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NCT01434511 Clinical Trial

Study of Modified Recombinant Factor VIII (OBI-1) in Subjects With Congenital Hemophilia A

Hemophilia A Clinical Trial

Official title:
Efficacy and Safety of B-Domain Deleted Recombinant Porcine Factor VIII (OBI-1) in the Treatment of Patients With Congenital Hemophilia A With Factor VIII Inhibitors

Clinical Trial Details — Status: Terminated

Administrative data
NCT number NCT01434511
Other study ID # OBI-1-302
Secondary ID
Status Terminated
Phase Phase 3
First received
Last updated
Start date October 3, 2011
Est. completion date July 29, 2013

Study information
Verified date April 2021
Source Takeda
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

This study is to test whether the study drug (OBI-1) is safe and effective for the treatment of serious bleeding episodes in people with congenital hemophilia A.

Recruitment information / eligibility
Status Terminated
Enrollment 1
Est. completion date July 29, 2013
Est. primary completion date July 29, 2013
Accepts healthy volunteers No
Gender All
Age group 6 Years and older
Eligibility Inclusion Criteria: - Written informed consent/assent from participant and/or participant's parent or legal representative. - Participants with congenital hemophilia A with human factor VIII inhibitor =30 BU assessed within 90 days prior to study entry. - Has previously or is currently demonstrating suboptimal hemostatic response to bypassing agents for treatment of bleeding episodes; suboptimal response is determined by the investigator , but minimally includes no or minimal evidence of response after at least two doses of bypassing agents, either for the current or a historic bleeding episode. - Has an anti-OBI-1 titer = 10 BU - Has any serious or life-threatening bleeding episode; or requires a surgical procedure that could lead to a serious bleeding episode if not well controlled. - Is willing and able to follow all instructions and attend all study visits. - Has no other significant hemostatic abnormality and: - Platelets =100,000/mm-cubed - Prothrombin time < 15 seconds - INR < 1.3 - Participants taking anti-thrombotics (such as clopidogrel, heparin or heparin analogue) may be included provided three half-lives of the agent have elapsed since the last dose of the agent. Exclusion Criteria: - Hemodynamically unstable after blood transfusion, fluid resuscitation and pharmacologic or volume replacement pressor therapy. This hemodynamic instability is characterized by symptomatic hypotension resulting in vital organ dysfunction, such as cardiac ischemia, oliguria (urine volume <0.5 mL/kg in the previous six hours), central nervous system hypoperfusion manifested by mental status change such as confusion (unless head injury or intracranial hemorrhage is present), pulmonary compromise, and/or acidosis (manifested by pH and lactate levels). - Bleeding episode assessed likely to resolve on its own if left untreated. - Use of hemophilia medication: recombinant factor VIIa within 3 hours prior to OBI-1 administration or activated prothrombin complex concentrate (aPCC) treatment within 6 hours prior to OBI-1 administration - Prior history of bleeding disorder other than congenital hemophilia A - Known major sensitivity (anaphylactoid reactions) to porcine or hamster products. Examples include therapeutics of porcine origin (e.g. previously marketed porcine factor VIII, Hyate-C®) and recombinant therapeutics prepared from hamster cells (e.g. Humira®, Advate® and Enbrel®). - Received any other investigational treatment within 30 days of the first OBI-1 treatment. - Anticipated need for treatment or device during the study that may interfere with the evaluation of the safety or efficacy of OBI-1, or whose safety or efficacy may be affected by OBI-1. - Is planning to father a child during the study - Has abnormal baseline findings, any other medical condition(s) or laboratory findings that, in the opinion of the investigator, might jeopardize the participant's safety or decrease the chance of obtaining satisfactory data needed to achieve the objectives of the study. - Inability or unwillingness to comply with the study design, protocol requirements, or the follow-up procedures.

Study Design

Related Conditions & MeSH terms

Intervention

Biological:
OBI-1
intravenous infusion, up to every 2-3 hours for the first 24 hours of treatment

Locations
Country Name City State
South Africa Charlotte Maxeke Johannesburg Academic Hospital Johannesburg Gauteng
United Kingdom Great Ormond Street Hospital London England
United States Indiana Hemophilia and Thrombosis Center Indianapolis Indiana

Sponsors (1)
Lead Sponsor Collaborator
Baxalta now part of Shire

Countries where clinical trial is conducted

United States,  South Africa,  United Kingdom, 

Outcome
Type Measure Description Time frame Safety issue
Primary Proportion of Serious Bleeding Episodes Responsive to OBI-1 This study was terminated early and only enrolled one participant. Due to concerns that the participant would be at risk of being re-identified, the study results are not posted. The decision to terminate this study was not related to any safety and/or efficacy concern of OBI-1 in the indication described within the OBI-1-302 study (Congenital Hemophilia A). 24 hours after initiation of treatment
Secondary Overall Proportion of Serious Bleeding Episodes Successfully Controlled With OBI-1 Therapy, as Assessed by the Investigator. Through 90 days ± 7days following final OBI-1 dose
Secondary Proportion of Bleeding Episodes Responsive to OBI-1 Therapy at Designated Assessment Time Points After the Initiation of Therapy, as Assessed by the Investigator Through 90 days ± 7days following final OBI-1 dose
Secondary Frequency of Infusions of OBI-1 Required to Successfully Control Qualifying Bleeding Episodes. Through 90 days ± 7days following final OBI-1 dose
Secondary Total Dose of OBI-1 Required to Successfully Control Qualifying Bleeding Episodes. Through 90 days ± 7days following final OBI-1 dose
Secondary Total Number of Infusions of OBI-1 Required to Successfully Control Qualifying Bleeding Episodes. Through 90 days ± 7days following final OBI-1 dose
Secondary Correlation Between Response to OBI-1 Therapy at Specified Time Points and Eventual Control of Serious Bleeding Episodes. Through 90 days ± 7days following final OBI-1 dose
Secondary Correlation Between the Pre-infusion Anti-OBI-1 Antibody Titers, the Total Dose of OBI-1, the Outcome at 24 Hours and the Eventual Control of the Bleeding Episode. Frame: Through 90 days ± 7days following final OBI-1 dose
Secondary Correlation Between the Pre-infusion Anti-OBI-1 Antibody Titers and the Recovery of OBI-1. Through 90 days ± 7days following final OBI-1 dose
Secondary Recovery and Elimination Rate Parameters of OBI-1 in Subjects With Inhibitors Treated With OBI-1 Therapy. Through 90 days ± 7days following final OBI-1 dose
Secondary Efficacy Assessment of OBI-1 in Participants With Anti-human Factor VIII Titers >30 Bethesda Units (BU) Through 90 days ± 7days following final OBI-1 dose
Secondary Anti-human Factor VIII Antibody Titer. Through 90 days ± 7days following final OBI-1 dose
Secondary Anti-OBI-1 Antibody Titer. Through 90 days ± 7days following final OBI-1 dose
Secondary Anti-host Cell Protein Baby Hamster Kidney (BHK) Antibody Titer. Through 90 days ± 7days following final OBI-1 dose
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