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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT03417245
Other study ID # EFC14769
Secondary ID ALN-AT3SC-004201
Status Completed
Phase Phase 3
First received
Last updated
Start date March 1, 2018
Est. completion date July 14, 2021

Study information

Verified date March 2022
Source Sanofi
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

Primary Objective: -To evaluate the efficacy of fitusiran compared to on-demand treatment with factor concentrates, as determined by the frequency of bleeding episodes. Secondary Objectives: - To evaluate the efficacy of fitusiran compared to on-demand treatment with factor concentrates, as determined by: - The frequency of spontaneous bleeding episodes. - The frequency of joint bleeding episodes. - Health-related quality of life (HRQOL) in participants >=17 years of age. - To determine the frequency of bleeding episodes during the onset period. - To determine the safety and tolerability of fitusiran.


Description:

The duration of treatment with fitusiran was 9 months. The estimated total time on study, inclusive of screening, was up to 11 months for all participants in the factor on-demand arm and for participants in the fitusiran arm who enrolled in the extension study (LTE15174). The estimated total time on the study was up to 17 months for participants in the fitusiran treatment arm who did not enroll in the extension study due to the requirement for up to an additional 6 months of follow-up monitoring for antithrombin levels. Participants who completed the study will be eligible for an open-label extension study LTE15174 (NCT03754790).


Recruitment information / eligibility

Status Completed
Enrollment 120
Est. completion date July 14, 2021
Est. primary completion date January 26, 2021
Accepts healthy volunteers No
Gender Male
Age group 12 Years and older
Eligibility Inclusion Criteria: - Males, >=12 years of age. - Severe hemophilia A or B without inhibitors. - Severity confirmed by a central laboratory where FVIII level was less than (<) 1 percent (%) or Factor IX (FIX) level was less than or equal to (<=) 2% at Screening. - On-demand use of factor concentrate to manage bleeding episodes for at least the last 6 months prior to Screening, and meet each of the following criterion: - Nijmegen modified Bethesda assay inhibitor titer of <0.6 Bethesda units per milliliter (BU/mL) at Screening. - No use of Bypassing agents to treat bleeding episodes for at least the last 6 months prior to Screening. - No history of immune tolerance induction therapy within the last 3 years prior to Screening. - A minimum of 6 bleeding episodes requiring factor concentrate treatment within the last 6 months prior to Screening. - Willing and complied with the study requirements and to provide written informed consent and assent. Exclusion Criteria: - Known co-existing bleeding disorders other than hemophilia A or B, i.e., Von Willebrand's disease, additional factor deficiencies, or platelet disorders. - Antithrombin (AT) activity <60% at Screening. - Co-existing thrombophilic disorder. - Clinically significant liver disease. - Active hepatitis C virus infection. - HIV positive with a cluster of differentiation-4 count of <200 cells/microliter. - History of arterial or venous thromboembolism. - Inadequate renal function. - History of multiple drug allergies or history of allergic reaction to an oligonucleotide or N-Acetylgalactosamine (GalNAc). - History of intolerance to SC injection(s). - Any other conditions or comorbidities that would make the participant unsuitable for enrollment or could interfere with participation in or completion of the study, per Investigator judgment.

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
fitusiran
by SC injection
factor concentrates
by intravenous (IV) injection

