetiapine XR Versus Risperidone at Month 12 in the ITT Population on Core Schizophrenic and Depressive Symptoms by Evaluating the Change From Baseline in CGI-SCH Overall Severity Score (Improved). For the CGI-SCH overall severity of illness, the score ranged from 1 (normal, not ill) to 7 (among the most severely ill). CGI-SCH score was divided into 3 classes: worsening (change score>0), stable (change score=0) and improved (change score<0). Change from baseline in CGI-SCH overall severity of illness in number of participants with CGI-SCH overall severity score improvement. 12 months No
Secondary The Effect of Quetiapine XR Versus Risperidone at Month 12 in the ITT Population on Core Schizophrenic and Depressive Symptoms by Evaluating the Change From Baseline in CGI-SCH Overall Severity Score For the CGI-SCH (Clinical Global Impression-Schizophrenia severity of illness scale) overall severity of illness, the score ranged from 1 (normal, not ill) to 7 (among the most severely ill). Change from baseline in CGI-SCH score was divided into 3 classes: worsening (change score>0), stable (change score=0) and improved (change score<0). 12 months No
Secondary The Effect of Quetiapine XR Versus Risperidone at Month 12 in the ITT Population on Core Schizophrenic and Depressive Symptoms by Evaluating the Change From Baseline in the Calgary Depression Scale for Schizophrenia (CDSS) Total Score The CDSS total score is the sum of 9 questions and ranges from 0 to 27. The higher the score, the more severe are the symptoms. 12 months No
Secondary The Effect of Quetiapine XR Versus Risperidone by Evaluating the Relapse Rate at Month 12 in the ITT Population Relapse is defined as at least one increase of greater than or equal to 2 points on the CGI-SCH overall severity score during the treatment period or at least one hospitalization due to psychiatric disorders during the treatment period. 12 months No
Secondary Evaluation of Effect of Quetiapine XR Versus Risperidone on the Health-related Quality of Life of Patients With Schizophrenia by Evaluating the Change From Baseline in EQ-5D(Euro Quality of Life-5 Dimension) Index Score at Month 12 in the ITT Population. The Euro Quality of Life - 5 dimension index (EQ-5D) is the result of the application of a formula that essentially attaches values (also called weights) to each of the levels (no, some, or heavy problems) in each dimension (mobility, self-care, usual activities, pain/discomfort, anxiety/depression). These weights are issued from a representative sample of the general population. The total possible maximum value was 1 (healthy life) and the minimum value was 0 (death). 12 months No
Secondary To Evaluate the Effect of Quetiapine XR Versus Risperidone at Month 12 in the ITT Population Regarding Health Economics Outcomes by Evaluating the Functional Improvement Rate of the Modified Vocational Status Index/ Location Code Index: Stable State Stable State was defined as having the same status in occupational and residential status as at Baseline. 12 months No
Secondary The Effect of Quetiapine XR Versus Risperidone Regarding Health Economics Outcomes by Evaluating the Mean Number of Lost School/Work Days at Month 12 in the ITT Population Workers and students are defined from the modified vocational status index excluding subjects "Retired" or "Unemployed, whether or not expected to work". 12 months No
Secondary The Effect of Quetiapine XR Versus Risperidone Regarding Health Economics Outcomes by Evaluating the Participants With at Least 1 Hospitalization Due to Psychiatric Disorders at Month 12 in the ITT Population All hospitalizations due to psychiatric disorders during the study (i.e. from Visit 1 to Termination date + 30 days) in inpatients units, in emergency wards, and in day clinics. 12 months No
Secondary Number of Subjects Who Had an Unscheduled Visits Due to Worsening of Schizophrenia, Dose Change, or Adverse Event at Month 12 in the ITT Population Unscheduled visits due to worsening of schizophrenia, dose change or adverse event including the hospitalizations due to psychiatric disorders during the study (i.e. from Visit 1 to Termination date + 30 days) in inpatients units, in emergency wards and in day clinics. Month 12 No
Secondary The Effect of Quetiapine XR Versus Risperidone Regarding Health Economics Outcomes by Evaluating the Time Between First Study Drug Intake and First Hospitalization for Patients With 1 Hospitalization in the ITT Population 12 months No
