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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT00902174
Other study ID # CQTI571A2301
Secondary ID
Status Completed
Phase Phase 3
First received May 13, 2009
Last updated February 16, 2016
Start date September 2009
Est. completion date May 2011

Study information

Verified date June 2013
Source Novartis
Contact n/a
Is FDA regulated No
Health authority United States: Food and Drug AdministrationAustria: Federal Office for Safety in Health CareBelgium: Federal Agency for Medicinal Products and Health ProductsFrance: Afssaps - Agence française de sécurité sanitaire des produits de santé (Saint-Denis)Germany: Federal Institute for Drugs and Medical DevicesItaly: The Italian Medicines AgencyNetherlands: The Central Committee on Research Involving Human Subjects (CCMO)Spain: Spanish Agency of MedicinesSweden: Medical Products AgencyUnited Kingdom: Medicines and Healthcare Products Regulatory AgencySwitzerland: SwissmedicKorea: Food and Drug AdministrationJapan: Pharmaceuticals and Medical Devices AgencyCanada: Health Canada
Study type Interventional

Clinical Trial Summary

A multinational, multicenter, double blind, placebo-controlled study evaluating the efficacy and safety of imatinib as an add-on therapy in the treatment of patients with severe pulmonary arterial hypertension (PAH).


Recruitment information / eligibility

Status Completed
Enrollment 202
Est. completion date May 2011
Est. primary completion date May 2011
Accepts healthy volunteers No
Gender Both
Age group 18 Years and older
Eligibility Key Inclusion criteria

- Male or female patients =18 years of age with a current diagnosis of pulmonary arterial hypertension (PAH) according to the Dana Point 2008 Meeting: World Health Organization (WHO) Diagnostic Group I, idiopathic or heritable (familial or sporadic) PAH, PAH associated with collagen vascular disease including systemic sclerosis, rheumatoid arthritis, mixed connective tissue diseases, and overlap syndrome. PAH following one year repair of congenital heart defect [Atrial Septal Defect (ASD), Ventricular Septal Defect (VSD) or Posterior Descending Artery (PDA)], or PAH associated with diet therapies or other drugs

- A Pulmonary Vascular Resistance (PVR) = 800 dynes.sec.cm-5 (as assessed by Right Heart Catheterization (RHC) at screening or in the 3 months preceding the screening visit) despite treatment with two or more specific PAH therapies, including Endothelin Receptor Antagonists (ERAs), phosphodiesterase 5 inhibitors (PDE5), or subcutaneous, inhaled, intravenous or oral prostacyclin analogues for = 3 months. Background therapy doses were to be stable for = 30 days except for warfarin and prostacyclin analogues ( = 30 days but doses could vary even within the month before enrollment).

- World Health Organization functional Class II-IV. For WHO Functional Class IV, one of the 2 or more specific PAH therapies were to be an inhaled, subcutaneous, intravenous or oral prostacyclin analogue, unless the subject showed intolerance of prostacyclin analogues.

- 6MWD = 150 meters and = 450 meters at screening. Distances of two consecutive 6MWTs were to be within 15% of one another.

Key Exclusion criteria

- With a pulmonary capillary wedge pressure > 15 mm Hg to rule out PAH secondary to left ventricular dysfunction.

- With a diagnosis of pulmonary artery or vein stenosis

- Left ventricular ejection fraction (LVEF) < 45%

- With Disseminated Intravascular Coagulation (DIC)

- With evidence of major bleeding or intracranial hemorrhage

- With a history of elevated intracranial pressure

- With a history of latent bleeding risk such as diabetic retinopathy, gastrointestinal bleeding due to gastric or duodenal ulcers, or colitis ulcerosa

- With a QTcF > 450 msec for males and > 470 msec for females at screening and baseline in the absence of right bundle branch block.