Locations

Country Name City State
Australia Investigational Site Number 6101 Camperdown
Australia Investigational Site Number 6103 Murdoch
Australia Investigational Site Number 6104 Prahran
China Investigational Site Number 8604 Beijing
China Investigational Site Number 8602 Guangzhou
China Investigational Site Number 8605 Hangzhou
China Investigational Site Number 8603 Shanghai
China Investigational Site Number 8601 Tianjin
Denmark Investigational Site Number 4501 Copenhagen
France Investigational Site Number 3303 Lyon
France Investigational Site Number 3305 Paris
France Investigational Site Number 3301 Rouen
Germany Investigational Site Number 4904 Berlin
Germany Investigational Site Number 4905 Frankfurt Am Main
Germany Investigational Site Number 4906 Leipzig
Hungary Investigational Site Number 3602 Budapest
India Investigational Site Number 9102 Bangalore
India Investigational Site Number 9104 Jaipur
India Investigational Site Number 9106 Lucknow
India Investigational Site Number 9108 Mumbai
India Investigational Site Number 9109 Mumbai
India Investigational Site Number 9111 Mumbai
India Investigational Site Number 9103 Pune
India Investigational Site Number 9105 Vellore
Israel Investigational Site Number 9701 Ramat-Gan
Italy Investigational Site Number 3904 Padova
Japan Investigational Site Number 8105 Isehara
Japan Investigational Site Number 8104 Saitama
Korea, Republic of Investigational Site Number 8201 Busan
Korea, Republic of Investigational Site Number 8202 Daejeon
Korea, Republic of Investigational Site Number 8204 Seoul
Malaysia Investigational Site Number 6004 Ampang
Malaysia Investigational Site Number 6002 Johor Bahru
Malaysia Investigational Site Number 6003 Kota Kinabalu
South Africa Investigational Site Number 2701 Parktown
South Africa Investigational Site Number 2702 Port Elizabeth
Spain Investigational Site Number 3402 Madrid
Taiwan Investigational Site Number 8805 Taichung
Taiwan Investigational Site Number 8807 Taichung
Taiwan Investigational Site Number 8801 Taipei
Taiwan Investigational Site Number 8804 Taipei
Taiwan Investigational Site Number 8808 Taoyuan
Turkey Investigational Site Number 9002 Adana
Turkey Investigational Site Number 9004 Antalya
Turkey Investigational Site Number 9008 Gaziantep
Turkey Investigational Site Number 9005 Istanbul
Turkey Investigational Site Number 9003 Izmir
Turkey Investigational Site Number 9009 Kayseri
Turkey Investigational Site Number 9006 Samsun
Ukraine Investigational Site Number 8001 Kyiv
Ukraine Investigational Site Number 8003 Kyiv
Ukraine Investigational Site Number 8002 Lviv
Ukraine Investigational Site Number 8005 Mykolaiv
United Kingdom Investigational Site Number 4402 Glasgow
United Kingdom Investigational Site Number 4401 London
United Kingdom Investigational Site Number 4407 London
United States Investigational Site Number 110 Akron Ohio
United States Investigational Site Number 125 Ann Arbor Michigan
United States Investigational Site Number 102 Chicago Illinois
United States Investigational Site Number 128 Gainesville Florida
United States Investigational Site Number 111 Las Vegas Nevada
United States Investigational Site Number 0140 Little Rock Arkansas
United States Investigational Site Number 119 New Orleans Louisiana
United States Investigational Site Number 103 Tampa Florida

Sponsors (1)

Lead Sponsor Collaborator
Genzyme, a Sanofi Company

Countries where clinical trial is conducted

United States,  Australia,  China,  Denmark,  France,  Germany,  Hungary,  India,  Israel,  Italy,  Japan,  Korea, Republic of,  Malaysia,  South Africa,  Spain,  Taiwan,  Turkey,  Ukraine,  United Kingdom, 

