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NCT03196297 Clinical Trial

A Trial Evaluating Efficacy and Safety of Prophylactic Administration of Concizumab in Patients With Severe Haemophilia A Without Inhibitors

Haemophilia A Clinical Trial

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Official title:
A Multi-Centre Trial Evaluating Efficacy and Safety of Prophylactic Administration of Concizumab in Patients With Severe Haemophilia A Without Inhibitors

Clinical Trial Details — Status: Completed

Administrative data
NCT number NCT03196297
Other study ID # NN7415-4255
Secondary ID U1111-1179-38722
Status Completed
Phase Phase 2
First received
Last updated
Start date August 16, 2017
Est. completion date June 3, 2020

Study information
Verified date November 2021
Source Novo Nordisk A/S
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

This trial is conducted in Asia, Europe and the United States of America (USA). The aim of the trial is to assess the efficacy of concizumab administered s.c. (subcutaneously, under the skin) once daily in preventing bleeding episodes in patients with severe haemophilia A without inhibitors.

Recruitment information / eligibility
Status Completed
Enrollment 36
Est. completion date June 3, 2020
Est. primary completion date June 22, 2018
Accepts healthy volunteers No
Gender Male
Age group 18 Years and older
Eligibility Inclusion Criteria: - Informed consent obtained before any trial-related activities. Trial-related activities are any procedures that are carried out as part of the trial, including activities to determine the suitability for the trial - Male patients aged 18 years or older at the time of signing informed consent, diagnosed with severe haemophilia A (FVIII activity below 1%), based on medical records or results at screening Exclusion Criteria: - Known or suspected hypersensitivity to trial product(s) or related products - Known inherited or acquired bleeding disorder other than haemophilia A - Presence of inhibitors (neutralising antibodies) to Factor VIII (equal to or above 0.6 Bethesda Units) at screening measured by the Nijmegen method

Study Design

Related Conditions & MeSH terms

Intervention

Drug:
Concizumab
0.15 mg/kg (with potential stepwise dose administration to 0.25 mg/kg) administered daily s.c (subcutaneously, under the skin). Treatment duration is 24 weeks in the main phase, and 52 weeks in the extension phase
Turoctocog alfa
Breakthrough bleeding episodes will be treated by the patients at home with turoctocog alfa at the discretion of the study doctor, who will also choose dose levels

Locations
Country Name City State
France Novo Nordisk Investigational Site Brest
France Novo Nordisk Investigational Site Caen
France Novo Nordisk Investigational Site Nantes Cedex 1
Germany Novo Nordisk Investigational Site Bonn
Germany Novo Nordisk Investigational Site Homburg
Italy Novo Nordisk Investigational Site Milano
Italy Novo Nordisk Investigational Site Rome
Japan Novo Nordisk Investigational Site Aichi
Japan Novo Nordisk Investigational Site Nara
Japan Novo Nordisk Investigational Site Tokyo
Japan Novo Nordisk Investigational Site Tokyo
Spain Novo Nordisk Investigational Site Madrid
Spain Novo Nordisk Investigational Site Málaga
Spain Novo Nordisk Investigational Site Valencia
Sweden Novo Nordisk Investigational Site Malmö
Sweden Novo Nordisk Investigational Site Solna
Thailand Novo Nordisk Investigational Site Bangkok
Turkey Novo Nordisk Investigational Site Ankara
Turkey Novo Nordisk Investigational Site Bornova-IZMIR
Turkey Novo Nordisk Investigational Site Edirne
Turkey Novo Nordisk Investigational Site Istanbul
Ukraine Novo Nordisk Investigational Site Lviv
United Kingdom Novo Nordisk Investigational Site Belfast
United Kingdom Novo Nordisk Investigational Site Cambridge
United Kingdom Novo Nordisk Investigational Site London
United Kingdom Novo Nordisk Investigational Site London
United States Novo Nordisk Investigational Site Indianapolis Indiana
United States Novo Nordisk Investigational Site Los Angeles California
United States Novo Nordisk Investigational Site Nashville Tennessee
United States Novo Nordisk Investigational Site Oklahoma City Oklahoma
United States Novo Nordisk Investigational Site Salt Lake City Utah

Sponsors (1)
Lead Sponsor Collaborator
Novo Nordisk A/S

Countries where clinical trial is conducted

United States,  France,  Germany,  Italy,  Japan,  Spain,  Sweden,  Thailand,  Turkey,  Ukraine,  United Kingdom, 

