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NCT05568719 Clinical Trial

Safety and Effectiveness of Giroctocogene Fitelparvovec or Fidanacogene Elaparvovec in Patients With Hemophilia A or B Respectively

Hemophilia A Clinical Trial

Official title:
A PHASE 3, NON-INVESTIGATIONAL PRODUCT, MULTI COUNTRY COHORT STUDY TO DESCRIBE THE LONG-TERM SAFETY AND EFFECTIVENESS OF A PRIOR SINGLE-DOSE TREATMENT WITH INVESTIGATIVE GIROCTOCOGENE FITELPARVOVEC OR FIDANACOGENE ELAPARVOVEC IN PARTICIPANTS WITH HEMOPHILIA A OR HEMOPHILIA B, RESPECTIVELY

Clinical Trial Details — Status: Recruiting

Administrative data
NCT number NCT05568719
Other study ID # C0371017
Secondary ID
Status Recruiting
Phase Phase 3
First received
Last updated
Start date December 28, 2022
Est. completion date April 8, 2038

Study information
Verified date May 2024
Source Pfizer
Contact Pfizer CT.gov Call Center
Phone 1-800-718-1021
Email ClinicalTrials.gov_Inquiries@pfizer.com
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

A study to learn about the long-term safety and efficacy of giroctocogene fitelparvovec or fidanacogene elaparvovec in patients with hemophilia A or hemophilia B respectively, who have received treatment through prior participation in a Pfizer-sponsored clinical trial. Data collection and participant visits will be based on standard of care.

Recruitment information / eligibility
Status Recruiting
Enrollment 263
Est. completion date April 8, 2038
Est. primary completion date April 8, 2038
Accepts healthy volunteers No
Gender Male
Age group 18 Years and older
Eligibility Inclusion Criteria: -Only participants who received investigational giroctocogene fitelparvovec or fidanacogene eleparvovec and were enrolled in a Pfizer-sponsored study (C0371002, C0371003, C0371005, C3731001, C3731003) are eligible. Exclusion Criteria: -None

Study Design

Related Conditions & MeSH terms

Intervention

Diagnostic Test:
Testing of hepatic AAV Vector integration
Evaluation of AAV vector integration in participants for whom a sample of liver has been obtained through biopsy or surgical resection when clinically indicated

Locations
Country Name City State
Australia Royal Prince Alfred Hospital Camperdown New South Wales
Turkey Ege Universitesi Hastanesi Izmir I?zmir
United States Mississippi Center For Advanced Medicine Madison Mississippi
United States The Childrens Hospital of Philadelphia Division of Hematology Philadelphia Pennsylvania
United States Washington Institute for Coagulation Seattle Washington
United States USF Health Morsani Center For Advanced Healthcare Tampa Florida

Sponsors (1)
Lead Sponsor Collaborator
Pfizer

Countries where clinical trial is conducted

United States,  Australia,  Turkey, 

References & Publications (5)

Berntorp E, Shapiro AD. Modern haemophilia care. Lancet. 2012 Apr 14;379(9824):1447-56. doi: 10.1016/S0140-6736(11)61139-2. Epub 2012 Mar 27. — View Citation

Blanchette VS, Key NS, Ljung LR, Manco-Johnson MJ, van den Berg HM, Srivastava A; Subcommittee on Factor VIII, Factor IX and Rare Coagulation Disorders of the Scientific and Standardization Committee of the International Society on Thrombosis and Hemostasis. Definitions in hemophilia: communication from the SSC of the ISTH. J Thromb Haemost. 2014 Nov;12(11):1935-9. doi: 10.1111/jth.12672. Epub 2014 Sep 3. No abstract available. — View Citation

Blanchette VS, McCready M, Achonu C, Abdolell M, Rivard G, Manco-Johnson MJ. A survey of factor prophylaxis in boys with haemophilia followed in North American haemophilia treatment centres. Haemophilia. 2003 May;9 Suppl 1:19-26; discussion 26. doi: 10.1046/j.1365-2516.9.s1.12.x. — View Citation

Lillicrap D. Extending half-life in coagulation factors: where do we stand? Thromb Res. 2008;122 Suppl 4:S2-8. doi: 10.1016/S0049-3848(08)70027-6. — View Citation

WFH guidelines: https://www1.wfh.org/publication/files/pdf-1472.pdf

Outcome
Type Measure Description Time frame Safety issue
Primary Incidence of thromboembolic events Day 1 to 10 years
Primary Incidence of factor inhibitor development FIX inhibitor development was defined as an inhibitor titer >= 0.6 Bethesda units per milliliter (BU/mL). Day 1 to 10 years
Primary Incidence of hepatic malignancy Day 1 to 10 years
Primary Incidence of liver abnormalities Day 1 to 10 years
Primary Factor activity level Factor activity level will be reported. Factor levels may be measured using different assay methods including a one-stage assay or by chromogenic substrate assay and a second one-stage assay. Day 1 to 10 years
Secondary Total ABR (treated or untreated; (excluding bleeds related to surgery) ABR (Annual Bleed Rate): number of bleeding episodes per year. This includes treated and untreated bleeds.
The ABR or the annualized number of bleeding episodes per year, will be derived for each participant for each observation period by using the following formula:
ABR = (Number of bleeds / Days in observation period) x 365.25 days/year.		 Day 1 to 10 years
Secondary Incidence of and time from vector infusion to resumption of prophylaxis Describe incidence of resumption of prophylaxis resumption and the time (in days) to resumption of prophylaxis after receiving vector infusion. Day 1 to 10 years
Secondary AIR of exogenous factor (excluding infusions related to surgery) The AIR or the annualized number of FIX infusions per year, will be derived for each participant for each observation period by using the following formula:
AIR = (Number of FIX infusions / Days in observation period) x 365.25 days/year.		 Day 1 to 10 years
Secondary Consumption of exogenous factor (excluding infusions related to surgery) The annualized TFC in international units (IU) will be derived for each participant for each observation period using the following formula:
Annualized TFC = (Total units of FIX infused (IU)/ Days in observation period) x 365.25 days/year		 Day 1 to 10 years
Secondary Incidence of Non-hepatic malignancy Day 1 to 10 years
Secondary Incidence of Auto-immune disorders Day 1 to 10 years
Secondary Incidence of SAEs An SAE was an AE resulting in any of the following outcomes or deemed significant for any other reason: death; initial or prolonged inpatient hospitalization; life-threatening experience (immediate risk of dying); persistent or significant disability/incapacity; congenital anomaly; development of a clinical thrombotic event; development of factor inhibitor; development of a hepatic malignancy; development of drug-related elevated hepatic transaminases that fail to improve with immunosuppressive regimens; occurrence of a malignancy with reasonable possibility of being related to study drug. Day 1 to 10 years
Secondary All cause mortality All-cause mortality was defined as the death due to any cause during the course of study. Incidence rate was defined as the total number of participants with admissible events divided by the total (for all qualifying participants) time at risk for the cohort/treatment group of interest. Incidence rate of all-cause deaths was reported in this outcome measure. Day 1 to 10 years
Secondary EQ-5D-5L dimension and VAS scores The EQ-5D-5L comprises a 5-item health status measure and a visual analog rating scale/feeling thermometer. Using the 5-dimensional Health State Classification, participants are asked to respond to five questions on different aspects of their health status that assess the following:
Mobility
Self-care
Usual activities
Pain/Discomfort
Anxiety/Depression		 Day 1 to 10 years
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