Secondary Number of Participants Using Antidepressants at Month 12 in the ITT Population The number of participants who were taking at least 1 antidepressant at Month 12. Antidepressants are all concomitant medications classified in the Anatomical Therapeutic Chemical(ATC)Subgroup "N06-Antidepressants". 12 months No
Secondary The Effect of Quetiapine XR Versus Risperidone Regarding Health Economics Outcomes by Evaluating the Number of Participants Using Other Psychotropic Medications at Month 12 in the ITT Population Other psychotropic medications include antiepileptics, anti-parkinson drugs, antipsychotics, and antidepressants. 12 months No
Secondary The Compliance of Patients Taking Quetiapine XR Versus Risperidone at Month 12 by Evaluating the Number of Participants Who Returned Study Drug at Month 12 in the ITT Population 12 months No
Secondary The Safety and Tolerability of Quetiapine XR Versus Risperidone by Evaluating the Number of Participants With a Treatment-emergent Adverse Event (TEAEs) at Month 12 in the Safety Population Treatment-emergent adverse events are defined as adverse events that occurred after the first intake of the study medication (or on the same day). 12 months No
Secondary The Safety and Tolerability of Quetiapine XR Versus Risperidone by Evaluating the Number of Participants Who Discontinued the Study Because of an TEAE at Month 12 in the Safety Population Treatment-emergent adverse events are defined as adverse events that occurred after the first intake of the study medication (or on the same day). 12 months No
Secondary The Safety and Tolerability of Quetiapine XR Versus Risperidone by Evaluating the Number of Participants Who Had at Least 1 Extra-pyramidal TEAE at Month 12 in the Safety Population Treatment-emergent adverse events are defined as adverse events that occurred after the first intake of the study medication (or on the same day). 12 months No
Secondary The Safety and Tolerability of Quetiapine XR Versus Risperidone by Evaluating the Number of Extra-pyramidal Events at Month 12 in the Safety Population Extra-pyramidal events include tremor, hypokinesia, muscle rigidity, hyperkinesia, and extrapyramidal disorder. 12 months No
Secondary The Safety and Tolerability of Quetiapine XR Versus Risperidone by Evaluating the Number of Participants Who Had at Least 1 Cardiac TEAE at Month 12 in the Safety Population Treatment-emergent adverse events are defined as adverse events that occurred after the first intake of the study medication (or on the same day). 12 months No
Secondary The Safety and Tolerability of Quetiapine XR Versus Risperidone by Evaluating the Mean Change From Baseline to Month 12 in Prolactin Levels in the Safety Population The normal range for men is 0 to 14, and for women is 0 to 24. 12 months No
Secondary The Safety and Tolerability of Quetiapine XR vs Risperidone by Evaluating the Number of Participants at Month 12 in Safety Population With Individual Symptoms Assessed by the Modified Udvalg for Kliniske Undersogelser, Side Effect Rating Scale: Neurologic Symptoms are graded according to degree (not present to severe) and causal relationship (improbable, possible, probable). An individual AE is defined as an AE with a worse degree compared with Baseline and with a possible or probable relationship to study drug. 12 months No
Secondary The Safety and Tolerability of Quetiapine XR Versus Risperidone by Evaluating the Number of Participants at Month 12 in the Safety Population With Individual Symptoms Assessed by the Modified UKU: Hyperprolactinaemia in Women Symptoms are graded according to degree (not present to severe) and causal relationship (improbable, possible, probable). Hyperprolactinaemia in women is defined as number of women who show the individual adverse event (AE) hyperprolactinaemia. An individual AE Hyperprolactinaemia is defined as an AE with a worse degree of hyperprolactinaemia compared with baseline and with a possible or probable relationship to study drug. Month 12 No
Secondary The Safety and Tolerability of Quetiapine XR Versus Risperidone by Evaluating the Number of Participants at Month 12 in the Safety Population With Individual Symptoms Assessed by the Modified UKU: Sexual Dysfunction in Men Symptoms are graded according to degree (not present to severe) and causal relationship (improbable, possible, probable). Sexual dysfunction in men is defined as number of men who show the individual adverse event (AE) sexual dysfunction. An individual AE sexual dysfunction is defined as an AE with a worse degree of sexual dysfunction compared with baseline and with a possible or probable relationship to study drug. Month 12 No
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