Neoplasms Clinical Trial
Official title:
Anti Xa Activity in Cancer Patients Receiving Low-molecular-weight Heparin for Venous Thromboembolism
Low molecular weight heparins (LMWH) are the reference molecule for the long term treatment of venous thromboembolism (VTE) in cancer patients but remains, however, associated with a high risk of recurrent thromboembolism. The high rate of recurrence may result from alterations in the pharmacokinetics of LMWH. The primary purpose of the study is to compare the pharmacokinetics of anti-Xa activity in patients with cancer and patients without cancer treated with curative dose of low molecular weight heparins (LMWH) for venous thromboembolism (VTE). The secondary purposes are 1/ to study the correlation between anti-Xa LMWH and concentration of plasma heparanase and 2/ to evaluate the predictive nature of the anti-Xa activity on the occurrence of thromboembolic recurrence in cancer patients treated with LMWH for VTE.
Purpose of the study:
The primary purpose of the study is to compare the pharmacokinetics of anti-Xa activity in
patients with cancer and patients without cancer treated with curative dose of low molecular
weight heparins (LMWH) for venous thromboembolism (VTE).
The secondary purposes are 1/ to study the correlation between anti-Xa LMWH and concentration
of plasma heparanase and 2/ to evaluate the predictive nature of the anti-Xa activity on the
occurrence of thromboembolic recurrence in cancer patients treated with LMWH for VTE.
Study design:
Multicentre cohort study of patients hospitalized with VTE:
1. Observational case-control study to compare the pharmacodynamics of anti-Xa activity
between patients cancer patients (n = 50) and non-cancer patients (n = 50) matched (1-1)
for age, renal function and LMWH
2. A prospective cohort study including 320 cancer patients with a 6 months follow-up.
Study hypothesis:
Venous thrombosis and pulmonary embolism are a common complication of cancer. They complicate
up to 10% of cancers and are the cause of fatality, morbidity and significant impaired
quality of life. The treatment of these diseases is difficult in this context. Low molecular
weight heparins (LMWH) are the reference molecule for the long term treatment of venous
thromboembolism (VTE) in cancer patients. Outside this context, their pharmacological
properties allow to administer a fixed dose without measuring anti-Xa activity. In the
presence of cancer, their use remains, however, associated with a high risk of recurrent
thromboembolism up to 9% after 6 months of treatment.
This high rate of recurrence may result from alterations in the pharmacokinetics of LMWH in
the presence of a cancer. The synthesis of heparanase by tumor cells might cause a decrease
in anti-Xa activity of LMWH and reduce their effectiveness. If this hypothesis is verified,
it could result in a change in the management of thrombosis in cancer patients and lead to a
dose adjustment of LMWH through the measurement of anti-Xa activity, which may allow reduce
the incidence of thromboembolic relapses during treatment.
Enrollment (Target or Actual Number of Subjects):
1. Pharmacokinetics study In a preliminary unpublished study of 37 cancer and non-cancer
subjects with the highest concentration of anti-Xa activity was measured. Included 100
subjects (50 cancer patients and 50 non-cancer) would detect a maximum level difference
of anti-Xa activity in plasma of 0.20 between cancer patients and cancer-with a power of
90% and a risk of the first kind 5%.
A difference of 0.20 seems relevant from these preliminary data (median 0.46 vs 0.65),
and returns to show that a cancer patient has over 70% chance of having a maximum
concentration of anti-Xa activity below that of a free cancer patient (nonparametric
Wilcoxon test).
2. Cohort study (cancer patients) The risk of recurrent thromboembolism was estimated
between 5 and 10% in cancer patients. By including 200 subjects, around twenty events
would be observed and corresponds to a reasonable number of subjects can be recruited
over 18 months (50 would already enroll in the pharmacodynamic study). The event rate
will be assessed on the first 100 patients that will have been followed for 6 months, if
event rate is lower than expected, the number of participants will be reassessed.
After over 2 years of inclusion, the event rate is lower than expected (7%). The number of
subjects required was therefore reassessed. To reach the number of 20 events necessary to our
analysis, a total of 320 cancer subjects must therefore be included.
Target Follow-Up, duration :
Study duration: 5 years and 6 months (inclusion: 5 years follow-up: 6 months). Duration of
participation: 3 a 10 days for non-cancer patients, 6 months for cancer patient.
Performance of the study:
1. Pharmacokinetics study Inclusion (as soon as the diagnosis is confirmed VTE): 1 tube of
blood taken before the start of treatment (at the time of another blood sample) for
determination of heparanase. After the start of treatment: 3 tubes of blood drawn for
determination of anti-Xa activity.
Assays will be centrally performed, blinded from the clinical data and from the group
knowledge of the group patient.
2. Prospective cohort study of cancer patients Followed for 6 months with consultation at
1, 3, and 6 months (normal monitoring).
Follow-up visits: Collection of clinical data (recurrent thromboembolism, hemorrhage, death,
tumor progression, cancer treatment since last visit, interruption of treatment with LMWH,
thrombocytopenia, anemia), and removal of 1 tube of blood (at the time of a another sample)
for determination of anti-Xa activity.
Thromboembolic recurrences will be validated centrally by an independent committee.
Prospects:
Reduce the incidence of thromboembolic recurrence in cancer patients treated with LMWH for
VTE by adapting the dose of LMWH with anti-Xa activity in this population if the hypothesis
is verified.
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