- With a history of ventricular tachycardia, ventricular fibrillation or ventricular flutter

- With a history of Torsades de Pointes

- With a history of long QT syndrome

- Having undergone atrial septostomy in the 3 months prior to the screening visit

Study Design

Allocation: Randomized, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment


Related Conditions & MeSH terms


Intervention

Drug:
imatinib mesylate
Two or 4 imatinib mesylate (QTI571) 100 mg film coated tablets once daily.
Placebo
Placebo to imatinib 100 mg film coated tablets

Locations

Country Name City State
Austria Novartis investigative site Innsbruck
Austria Novartis Investigative Site Vienna
Belgium Novartis Investigative Site Bruxelles
Belgium Novartis Investigative Site Leuven
Canada Novartis Investigative Site Calgary
Canada Novartis Investigative Site Edmonton
Canada Novartis Investigative Site London
Canada Novartis Investigative Site Montreal
Canada Novartis Investigative Site Ottawa
Canada Novartis investigative site Toronto
Canada Novartis Investigative Site Vancouver
France Novartis Investigative Site Clamart Cedex
Germany Novartis Investigative Site Berlin
Germany Novartis Investigative Site Dresden
Germany Novartis Investigative Site Giessen
Germany Novartis Investigative Site Greifswald
Germany Novartis Investigative Site Hamburg
Germany Novartis Investigative Site Hannover
Germany Novartis Investigative Site Heidelberg
Germany Novartis Investigative Site Homburg
Germany Novartis Investigative Site Koln
Germany Novartis investigative site Lowenstein
Germany Novartis Investigative Site Munchen
Germany Novartis Investigative Site Regensberg
Germany Novartis Investigative Site Wurzberg
Italy Novartis Investigative Site Bologna
Italy Novartis Investigative Site Pavia
Italy Novartis Investigative Site Pisa
Italy Novartis Investigative Site Roma
Japan Novartis Investigative Site Bunkyo-ku
Japan Novartis Investigative Site Hamamatsu
Japan Novartis Investigative Site Mitaka
Japan Novartis Investigative Site Okayama
Japan Novartis Investigative Site Sendai
Japan Novartis Investigative Site Suita
Korea, Republic of Novartis Investigative Site Seoul
Netherlands Novartis Investigative Site Amsterdam
Spain Novartis Investigative Site Barcelona
Spain Novartis Investigative Site Caceras
Spain Novartis Investigative Site La Coruna
Spain Novartis investigative site La Laguna
Spain Novartis Investigative Site Las Palmas de Gran Canarias
Spain Novartis Investigative Site Madrid
Spain Novartis Investigative Site Malaga
Spain Novartis Investigative Site Santa Cruz de Tenerife
Spain Novartis Investigative Site Santander
Spain Novartis Investigative Site Sevilla
Spain Novartis investigative site Valencia
Spain Novartis Investigative Site Valladolid
Sweden Novartis Investigative Site Lund
Sweden Novartis Investigative Site Stockholm
Sweden Novartis Investigative Site Umea
Sweden Novartis Investigative Site Uppsala
Switzerland University Hospital Basel Basel
Switzerland Novartis Investigative Site Bern
Switzerland Novartis Investigative Site Lausanne
Switzerland Novartis Investigative Site St. Gallen
United Kingdom Novartis Investigative Site Cambridge
United Kingdom Novartis Investigative Site Clydebank
United Kingdom Novartis Investigative Site London
United Kingdom Novartis Investigative Site Newcastle Upon Tyne
United Kingdom Novartis Investigative Site Sheffield
United States Novartis Investigative Site Atlanta Georgia
United States Novartis Investigative Site Aurora Colorado
United States Novartis Investigative Site Baltimore Maryland
United States Novartis Investigative Site Birmingham Alabama
United States Novartis Investigative Site Boston Massachusetts
United States Novartis Investigative Site Boston Massachusetts
United States Novartis Investigative Site Boston Massachusetts
United States Novartis Investigative Site Chicago Illinois
United States Novartis Investigative Site Cincinnati Ohio
United States Novartis Investigative Site Clearwater Florida
United States Novartis Investigative Site Cleveland Ohio
United States Novartis Investigative Site Cleveland Ohio
United States Novartis Investigative Site Dallas Texas
United States Novartis Investigative Site Durham North Carolina
United States Novartis Investigative Site Houston Texas
United States Novartis Investigative Site Knoxville Tennessee
United States Novartis Investigative Site Los Angeles California
United States Novartis Investigative Site Miami Beach Florida
United States Novartis Investigative Site Milwaukee Wisconsin
United States Novartis Investigative Site Minneola New York
United States Novartis Investigative Site New York New York
United States Novartis Investigative Site New York New York
United States Novartis Investigative Site Oklahoma City Oklahoma
United States Novartis Investigative Site Omaha Nebraska
United States Novartis Investigative Site Philadelphia Pennsylvania
United States Novartis Investigative Site Phoenix Arizona
United States Novartis Investigative Site Pittsburgh Pennsylvania
United States Novartis Investigative Site Pittsburgh Pennsylvania
United States Novartis Investigative Site Portland Oregon
United States Novartis Investigative Site Rochester Minnesota
United States Novartis Investigative Site San Francisco California
United States Novartis Investigative Site St. Louis Missouri
United States Novartis Investigative Site Weston Florida

