Deep Vein Thrombosis Clinical Trial
Official title:
Absence of Residual Vein Thrombosis After an Episode of Unprovoked Deep Vein Thrombosis: Short-Term Anticoagulation is Safe.
Background. The optimal duration of oral anticoagulant treatment in patients with idiopathic
Deep Vein Thrombosis (DVT)of the lower limbs is still uncertain. Residual Vein Thrombosis
(RVT) has been found able to establish the patient' risk for recurrent thrombotic events. In
the present study we conducted a RVT-based therapeutic strategy, withholding OAT after 3
months in patients without RVT while continuing anticoagulants for at least additional 9
months in those in whom RVT persists.
Methods Patients with a first episode of symptomatic unprovoked proximal Vein Thrombosis
(VT) were given Oral Anticoagulant Treatment (OAT) for 3 months. Residual Vein Thrombosis
(RVT), ultrasonographically-detected, will be then assessed. Patients without RVT did not
continue OAT (Group B), whereas those with RVT will continue OAT for at least additional 9
months. Patients were followed-up prospectively focusing on the study outcomes: occurrence
of recurrent venous thromboembolism and major bleeding over a period of at least 12 months
after OAT discontinuation.
INTRODUCTION Long-term anticoagulant treatment with adjusted doses of vitamin K antagonists
is highly effective in preventing recurrent events after a first episode of unprovoked
Venous ThromboEmbolism (VTE), even if the optimal duration of this therapy is still
uncertain. Since the risk of recurrency is greatest in the first year after the initial
thrombotic episode and gradually diminishes thereafter, the benefit of an extended course of
anticoagulant treatment may be offset over time by the persisting risk of clinically
important bleeding.
A potential clinically relevant approach for establishing the optimal duration of Oral
AntCoagulant Therapy (OAT) is that of predicting the individual risk for thrombotic
recurrency after the index Deep Vein Thrombosis (DVT). Although the current scheme for
establishing the duration of OAT is based on the nature of index DVT (idiopathic or
provoked), some new data starting to select other parameters to optimize this decision.
Recently, the use of D-dimer has been proven to be effective for selecting OAC duration;
however, this investigation evaluated only patients with idiopathic DVT and, moreover, the
use of D-dimer can not be easily handle by most of Institutions.
In earlier prospective studies conducted in patients with symptomatic DVT, the presence of a
residual thrombus was associated with an increased risk of thrombotic recurrencies either in
idiopathic or provoked venous thrombosis. Interestingly, recurrent events occurred not only
in the previously affected veins but also in other sites, thus suggesting that Residual Vein
Thrombosis (RVT) may express a pro-thrombotic status. Based on these findings, the detection
of RVT may be, therefore, of help in establishing the duration of anticoagulation. Recently,
we have conducted a randomized, prospective, follow-up study in patients with a first
episode of symptomatic DVT treated with OAT for 3 months in whom OAT duration was based upon
RVT findings. In patients without RVT, the risk of recurrent DVT was low even if the
treatment was stopped after only 3 months.
To further confirm our preliminary data and to enforce the safety of withholding OAT after 3
months in patients without RVT, we conducted a prospective study in patients with idiopathic
DVT of the lower limbs.
METHODS Study patients. Patients with a first episode of documented unprovoked and provoked
proximal DVT will be eligible for the study if they had completed at least three months of
OAT (target INR 2.5, range 2.0-3.0). Unprovoked DVTs are defined as thrombotic episodes
occurred in apparently healthy individuals. Patients with active cancer, limited life
expectancy, antiphospholipid antibody syndrome, or an other known thrombophilic status (such
as antithrombin deficiency), serious liver disease, those who lived too far from the center
will be excluded from the study. The study has been approved by the institutional review
boards of all participating centers. All enrolled patients will provide written informed
consent.
Study Design. This is a multicenter prospective study in patients with a first episode of
symptomatic proximal DVT detected by Compression UltraSonography (C-US) and receiving OAT
[warfarin (Coumadin, Bristol Myers Squibb) for 3 months. At this time, subjects who agreed
to participate have a physical examination to assess baseline clinical conditions and to
exclude contraindications. C-US of the proximal deep vein system in both legs will be
performed, measuring the diameters of any detectable thrombus in the Common Femoral Vein
(CFV) and Popliteal Veins (PV). Images will be obtained in transverse section only. Lumen
compressibility will be then evaluated on CFV and PV by gentle pressure of the probe, as
previously described. Briefly, the major and the minor diameters of the vein segment are
measured and recorded before and after compression. C-US findings are scored as "absence of
RVT" when residual thrombus occupied, at maximum compressibility, less than 40% of the vein
area. Patients without RVT will not continue anticoagulation (Group B), whereas those with
RVT will continue OAT (INR 2.0-3.0) for at least additional 9 months.
Study outcomes and Follow-up. From the assignment visit, patients will be followed up for at
least one year after OAT discontinuation; during the follow-up period, patients will be
contacted by the clinical centers every 3 months. C-US will be performed only when recurrent
symptomatic DVT is suspected. The study outcome is the composite of confirmed recurrent
venous thromboembolism (including DVT and/or fatal or non-fatal pulmonary embolism) and
major bleeding events from the index DVT to the last day of follow-up. In cases of suspected
DVT recurrence the results of ultrasonography will be compared with the previous
examination. A diagnosis of recurrent venous thrombosis is made if a previously fully
compressible segment (contralateral or ipsilateral) became incompressible. In absence of a
previous normal C-US, DVT recurrence is diagnosed if a previously non-occlusive thrombus
shifted to occlusive thrombus, provided the vein area before compression had increased > 4
mm); in undetermined cases, contrast venography was performed. In patients with suspected
pulmonary embolism, diagnosis of recurrence is based on objective algorithms using clinical
probability, ventilation-perfusion lung scanning/helical computed tomography, compression
ultrasonography and/or D-dimer if indicated. The diagnosis of clinically relevant
haemorrhage will be made in case of decrease of haemoglobin levels > 2.0 gr/dl,
retroperitoneal, intracranial or life-threatening. Patients has been instructed to contact
the clinical center immediately if symptoms developed suggestive of venous thromboembolism
or bleeding. All suspected outcome events and all deaths will be evaluated by a central
adjudication committee whose members were unaware of the name of the subject, the enrolling
center, the C-US findings and the assigned group.
Statistical analysis. Baseline differences between groups will be assessed by the chi-square
test (Yates' correction) for categorical variables and t-test or Mann-Withney U test for
continuous variables, as appropriate. Data will be analyzed on intention-to-treat basis.
Kaplan-Meier survival curves are plotted to estimate the cumulative incidence of symptomatic
recurrent venous thromboembolism and major bleeding. Patients who during the study will
develop clinical conditions interfering with the study outcomes (such as ischemic heart
disease, cancer, stroke, superficial vein thrombosis, etc) and left the assigned group will
be regularly followed-up and included in analysis. Hazard ratios and their 95 percent
confidence intervals will be calculated using the Cox's proportional hazards model. The data
will be analyzed using the Prism statistical software package (Version 3.0, GraphPad
Software Incorporated, San Diego, CA) and the SPSS statistical package (Version 14.0, SPSS
Inc., Chicago, IL).
;
Allocation: Non-Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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