Outcome

Type Measure Description Time frame Safety issue
Primary Estimated Annualized Bleeding Rate (ABR) for Treated Bleeds During the Efficacy Period ABR for a participant during efficacy period (EP) was defined as annualized number of bleeding episodes during EP annualized to a 1-year interval of time. Treated Bleeding episode: any occurrence of hemorrhage that required administration of by-passing agents (BPA) or factor. It started from first sign of a bleed and ended no more than 72 hours after last treatment for bleed, within which any symptoms of bleeding at same location or injections less than or equal to (<=) 72 hours apart were considered the same bleeding episode. EP was defined as time duration starting from Day 29 when antithrombin (AT) lowering capacity of fitusiran had achieved therapeutic target range to the earliest of Day 246 or last day of bleeding follow up (maximum duration of EP: from Day 29 to Day 246). This outcome measure (OM) presents estimated results (i.e., results received by applying negative binomial [NB] regression model on data collected during EP). From Day 29 up to Day 246 or up to the last day of bleeding follow up (any day up to Day 246), whichever was the earliest
Primary Observed Annualized Bleeding Rate (ABR) for Treated Bleeds During the Efficacy Period ABR for a participant during EP was defined as annualized number of bleeding episodes during EP annualized to a 1-year interval of time. ABR= number of bleeding episodes during EP divided by total number of days during EP*365.25. A bleeding episode was defined as any occurrence of hemorrhage that required administration of BPA or factor. It started from the first sign of a bleed and ended no more than 72 hours after the last treatment for the bleed, within which any symptoms of bleeding at the same location or injections <=72 hours apart were considered the same bleeding episode. EP was defined as time duration starting from Day 29 when the AT lowering capacity of fitusiran had achieved therapeutic target range to the earliest of Day 246 or the last day of bleeding follow up (maximum duration of EP: from Day 29 to Day 246). This OM presents observed results (i.e., descriptive statistics values based on the data collected during EP). From Day 29 up to Day 246 or up to the last day of bleeding follow up (any day up to Day 246), whichever was the earliest
Secondary Estimated Annualized Bleeding Rate (ABR) for Treated Bleeds During the Treatment Period ABR for a participant during treatment period (TP) was defined as annualized number of bleeding episodes during TP annualized to a 1-year interval of time. Bleeding episode: any occurrence of hemorrhage that required administration of BPA or factor. It started from first sign of a bleed and ended no more than 72 hours after last treatment for bleed, within which any symptoms of bleeding at same location or injections <=72 hours apart were considered the same bleeding episode. TP was sum of onset period (first 28 days after first dose of fitusiran) and EP (starting on Day 29 when AT lowering capacity of fitusiran had achieved therapeutic target range to earliest of Day 246 or last day of bleeding follow up (maximum duration of TP: from Day 1 to Day 246). This OM presents estimated results (i.e., results received by applying NB regression model on data collected during TP). From Day 1 up to Day 246 or up to the last day of bleeding follow up (any day up to Day 246), whichever was the earliest
Secondary Observed Annualized Bleeding Rate (ABR) for Treated Bleeds During the Treatment Period ABR for a participant during TP was defined as annualized number of bleeding episodes during TP annualized to a 1- year interval of time. ABR= number of bleeding episodes during TP divided by total number of days during TP*365.25. Bleeding episode: any occurrence of hemorrhage that required administration of BPA or factor. It started from the first sign of a bleed and ended no more than 72 hours after last treatment for bleed, within which any symptoms of bleeding at the same location or injections <=72 hours apart were considered the same bleeding episode. TP was sum of onset period (first 28 days after the first dose of fitusiran) and EP (starting on Day 29 when AT lowering capacity of fitusiran had achieved therapeutic target range to the earliest of Day 246 or the last day of bleeding follow up (maximum duration of TP: from Day 1 to Day 246). This OM presents observed results (i.e., descriptive statistics values based on data collected during TP). From Day 1 up to Day 246 or up to the last day of bleeding follow up (any day up to Day 246), whichever was the earliest
Secondary Estimated Annualized Spontaneous Bleeding Rate for Treated Bleeds During the Efficacy Period Annualized spontaneous bleeding rate for a participant during EP was defined as annualized number of spontaneous bleeding episodes during EP annualized to a 1-year interval of time. Spontaneous bleeding episode was bleeding event that occurred for no apparent or known reason, particularly into joints, muscles, and soft tissues. It started from first sign of a bleed and ended no more than 72 hours after last treatment for the bleed, within which any symptoms of bleeding at the same location or injections <=72 hours apart were considered the same bleeding episode. EP was defined as time duration starting from Day 29 when AT lowering capacity of fitusiran had achieved therapeutic target range to the earliest of Day 246 or last day of bleeding follow up (maximum duration of EP: from Day 29 to Day 246). This OM presents estimated results (i.e., results received by applying NB regression model on data collected during EP). From Day 29 up to Day 246 or up to the last day of bleeding follow up (any day up to Day 246), whichever was the earliest
Secondary Observed Annualized Spontaneous Bleeding Rate for Treated Bleeds During the Efficacy Period ABR for participant during EP was defined as annualized number of spontaneous bleeding episodes during EP annualized to a 1-year interval of time. ABR=number of treated spontaneous bleeding episodes during EP divided by total number of days during EP*365.25. Spontaneous bleeding episode was bleeding event that occurred for no apparent or known reason, into joints, muscles, and soft tissues. It started from the first sign of a bleed and ended no more than 72 hours after the last treatment for the bleed, within which any symptoms of bleeding at the same location or injections <=72 hours apart were considered the same bleeding episode. EP: time duration starting from Day 29 when the AT lowering capacity of fitusiran had achieved therapeutic target range to earliest of Day 246 or the last day of bleeding follow up (maximum duration of EP: from Day 29 to Day 246).This OM presents observed results (i.e., descriptive statistics values based on data collected during EP). From Day 29 up to Day 246 or up to the last day of bleeding follow up (any day up to Day 246), whichever was the earliest