Sponsors (1)

Lead Sponsor Collaborator
Novartis Pharmaceuticals

Countries where clinical trial is conducted

United States,  Austria,  Belgium,  Canada,  France,  Germany,  Italy,  Japan,  Korea, Republic of,  Netherlands,  Spain,  Sweden,  Switzerland,  United Kingdom, 

Outcome

Type Measure Description Time frame Safety issue
Primary Difference in Six-minute Walk Distance Test (6MWD) Between Imatinib and Placebo at 24 Weeks This standardized walk course was 30 meters in length. During the walk the participant was connected to a portable pulse oximeter via a finger probe. Participants were instructed to walk at a comfortable speed for as far as they could manage in 6 minutes. The total distance walked (in meters) was recorded. Results were compared between the 2 groups. 24 weeks No
Secondary Clinical Worsening Comparing Imatinib Versus Placebo for Adjudicated Cases Clinical worsening per participant was measured by the onset of any adjudicated event (all cause mortality; overnight hospitalization for worsening of Pulmonary Arterial Hypertension (PAH); worsening of WHO functional class by one level; 15% decline in Six Minute Walk Distance (6MWD) measured on two consecutive occasions) at 24 weeks treatment, comparing imatinib to placebo groups. A cox regression analysis model was used. 24 weeks No
Secondary Change From Baseline in Right Atrial Pressure Change from baseline in right atrial pressure (mmHg) was measured via right heart catheterization according to the local hospital procedures. The right atrial pressure was assessed when the participant was in a stable hemodynamic rest state. A higher right atrial pressure number indicates worsening. baseline and week 24 No
Secondary Change From Baseline in Mean Pulmonary Arterial Pressure Change from baseline in mean pulmonary arterial pressure (mmHg) was measured via right heart catheterization according to the local hospital procedures. The mean pulmonary arterial pressure was assessed when the participant was in a stable hemodynamic rest state. A higher mean pulmonary arterial pressure number indicates worsening. baseline and week 24 No
Secondary Change From Baseline in Mean Pulmonary Capillary Wedge Pressure Change from baseline in mean pulmonary capillary wedge pressure (mmHg)was measured via right heart catheterization according to the local hospital procedures. The right atrial mean pulmonary capillary wedge pressure was assessed when the participant was in a stable hemodynamic rest state. baseline and week 24 No
Secondary Change From Baseline in Systemic Vascular Resistance Change from baseline in systemic vascular resistance (dynes*sec*cm^-5) was measured via right heart catheterization according to the local hospital procedures. The systemic vascular resistance was assessed when the participant was in a stable hemodynamic rest state. Reduction from baseline in mean systemic vascular resistance indicates improvement. baseline and week 24 No
Secondary Change From Baseline in Pulmonary Vascular Resistance Change from baseline in pulmonary vascular resistance (dynes*sec*cm^-5) was measured via right heart catheterization according to the local hospital procedures. The pulmonary vascular resistance was assessed when the participant was in a stable hemodynamic rest state. Reduction from baseline in pulmonary vascular resistance indicates improvement. baseline and week 24 No
Secondary Change From Baseline in Pulmonary Resistance Index Change from baseline in pulmonary resistance index (dynes*sec*cm^-5/m2) was measured via right heart catheterization according to the local hospital procedures. The pulmonary resistance index was assessed when the participant was in a stable hemodynamic rest state. A reduction from baseline in pulmonary resistance index indicates improvement. baseline and week 24 No
