Dose-adjustment of Enoxaparin by a Bayesian Pharmacological Approach in Pediatric Kidney Transplant Recipients (OPTI-TREX)

Phase 4RecruitingNCT05672550

Assistance Publique - Hôpitaux de Paris50 enrolled

Overview

Allograft vascular thrombosis is a devastating complication in kidney transplantation in adults and older children. Though uncommon, it is often irreversible and represents the main cause of graft loss within after kidney transplantation in adults and in the first post-operative year in children. Since allograft thrombosis is usually observed in the first 48h post-operatively, the need to promptly achieve appropriate anticoagulation in at-risk patients is of utmost importance. However, no consensus exists regarding the optimal prophylaxis in the peri-transplant period and the following dose-adjustment, and practices are highly heterogeneous among centers. Moreover, the therapeutic target is very narrow and antithrombotic agents may conversely increase the risk of allograft hematoma. Enoxaparin is a low molecular weight heparin commonly used in this context, but off-label in children. Therapeutic ranges are based on anti-Xa levels 4 to 6 hours following injection and extrapolated from adults although evidences suggest that such extrapolation may be inappropriate in many circumstances. The current pediatric practice of dose adjustment to achieve and maintain a target anti-Xa range is empirical and dependent on the physician. The aim of the proposed clinical trial is to assess the efficacy/safety profile of this bayesian-based dose optimization in the clinical setting, as compared to the current practices of empirical adjustment. This should greatly improve the personalized management of renal transplanted children, a subset of patients with singular renal function and little-investigated pharmacokinetics and help standardizing and rationalizing practices.

The investigators will compare the efficacy of the Bayesian based dose versus the dose determined in a usual empirical way based on each physician's experience. The primary endpoint is the Anti-Xa activity within the target range 28 to 30 hours after initiation of the treatment. This is an open labelled randomized clinical trial. The randomization will proceed during the inclusion visit by the local pediatric nephrologist or intensivist just before the first enoxaparin injection, administered within 24 hours post-transplantation. The investigators will conduct a national multicentric study with 9 inclusion centers which are all nephrology units specialized in renal transplantation.

Study Type

INTERVENTIONAL

Allocation

RANDOMIZED

Interventions

Bayesian based dose adjustment of enoxaparinDRUG

A first recommended dose of enoxaparin 50 IU/kg subcutaneously is administered during transplantation or within the first 24 hours. Then a Bayesian estimate of individual pharmacokinetics is performed to adapt the next twice daily (Hour 12;Hour 24) enoxaparin dose until achievement of the target on two consecutive measurements. Then anti-Xa activity will be evaluated once a day until day 7.

Usual dose adjustment of enoxaparinDRUG

A first recommended dose of enoxaparin 50 IU/kg is administered during transplantation or within the first 24 hours. Then anti-Xa activity is measured and twice-daily (hour 12 ; hour 24) enoxaparin empirical dose-adjustment is performed according to the usual practices in the investigating centers to target.

Eligibility

Sex: ALLMin age: 2 YearsMax age: 20 Years

Medical Language ↔ Plain English

Inclusion Criteria: 1. Pediatric renal transplant recipients 2. Aged ≥ 2 years and ≤18 years 3. With an indication for enoxaparin treatment in the first post-transplant week according to the local transplant team such as inherited or acquired thrombotic disorders (eg. but not exclusive protein C, protein S, and antithrombin III deficiency; factor V Leiden mutation (FV506Q), prothrombin mutation (G20210A), mutation in the MTHFR (methyl Tetra hydro folate reductase) gene (C677T), and antiphospholipid antibodies (anticardiolipin antibodies and lupus anticoagulants), history of thrombosis, donor age \< 2 years, recipient age \< 5 years, cold ischemia time \>24h, multiple renal vessels. 4. Informed consent form signed by the legal guardian(s) 5. Affiliated to a health insurance system, including AME Exclusion Criteria 1. Per-transplant technical surgical problems 2. Pre-inclusion allograft thrombosis (before randomization and enoxaparin administration) 3. Peri-operative thrombosis or uncontrolled bleeding (before randomization and enoxaparin administration) 4. Peri-operative hemodynamic instability 5. Medical history of heparin-induced thrombocytopenia 6. Allergic reaction to enoxaparin or excipients 7. Pregnancy 8. LMWH (Low molecular weight heparins) prophylactic before transplant 9. UFH (unfractionated heparin) treatment during renal transplantation with an anti-Xa level detectable 4-6h post administration

Locations (18)

Hôpital Pellegrin

Bordeaux, France

RECRUITING

Hôpital Pellegrin

Bordeaux, France

NOT_YET_RECRUITING

CHU Félix Guyon

La Réunion, France

RECRUITING

CHU Félix Guyon

La Réunion, France

NOT_YET_RECRUITING

Hôpital Mère Enfant

Lyon, France

RECRUITING

Hôpital Mère Enfant

Lyon, France

NOT_YET_RECRUITING

Hôpital de la Villeneuve

Montpellier, France

RECRUITING

Hôpital de la Villeneuve

Montpellier, France

NOT_YET_RECRUITING

Hôtel Dieu

Nantes, France

RECRUITING

Hôtel Dieu

Nantes, France

NOT_YET_RECRUITING

...and 8 more locations

Outcomes

Primary Outcomes

Anti-Xa activity within the target range

Anti-Xa activity within the target range (i.e., success defined by an anti-Xa activity ≥0.3 IU/mL and ≤0.5 IU/mL).