Secondary Estimated Annualized Joint Bleeding Rate for Treated Bleeds During the Efficacy Period Annualized joint bleeding rate for a participant during EP was defined as annualized number of bleeding episodes during EP annualized to a 1-year interval of time. Joint bleeding episode was characterized by an unusual sensation in the joint ("aura") in combination with 1) increasing swelling or warmth over the skin, joint, 2) increasing pain, or 3) progressive loss of range of motion or difficulty in using the limb as compared with Baseline. It started from first sign of a bleed and ended no more than 72 hours after last treatment for the bleed. EP was defined as time duration starting from Day 29 when the AT lowering capacity of fitusiran had achieved therapeutic target range to the earliest of Day 246 or the last day of bleeding follow up (maximum duration of EP: from Day 29 to Day 246). This OM presents estimated results (i.e., results received by applying NB regression model on data collected during EP). From Day 29 up to Day 246 or up to the last day of bleeding follow up (any day up to Day 246), whichever was the earliest
Secondary Observed Annualized Joint Bleeding Rate for Treated Bleeds During the Efficacy Period Annualized joint bleeding rate for participant during EP was defined as annualized number of joint bleeding episodes during EP annualized to 1-year interval of time. ABR= number of treated joint bleeding episodes during EP divided by total number of days during EP*365.25. A joint bleeding episode was characterized by an unusual sensation in joint ("aura") in combination with 1) increasing swelling or warmth over skin, joint, 2) increasing pain, or 3) progressive loss of range of motion or difficulty in using limb as compared with Baseline. It started from first sign of a bleed and ended no more than 72 hours after the last treatment for the bleed. EP: time duration starting from Day 29 when the AT lowering capacity of fitusiran had achieved therapeutic target range to the earliest of Day 246 or last day of bleeding follow up (maximum duration of EP: from Day 29 to Day 246). This OM presents observed results (i.e., descriptive statistics values based on data collected during EP). From Day 29 up to Day 246 or up to the last day of bleeding follow up (any day up to Day 246), whichever was the earliest
Secondary Health-related Quality of Life (HRQOL): Change From Baseline in Haemophilia Quality of Life Questionnaire for Adults (Haem-A-QOL) Physical Health Score at Month 9 Haem-A-QoL: participant-reported questionnaire designed for adult participants (>=17 years of age) with hemophilia; and consisted of 46 items comprising 10 domains (physical health, feelings, view of yourself, sports and leisure, work and school, dealing with hemophilia, treatment, future, family planning, partnership and sexuality). Scoring for each item was based on a 5-point Likert scale (1= never, 2= rarely, 3= sometimes, 4= often, and 5=all the time), and higher scores represented greater impairment. Change from baseline in physical health domain score was reported in this outcome measure. Raw score for physical health domain were transformed to a scale ranged from 0 (better health outcome) to 100 (worst health outcome), where lower scores denoted better physical health. Baseline (Day 1), Month 9
Secondary Health-related Quality of Life (HRQOL): Change From Baseline in Haem-A-QOL Total Score at Month 9 Haem-A-QoL: participant-reported questionnaire designed for adult participants (>=17 years of age) with hemophilia; and consisted of 46 items comprising 10 domains (physical health, feelings, view of yourself, sports and leisure, work and school, dealing with hemophilia, treatment, future, family planning, partnership and sexuality). Scoring for each item was based on a 5-point Likert scale (1= never, 2= rarely, 3= sometimes, 4= often, and 5=all the time), and higher scores represent greater impairment. Raw score for each domain were transformed to a scale ranged between 0 and 100, where lower scores denoted better health. Haem-A-QoL total score was average of all domain scores and ranged from 0 (better health outcome) to 100 (worst health outcome), where lower scores denoted better physical health. Baseline (Day 1), Month 9
Secondary Estimated Annualized Bleeding Rate (ABR) for Treated Bleeds During the Onset Period ABR was annualized number of bleeding episodes during onset period per participant annualized to a 1-year interval of time. A treated bleeding episode was defined as any occurrence of hemorrhage that required administration of BPA or factor. It started from the first sign of a bleed and ended no more than 72 hours after the last treatment for the bleed, within which any symptoms of bleeding at the same location or injections <=72 hours apart were considered the same bleeding episode. The onset period was defined as time interval from Day 1 to the earlier of Day 28 or the last day of bleeding follow up. This OM presents estimated results (i.e., results received by applying NB regression model on data collected during onset period). From Day 1 up to Day 28 or up to the last day of bleeding follow up (any day up to Day 28), whichever was the earliest
Secondary Number of Participants With Treatment Emergent Adverse Events (TEAEs) and Treatment-Emergent Serious Adverse Events (TESAEs) An adverse event (AE) was defined as any untoward medical occurrence in a participant who received study drug which did not necessarily have a causal relationship with the treatment. Treatment-emergent AEs were defined as any AE with onset date after first dose of fitusiran in the fitusiran prophylaxis arm or after Day 1 visit in the factor on-demand arm. A serious AE (SAE) was defined as any untoward medical occurrence that at any dose: resulted in death, was life-threatening, required inpatient hospitalization or prolongation of existing hospitalization, resulted in persistent or significant disability or incapacity, was a congenital anomaly or birth defect, or was a medically important event. From Baseline (Day 1) up to 15 months (i.e., 9 months treatment period + 6-month follow-up)
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