Research Into the Effect of a Clot-dissolving Agent and Its Inhibitor
NCT ID: NCT01694381
Last Updated: 2021-01-19
Study Results
The study team has not published outcome measurements, participant flow, or safety data for this trial yet. Check back later for updates.
Basic Information
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TERMINATED
EARLY_PHASE1
8 participants
INTERVENTIONAL
2012-09-30
2012-10-31
Brief Summary
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The primary objectives of the study are:
* To assess the overall safety and tolerability related to systemic plasminogen activation of single doses of M5 over a wide dose range (study part I).
* To assess the effect of single doses of C1-inhibitor on the overall safety and tolerability of single doses of M5 and its effect on M5-induced coagulation changes (study part II).
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Detailed Description
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While it has a negligible effect on urokinase (UK), C1INH inhibits tcM5 irreversibly, preventing non-specific plasminogen activation, responsible for bleeding complications. The effect of endogenous C1INH can be augmented by the addition of exogenous C1INH. In vitro studies in rats and dogs indicated that adding C1INH to plasma prior to clot lysis by M5 prevented bleeding, fibrinogenolysis and plasminogen depletion but did not affect the rate of fibrinolysis. In a recent pilot rat stroke study, at similarly effective doses, M5, preceded by C1INH adjunctive therapy, was equivalent to tPA alone but caused significantly less ICH, was much more effective than tPA preceded by adjunctive C1INH, and was the only group with a significant functional improvement at 24h.
Dose restrictions which limit efficacy of tPA-based thrombolysis are expected to be circumvented by M5 preceded by adjunctive C1INH. C1INH is a commercially available plasma derived product with a well-established safety and efficacy profile and is currently indicated and available for routine prophylaxis of hereditary angioedema (HAE).
Conditions
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Study Design
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RANDOMIZED
PARALLEL
TREATMENT
QUADRUPLE
Study Groups
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mutant pro-urokinase (M5) alone
In the first study part subjects in cohorts of 4 will receive ascending doses of either M5 (3 subjects) or M5-placebo (1 subject) without C1-inhibitor.
M5
single point mutant of serine protease prourokinase
Mutant pro-urokinase (M5) and its inhibitor, C1 inhibitor
In the second study part subjects in cohorts of 5 will receive ascending doses of either M5 or M5-placebo, preceded by a single intravenous dose of C1-inhibitor or C1-inhibitor-placebo. Each subject will randomly be allocated to one of the following treatment arms within one cohort:
* C1-inhibitor followed by M5 (3 subjects);
* C1-inhibitor followed by M5-placebo (1 subject);
* C1-inhibitor-placebo followed by M5-placebo (1 subject).
Dose levels of both M5 and C1-inhibitor within each cohort will be chosen based on the available safety, pharmacokinetic and pharmacodynamic data of the preceding cohorts.
M5
single point mutant of serine protease prourokinase
C1-inhibitor
a protease inhibitor belonging to the serpin superfamily.
Interventions
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M5
single point mutant of serine protease prourokinase
C1-inhibitor
a protease inhibitor belonging to the serpin superfamily.
Eligibility Criteria
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Inclusion Criteria
* Be without clinical significant abnormalities according to the investigator's judgment, based on a detailed medical history, a complete physical examination (including vital signs), a standard 12-lead electrocardiogram, urinalysis, and routine clinical laboratory tests.
* Have endogenous C1-inhibitor, α2-antiplasmin, fibrinogen, and plasminogen levels within the laboratory's reference range.
* Have a negative serology for HIV, HBsAg, and HCV.
* Have a negative test for alcohol and drugs of abuse at screening and on study day -1.
* Be capable of understanding and willing to comply with the conditions and restrictions of the protocol.
* Have read, understood and provided written informed consent.
Exclusion Criteria
* Has a reasonable chance of developing a clinically significant bleeding event or a bleeding event that may go undetected for a considerable amount of time during the study, for example:
* Has undergone major (internal) surgery or trauma within the last three months of the anticipated dosing day;
* Has an intestinal or cerebral vascular malformation;
* Has participated in high impact contact sports, such as kick-boxing, within two weeks of the anticipated dosing day.
* Has received any systemically absorbed drug or substance (including prescription, over-the-counter, or alternative remedies) that is not permitted by this protocol prior to dosing without undergoing a wash-out period of at least seven times the elimination half-life of the product. For aspirin or other products inhibiting thrombocyte-aggregation the wash-out period must not be less than 28 days.
* Has smoked tobacco in any form within three months of dosing, or has ever smoked more than five cigarettes per day (or equivalent) on average.
* Has received blood or plasma derivatives in the year preceding the administration day.
* Has lost blood or plasma outside the limits of the local blood donation service (i.c. Sanquin) three months prior to dosing.
* Has a known hypersensitivity to any of the investigational material or related compounds.
* Has a history of severe hypersensitivity or of an allergy with severe reactions.
* Has a history of substance abuse, including caffeine, tobacco, and alcohol.
* Has a condition or demonstrates an attitude that in the opinion of the investigator might jeopardise the subject's health or well-being, or the scientific integrity of the study results.
* Is mentally or legally incapacitated to provide informed consent.
18 Years
35 Years
MALE
Yes
Sponsors
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TSI, LLC
INDUSTRY
Responsible Party
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Principal Investigators
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Koos Burggraaf, MD, PhD
Role: PRINCIPAL_INVESTIGATOR
Center for Human Drug Research
Locations
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Center for Human Drug Research
Leiden, , Netherlands
Countries
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References
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Tomasi S, Sarmientos P, Giorda G, Gurewich V, Vercelli A. Mutant prourokinase with adjunctive C1-inhibitor is an effective and safer alternative to tPA in rat stroke. PLoS One. 2011;6(7):e21999. doi: 10.1371/journal.pone.0021999. Epub 2011 Jul 14.
Pannell R, Kung W, Gurewich V. C1-inhibitor prevents non-specific plasminogen activation by a prourokinase mutant without impeding fibrin-specific fibrinolysis. J Thromb Haemost. 2007 May;5(5):1047-54. doi: 10.1111/j.1538-7836.2007.02453.x.
Gurewich V, Pannell R, Simmons-Byrd A, Sarmientos P, Liu JN, Badylak SF. Thrombolysis vs. bleeding from hemostatic sites by a prourokinase mutant compared with tissue plasminogen activator. J Thromb Haemost. 2006 Jul;4(7):1559-65. doi: 10.1111/j.1538-7836.2006.01993.x.
Liu JN, Liu JX, Liu Bf BF, Sun Z, Zuo JL, Zhang Px PX, Zhang J, Chen Yh YH, Gurewich V. Prourokinase mutant that induces highly effective clot lysis without interfering with hemostasis. Circ Res. 2002 Apr 19;90(7):757-63. doi: 10.1161/01.res.0000014825.71092.bd.
Other Identifiers
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2012-002225-30
Identifier Type: EUDRACT_NUMBER
Identifier Source: secondary_id
TS01-01
Identifier Type: -
Identifier Source: org_study_id
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