Outcome
Type Measure Description Time frame Safety issue
Primary The Number of Bleeding Episodes During at Least 24 Weeks From Treatment Onset The number of bleeding episodes that were treated during at least 24 weeks from treatment onset are presented. The data is presented while on last dose level when the bleed occurred. During at least 24 weeks from treatment onset
Secondary The Number of Bleeding Episodes During at Least 76 Weeks From Treatment Onset The number of bleeding episodes that were treated during at least 76 weeks from treatment onset are presented. The data is presented while on last dose level when the bleed occurred. During at least 76 weeks from treatment onset
Secondary The Number of Spontaneous Bleeding Episodes During at Least 24 Weeks From Treatment Onset Bleeds that were not linked to a specific, known action or event are called spontaneous bleeding episodes. The number of spontaneous bleeding episodes that were treated during at least 24 weeks from treatment onset are presented. The data is presented while on last dose level when the bleed occurred. During at least 24 weeks from treatment onset
Secondary The Number of Spontaneous Bleeding Episodes During at Least 76 Weeks From Treatment Onset Bleeds that were not linked to a specific, known action or event are called spontaneous bleeding episodes. The number of spontaneous bleeding episodes that were treated during at least 76 weeks from treatment onset are presented. The data is presented while on last dose level when the bleed occurred. During at least 76 weeks from treatment onset
Secondary Number of Treatment-emergent Adverse Events (TEAEs) During at Least 24 Weeks From Treatment Onset An adverse event (AE) was any untoward medical occurrence in a participant administered a medicinal product, and which does not necessarily had a causal relationship with this treatment. A TEAE was defined as an event that had onset from the first exposure to treatment until the last visit in the trial. Number of TEAEs that occurred during at least 24 weeks from treatment onset (week 0) are presented. The data is presented per dose level participants were on at the time of onset of the adverse event. During at least 24 weeks from treatment onset (week 0)
Secondary Number of Treatment-emergent Adverse Events (TEAEs) During at Least 76 Weeks From Treatment Onset An adverse event (AE) was any untoward medical occurrence in a participant administered a medicinal product, and which does not necessarily had a causal relationship with this treatment. A TEAE was defined as an event that had onset from the first exposure to treatment until the last visit in the trial. Number of TEAEs that occurred during at least 76 weeks from treatment onset (week 0) are presented. The data is presented per dose level participants were on at the time of onset of the adverse event. During at least 76 weeks from treatment onset (week 0)
Secondary Occurrence of Anti-concizumab Antibodies During at Least 24 Weeks From Treatment Onset Occurrence of anti-concizumab antibodies during at least 24 weeks from treatment onset (week 0) is presented. In the reported data, 'Yes' infers number of participants who showed positive anti-concizumab antibody tests whereas 'No' infers number of participants who showed negative anti-concizumab antibody tests. During at least 24 weeks from treatment onset (week 0)
Secondary Occurrence of Anti-concizumab Antibodies During at Least 76 Weeks From Treatment Onset Occurrence of anti-concizumab antibodies during at least 76 weeks from treatment onset (week 0) is presented. In the reported data, 'Yes' infers number of participants who showed positive anti-concizumab antibody tests whereas 'No' infers number of participants who showed negative anti-concizumab antibody tests. During at least 76 weeks from treatment onset (week 0)
Secondary Change in Fibrinogen During 24 Weeks From Treatment Onset Change in fibrinogen during 24 weeks from treatment onset (week 0) is presented. The data is presented per the last dose level which the participants have reached at the time of assessment. During 24 weeks from treatment onset (week 0)
Secondary Change in Fibrinogen During at Least 76 Weeks From Treatment Onset Change in fibrinogen during at least 76 weeks from treatment onset (week 0) is presented. The data is presented per the last dose level which the participants have reached at the time of assessment. During at least 76 weeks from treatment onset (week 0)
Secondary Change in D-dimer During 24 Weeks From Treatment Onset Change in D-dimer during at least 24 weeks from treatment onset (week 0) is presented. The data is presented per the last dose level which the participants have reached at the time of assessment. During 24 weeks from treatment onset (week 0)
Secondary Change in D-dimer During at Least 76 Weeks From Treatment Onset Change in D-dimer during at least 76 weeks from treatment onset (week 0) is presented. The data is presented per the last dose level which the participants have reached at the time of assessment. During at least 76 weeks from treatment onset (week 0)
Secondary Change in Prothrombin Fragment 1 + 2 (F1 + F2) During 24 Weeks From Treatment Onset Change in F1 + F2 during 24 weeks from treatment onset (week 0) is presented. The data is presented per the last dose level which the participants have reached at the time of assessment. During 24 weeks from treatment onset (week 0)
Secondary Change in Prothrombin Fragment 1 + 2 (F1 + F2) During at Least 76 Weeks From Treatment Onset Change in F1 + F2 during at least 76 weeks from treatment onset (week 0) is presented. The data is presented per the last dose level which the participants have reached at the time of assessment. During at least 76 weeks from treatment onset (week 0)
Secondary Change in Prothrombin Time (PT) During 24 Weeks From Treatment Onset Change in PT during 24 weeks from treatment onset (week 0) is presented. The data is presented per the last dose level which the participants have reached at the time of assessment. During 24 weeks from treatment onset (week 0)