Secondary Change From Baseline in Cardiac Output Change from baseline in cardiac output (L/min) was measured via right heart catheterization according to the local hospital procedures. The cardiac output was assessed when the participant was in a stable hemodynamic rest state. An increase from baseline (higher number) in cardiac output indicates improvement. 24 weeks No
Secondary Change From Baseline in Systolic Arterial Blood Pressure Change from baseline in systolic arterial blood pressure (mmHg) was measured via right heart catheterization according to the local hospital procedures. The systolic arterial blood was assessed when the participant was in a stable hemodynamic rest state. baseline and week 24 No
Secondary Change From Baseline in Diastolic Arterial Blood Pressure Change from baseline in diastolic arterial blood pressure (mmHg) was measured via right heart catheterization according to the local hospital procedures. The diastolic arterial blood pressure was assessed when the participant was in a stable hemodynamic rest state. baseline and week 24 No
Secondary Change From Baseline in Heart Rate Change from baseline in heart rate (bpm) was measured via right heart catheterization according to the local hospital procedures. The heart rate was assessed when the participant was in a stable hemodynamic rest state. 24 weeks No
Secondary Change in Borg Dyspnea Score During 6-minute Walk Test Change in Borg scale was measured at different time points at week 24. The Borg Scale consists of scale range of 0 to 10. Participants pointed to indicate their level of dyspnea before and at the end of exercise testing (where 0 indicates no breathlessness at all and 10 indicates maximum breathlessness). A reduction in this score indicates an improvement. week 24 No
Secondary Covariance of End of Study CAMPHOR Score The CAMPHOR test consists of 65 items and 3 scales. Two scales measure Health Related Quality of Life. 1) Symptoms: consists of 25 items measuring loss or abnormality of psychological, physiological or anatomical structure or function; further sub-divided into 3 subscales (energy, breathlessness and mood), 2) Disability: consists of 15 items measuring any restriction or lack of ability to perform an activity. 3) Quality of Life (QOL): consists of 25 items defining how individuals perceived ability and capacity to satisfy their needs. The 25-item symptom and QOL scales score from 0-25 where a higher score indicates the presence of more symptoms and poor QOL, respectively. The 15-item functioning scale scores 0-30; a higher score indicates poor functioning. Week 24 No
Secondary Plasma Concentration of QTI571 200 mg and Its Metabolite (GCP74588) Pre-dose and Between 0 Hour to 3 Hour Post-dose Per Participant Blood samples were taken from each subject participating in the study (placebo group and active treatment group) once predose and once between 0 hour to 3 hour post dose at day 1 (baseline), day 14, day 28 and day 168.
The parent compound QTI571 and its active metabolite, GCP74588, were measured in plasma by validated liquid chromatography-mass spectrometry (HPLC-MS/MS) assay.
predose and between 0 hour to 3 hour post dose at day 1, day 14, day 28 and day 168 No
Secondary Plasma Concentration of QTI571 400 mg and Its Metabolite (GCP74588) Pre-dose and Between 0 Hour to 3 Hour Post-dose Per Participant Blood samples were taken from each subject participating in the study (placebo group and active treatment group) once predose and once between 0 hour to 3 hour post dose at day 1 (baseline), day 14, day 28 and day 168.
The parent compound QTI571 and its active metabolite, GCP74588, were measured in plasma by validated liquid chromatography-mass spectrometry (HPLC-MS/MS) assay.
predose and between 0 hour to 3 hour post dose at day 1, day 14, day 28 and day 168 No
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