Prevention of Thrombosis Recurrence in Patients With Low Circulating Levels of Antithrombin.
NCT ID: NCT01382550
Last Updated: 2012-09-13
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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UNKNOWN
900 participants
OBSERVATIONAL
1993-03-31
Brief Summary
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Detailed Description
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In each case, objective diagnosis has to be achieved by compression ultrasonography, the diagnosis being based on the lack of compressibility of one or more venous segments. PE has to be documented by ventilation/perfusion lung scanning or by spiral computed tomography (CT).
For each subject, information about pregnancy, active malignancy, recent (\<3 mo) surgery or trauma, fracture, immobilization, acute medical illness, use of oral contraceptives, long-distance travel, personal or family history of arterial and/or venous thrombosis or repeated birth losses will be collected. In the presence of at least one of the previous risk factors, VTE will be defined as secondary otherwise idiopathic. Further information, collected from the whole population by a trained staff, were the following: gender, age, weight, height, body mass index (BMI), waist circumference, personal history of symptomatic atherosclerosis (i.e. ischemic stroke, transient ischemic attack, acute myocardial infarction, angina, intermittent claudication), arterial hypertension, use of antihypertensive drugs, diabetes mellitus, use of antidiabetic drugs, hyperlipidemia, use of statins, smoking habit (use of cigarettes/d), current use of heparin, use of oral anticoagulant (how long) or of antiplatelet drugs (how long), chronic consumption of other drugs.
All these information will be collected by a trained staff on admission and during follow-up visits (every 4-6 months).
Exclusion criteria: missing data during the follow-up; contraindications to or lack of compliance to oral anticoagulation (OAT), lack of informed consent; history of previous VTE event; indication for continuous oral anticoagulation (e.g., an artificial heart valve or chronic atrial fibrillation); events occurring during pregnancy, malignancy, puerperium, oral contraceptive intake, hormone replacement therapy; deficiencies of Prot. C and Prot S or combined inhibitor deficiencies.
Laboratory Studies All laboratory evaluations will be carried out at least 2 weeks after cessation of the anticoagulant therapy or after a switching to low-molecular weight heparin (LMWH) treatment. Antithrombin (AT) functional activity will be measured and VTE patients will be stratified into 3 subgroups of AT% (1st: \<70%, 2nd: 70-80, 3rd: \>81%). AT measurements will be confirmed in a second sample collected 3 months later. In case of discrepancy between the results of the 2 tests, a third sample will be collected. Protein C and S; antiphospholipid antibodies (IgG and IgM); homocysteine, and factor V Leiden and prothrombin 20210A polymorphisms will be determined using commercially available kits by technicians who had been unaware of the patients' treatment assignments and of the clinical course.
Antithrombotic treatment The antithrombotic treatment will be decided according to the usual practice of the enrolling Center. The duration of the initial treatment with parenteral anticoagulation (Low Molecular Weight Heparin or Fondaparinux), the beginning of oral anticoagulation (OAT) with Vit K inhibitors and the International Normalized Ratio (INR) target will be recorded.
According to Center indications the OAT duration (6 months, 12 months or long-lasting) will be recorded and population will be stratified accordingly. The length of therapy will be counted from the date when a stable prothrombin time within the target INR range is achieved.
The occurrence of surgery, trauma, prolonged immobilization (\>7 days), pregnancy (VTE risk periods) during the follow-up and the use of adequate anti-thrombotic prophylaxis will be recorded.
Follow-up Subjects will be followed-up at 3, 6, and 12 months after enrollment and at least every 6 months thereafter either by a visit to the Center or by telephone contact. INR values will be reported by telephone twice monthly. At each visit the patients will be asked about new symptoms of VTE and about bleeding manifestations. When appropriate, a clinical assessment will be made and diagnostic tests will be performed.
Information on major and minor bleedings during oral anticoagulation will be collected in the whole sample. Major bleedings will be defined as hemorrhages that were either retroperitoneal or intracranial or associated with a decrease in hemoglobin of at least 2.0 g per deciliter or that had required either transfusion of at least 2 units of blood (or of red cells) or an invasive procedure, including surgery, to stop them or if they warranted permanent OAT withdrawing.