Secondary Change in Prothrombin Time (PT) During at Least 76 Weeks From Treatment Onset Change in PT during at least 76 weeks from treatment onset (week 0) is presented. The data is presented per the last dose level which the participants have reached at the time of assessment. During at least 76 weeks from treatment onset (week 0)
Secondary Change in Activated Partial Thromboplastin Time (APTT) During 24 Weeks From Treatment Onset Change in APTT during 24 weeks from treatment onset (week 0) is presented. The data is presented per the last dose level which the participants have reached at the time of assessment. During 24 weeks from treatment onset (week 0)
Secondary Change in Activated Partial Thromboplastin Time (APTT) During at Least 76 Weeks From Treatment Onset Change in APTT during at least 76 weeks from treatment onset (week 0) is presented. The data is presented per the last dose level which the participants have reached at the time of assessment. During at least 76 weeks from treatment onset (week 0)
Secondary Change in Anti-thrombin (AT) During 24 Weeks From Treatment Onset Change in AT during 24 weeks from treatment onset (week 0) is presented. The data is presented per the last dose level which the participants have reached at the time of assessment. During 24 weeks from treatment onset (week 0)
Secondary Change in Anti-thrombin (AT) After at Least 76 Weeks From Treatment Change in AT after at least 76 weeks from treatment onset (week 0) is presented. The data is presented per the last dose level which the participants have reached at the time of assessment. During at least 76 weeks from treatment onset (week 0)
Secondary Concentration of Concizumab Prior to the Last Dose Administration at 24 Weeks Concentration of concizumab prior to the last dose administration at 24 weeks is presented. The data is presented per the last dose level which the participants have reached at the time of assessment. Prior to the last dose administration at 24 weeks
Secondary Concentration of Concizumab Prior to the Last Dose Administration After at Least 76 Weeks Concentration of concizumab prior to the last dose administration after at least 76 weeks is presented. The data is presented per the last dose level which the participants have reached at the time of assessment. Prior to the last dose administration after at least 76 weeks
Secondary Free Tissue Factor Pathway Inhibitor (TFPI) Concentration Value Prior to the Last Dose Administration at 24 Weeks Free TFPI (TFPI not bound to concizumab) concentration value prior to the last dose administration at 24 weeks is presented. The data is presented per the last dose level which the participants have reached at the time of assessment. Prior to the last dose administration at 24 weeks
Secondary Free Tissue Factor Pathway Inhibitor (TFPI) Concentration Value Prior to the Last Dose Administration After at Least 76 Weeks Free TFPI concentration value prior to the last dose administration after at least 76 weeks is presented. The data is presented per the last dose level which the participants have reached at the time of assessment. Prior to the last dose administration after at least 76 weeks
Secondary Peak Thrombin Generation Prior to the Last Dose Administration at 24 Weeks Peak thrombin generation is the maximal concentration of thrombin formed at a given point in time. Peak thrombin generation prior to the last dose administration at 24 weeks is presented. The data is presented per the last dose level which the participants have reached at the time of assessment. Prior to the last dose administration at 24 weeks
Secondary Peak Thrombin Generation Prior to the Last Dose Administration After at Least 76 Weeks Peak thrombin generation is the maximal concentration of thrombin formed at a given point in time. Peak thrombin generation prior to the last dose administration after at least 76 weeks is presented. The data is presented per the last dose level which the participants have reached at the time of assessment. Prior to the last dose administration after at least 76 weeks
Secondary Endogenous Thrombin Potential Prior to the Last Dose Administration at 24 Weeks The endogenous thrombin potential (ETP), defined as the amount of thrombin which can be generated after the in vitro activation of coagulation with tissue factor as trigger and phospholipids as platelet substitute. Endogenous thrombin potential prior to the last dose administration at 24 weeks is presented. The data is presented per the last dose level which the participants have reached at the time of assessment. Prior to the last dose administration at 24 weeks
Secondary Endogenous Thrombin Potential Prior to the Last Dose Administration After at Least 76 Weeks The endogenous thrombin potential (ETP), defined as the amount of thrombin which can be generated after the in vitro activation of coagulation with tissue factor as trigger and phospholipids as platelet substitute. Endogenous thrombin potential prior to the last dose administration after at least 76 weeks is presented. The data is presented per the last dose level which the participants have reached at the time of assessment. Prior to the last dose administration after at least 76 weeks
Secondary Thrombin Generation Velocity Index Prior to the Last Dose Administration at 24 Weeks Thrombin generation velocity index represents the effective rate of thrombin generation between lag time and time to peak. Thrombin generation velocity index prior to the last dose administration at 24 weeks is presented. The data is presented per the last dose level which the participants have reached at the time of assessment. Prior to the last dose administration at 24 weeks
Secondary Thrombin Generation Velocity Index Prior to the Last Dose Administration After at Least 76 Weeks Thrombin generation velocity index represents the effective rate of thrombin generation between lag time and time to peak. Thrombin generation velocity index prior to the last dose administration after at least 76 weeks is presented. The data is presented per the last dose level which the participants have reached at the time of assessment. Prior to the last dose administration after at least 76 weeks
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