The goal of the CRETE Studies is to investigate the newly identified age-dependent heterogeneity in the efficacy of enoxaparin in reducing the risk of central venous catheter-associated deep venous thrombosis in critically ill children.
Pediatric venous thromboembolism (VTE), which is predominantly deep venous thrombosis (DVT), is a top contributor to harm in hospitalized children. Its incidence increased by \>300% in the past 2 decades. Critical illness and central venous catheter (CVC) are the most important risk factors for VTE in children. Among critically ill children, the risk of CVC-associated DVT (CADVT) is as high as 54% with 72% of cases in infants \<1-year old. Pharmacologic prophylaxis is the most effective strategy against VTE in adults. However, due to paucity of age-appropriate evidence on its efficacy against CADVT, pharmacologic prophylaxis is uncommon in children. Extrapolation of evidence from adults is not appropriate because the hemostatic system changes significantly with age. The investigators recently completed a Bayesian phase 2b randomized clinical trial. In this trial, the investigators randomized critically ill children to early administration of prophylactic dose of enoxaparin, the most commonly used anticoagulant for prophylaxis, or usual care. Prophylaxis with enoxaparin appeared to reduce the risk of CADVT by half. In post hoc analyses, reduction was limited to older children 1-17 years old. The goal of the CRETE Studies is to investigate this newly identified age-dependent heterogeneity in the efficacy of enoxaparin in reducing the risk of CADVT in critically ill children. To achieve this goal, the investigators aim (1) to confirm the efficacy and safety of early administration of prophylactic dose of enoxaparin in reducing the risk of CADVT in critically ill older children; (2) to determine the efficacy and safety of early administration of therapeutic dose of enoxaparin in reducing the risk of CADVT in critically ill infants; and, (3) to probe the mechanisms that underly the age-dependent heterogeneity in the efficacy of enoxaparin in reducing the risk of CADVT in critically ill children. The investigators will conduct 2 multicenter Bayesian explanatory randomized clinical trials in parallel to address Specific Aims 1 and 2. Depending on age, subjects will be randomized to different doses of enoxaparin vs usual care. Subjects will be systematically assessed for the development of CADVT using ultrasonography and clinically for bleeding. Using plasma obtained from subjects in the 2 trials, the investigators will conduct an exploratory mechanistic nested case-control study to address Specific Aim 3. Biomarkers of selected mechanisms underlying CVC-associated thrombus formation, particularly thrombin generation, will be compared between subjects with and without CADVT. The investigators will use Bayesian methods to improve the efficiency in the conduct and analyses of these studies. The CRETE Studies will provide high-quality age-appropriate evidence that will inform preventive strategies against CADVT and decrease harm in hospitalized children.
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
PREVENTION
Masking
SINGLE
Enrollment
258
Enoxaparin is a LMWH produced from UFH that exerts its anticoagulant effects by binding to and inducing a conformational change in antithrombin to accelerate the inactivation of factor Xa and thrombin. Age-specified dose of enoxaparin will be administered within 24 hours after insertion of the CVC with the dose subsequently adjusted to pre-specified anti-Xa target.
Children's of Alabama
Birmingham, Alabama, United States
Number of children with CADVT
Thrombus in the central vein where the CVC was inserted that is diagnosed with systematic ultrasonographic surveillance.
Time frame: Up to removal of CVC (maximum of 28 days)
Number of children with any VTE
Thrombus in the deep vein of any extremity or PE that is confirmed radiologically
Time frame: Up to removal of CVC (maximum of 28 days)
Number of children with clinically apparent CADVT
Any CADVT, except one that is only diagnosed with the systematic ultrasonographic surveillance.
Time frame: Up to removal of CVC (maximum of 28 days)
Number of children with clinically apparent VTE
Any VTE, except one that is only diagnosed with the systematic ultrasonographic surveillance.
Time frame: Up to removal of CVC (maximum of 28 days)
Number of children with clinically relevant bleeding
Bleeding that is fatal, with drop in hemoglobin by ≥2 g/dl in 24 hours, requires medical or surgical intervention to restore hemostasis, or in the retroperitoneum, pulmonary or central nervous system.
Time frame: Maximum of 36 hours after the last dose of enoxaparin
Number of children with any bleeding
Any overt or macroscopic evidence of bleeding.
Time frame: Maximum of 36 hours after the last dose of enoxaparin
Number of children with heparin-induced thrombocytopenia
Unexplained drop in platelet count to \<50 x 10\^3/mcL or by 50 percent of baseline platelet count in the ICU within 21 days following exposure to heparin, and with a positive anti-platelet factor 4 antibody.
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Arkansas Children's Hospital
Little Rock, Arkansas, United States
RECRUITINGChildren's Hospital Colorado
Aurora, Colorado, United States
RECRUITINGYale-New Haven Children's Hospital
New Haven, Connecticut, United States
RECRUITINGUniversity of Florida -UF Health
Gainesville, Florida, United States
RECRUITINGJohns Hopkins All Children's
St. Petersburg, Florida, United States
RECRUITINGChildren's Hospital of Illinois at OSF Saint Francis Medical Center
Peoria, Illinois, United States
RECRUITINGStead Family Children's Hospital
Iowa City, Iowa, United States
RECRUITINGChildren's Hospital St. Louis
St Louis, Missouri, United States
RECRUITINGHassenfeld Children's Hospital
New York, New York, United States
RECRUITING...and 12 more locations
Time frame: Maximum of 36 hours after the last dose of enoxaparin