Study end points The incidence of objectively documented recurrent VTE (DVT and/or PE) during the life-long follow-up is the primary outcome of this study. Contralateral DVT and PE will be computed as a recurrence. Ipsilateral DVT will be adjudicated recurrent if the results of the tests are worse than those obtained in a previous test or if the thrombus is diagnosed in another venous district of the leg. DVT of the arm; CT or MRI-documented occlusion of cerebral/abdominal veins; ultrasound-documented thrombosis of the great saphenous vein of the leg not involved in the first appearance will be also defined as a recurrence. The total (minor and major) bleeding occurrence during the life-long follow-up represents the safety end-point of this study and will be analyzed according to the thrombolysis in myocardial infarction (TIMI) bleeding score.
Sample size Assuming a 20:1:1 sample size ratio between AT% subgroups (AT%\> 80%; AT%=70-80%; and AT%\<70%, respectively), to detect an increase in the incidence of recurrent events from 0.3 in the control population (AT% \> 80%) to 0.6 in each of the other two subgroups (AT%=70-80% and AT%\<70%), a sample size of about 900 subjects is needed (power= 95%; α=0.025, to allow for two independent comparisons).
Expected results Among individuals with a history of first VTE stratified according to AT% levels, the risk/benefit analysis of this study will help identify group(s) of individuals with a strong indication to long-term oral anticoagulation.
Conditions
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Keywords
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Study Design
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COHORT
PROSPECTIVE
Study Groups
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VTE subjects
subjects with a recent (\<3 months) first VTE event undergoing long-lasting OAT or 12-month OAT
Exclusion criteria: missing data during the follow-up; contraindications to or lack of compliance to oral anticoagulation (OAT), lack of informed consent; history of previous VTE event; indication for continuous oral anticoagulation (e.g., an artificial heart valve or chronic atrial fibrillation); events occurring during pregnancy, malignancy, puerperium, oral contraceptive intake, hormone replacement therapy; deficiencies of Prot. C and Prot S or combined inhibitor deficiencies.
long-lasting OAT or 12-month OAT
The antithrombotic treatment will be decided according to usual practice of enrolling Centers. The duration of the initial treatment with parenteral anticoagulation (Low Molecular Weight Heparin or Fondaparinux), the beginning of oral anticoagulation (OAT) with Vit K inhibitors and the International Normalized Ratio (PT-INR) target will be recorded.
According to Center indications the OAT duration (6 months, 12 months or long-lasting) will be recorded and population will be stratified accordingly. The length of therapy will be counted from the date when a stable PT-INR is achieved.
The occurrence of surgery, trauma, prolonged immobilization (\>7 days), pregnancy (VTE risk periods) during the follow-up and the use of adequate anti-thrombotic prophylaxis will be recorded.
Interventions
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long-lasting OAT or 12-month OAT
The antithrombotic treatment will be decided according to usual practice of enrolling Centers. The duration of the initial treatment with parenteral anticoagulation (Low Molecular Weight Heparin or Fondaparinux), the beginning of oral anticoagulation (OAT) with Vit K inhibitors and the International Normalized Ratio (PT-INR) target will be recorded.
According to Center indications the OAT duration (6 months, 12 months or long-lasting) will be recorded and population will be stratified accordingly. The length of therapy will be counted from the date when a stable PT-INR is achieved.
The occurrence of surgery, trauma, prolonged immobilization (\>7 days), pregnancy (VTE risk periods) during the follow-up and the use of adequate anti-thrombotic prophylaxis will be recorded.
Eligibility Criteria
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Inclusion Criteria
Exclusion Criteria
18 Years
80 Years
ALL
No
Sponsors
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Federico II University
OTHER
Responsible Party
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Giovanni Di Minno
Director of the Dept of Clinical and Experimental Medicine
Principal Investigators
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Giovanni Di Minno, Prof
Role: STUDY_CHAIR
Federico II University
Matteo Nicola Dario Di Minno, MD
Role: PRINCIPAL_INVESTIGATOR
Federico II University
Anna Maria Cerbone, MD
Role: PRINCIPAL_INVESTIGATOR
Federico II University
Antonella Tufano, MD
Role: PRINCIPAL_INVESTIGATOR
Federico II University
Locations
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Federico II University
Naples, Italy, Italy
Countries
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Central Contacts
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Facility Contacts
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Giovanni Di Minno, Prof
Role: primary
References
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Di Minno MN, Dentali F, Lupoli R, Ageno W. Mild antithrombin deficiency and risk of recurrent venous thromboembolism: a prospective cohort study. Circulation. 2014 Jan 28;129(4):497-503. doi: 10.1161/CIRCULATIONAHA.113.003756. Epub 2013 Oct 21.
Other Identifiers
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AT 63/11
Identifier Type: -
Identifier Source: org_study_id