Informations générales (source: ClinicalTrials.gov)
A Randomized Phase III Multicenter Trial Comparing the Efficacy and Safety of Anakinra Versus Intravenous Immunoglobulin (IVIG) Retreatment, in Patients With Kawasaki Disease Who Failed to Respond to Initial Standard IVIG Treatment (ANACOMP)
Interventional
Phase 3
Assistance Publique - Hôpitaux de Paris (Voir sur ClinicalTrials)
octobre 2023
mars 2027
29 juin 2024
Kawasaki disease (KD) is the most frequent vasculitis in younger children <5years, and
the first cause of acquired ischemic myocardiopathy in childhood. Exceptionally, KD may
cause early death during the acute phase by myocardial infarction, but may compromise the
long-term cardiovascular outcome by accelerating atherosclerotic disease.
The incidence of KD is high in far-Eastern countries and Hawaii but KD is relatively rare
in other regions (10/100000 children <5years in northern Europe) which makes it difficult
to develop research on these rare population.
Early recognition and treatment by intravenous immunoglobulins (IVIG) influences the
prognosis positively. IVIG are the standard of care and decrease significantly the risk
of coronary aneurysms. However, despite a first infusion of IVIG, 20% of KD patients
remain febrile and have high risk of coronary vasculitis. Recent Japanese research group
assessed additional cyclosporine treatment in first line KD treatment but failed
preventing relapse. To date there is no agreement for a more effective second line
treatment.
Based on the auto-inflammatory pattern of KD, the investigators hypothesize that anti
IL-1 blocking agents could bring a rapid and sustained effect on systemic and coronary
inflammation in patients with KD.
Our hypotheses are:
1. Anakinra treatment may reduce the early and long-term mortality of patients with
Kawasaki Disease (KD), by a rapid and sustained effect on vascular inflammation.
2. The safety of anakinra is good, as the drug has a very short half-life, which allows
its rapid withdrawal in case of serious adverse event.
The use of anakinra is not associated with the risk of contamination by infectious
agents, which remain even minimal, a possibility with the use of IVIG.
Etablissements
| Les établissements d'Île-de-France ayant mis à jour leurs données Origine et niveau de fiabilité des données | |||||
|---|---|---|---|---|---|
| AP-HP - Hôpital Bicêtre | KONE PAUT Isabelle | 02/12/2024 12:47:04 | Contacter | ||
| AP-HP - Hôpital Jean Verdier | KONE PAUT Isabelle | 02/12/2024 12:47:04 | Contacter | ||
| AP-HP - Hôpital Louis Mourier | KONE PAUT Isabelle | 02/12/2024 12:47:04 | Contacter | ||
| AP-HP - Hôpital Necker-Enfants Malades | KONE PAUT Isabelle | 02/12/2024 12:47:04 | Contacter | ||
| AP-HP - Hôpital Robert Debré | KONE PAUT Isabelle | 02/12/2024 12:47:04 | Contacter | ||
| CHI DE CRETEIL | Fouad MADHI | 11/02/2025 10:14:07 | Contacter | ||
| Les établissements sans correspondance certaine dans le répertoire FINESS dont les données sont issues de ClinicalTrials.gov Origine et niveau de fiabilité des données | |||||
| CHU de Bicêtre - 94270 - Le Kremlin-Bicêtre - Val De Marne - France | Isabelle KONE-PAUT, Pr | Contact (sur clinicalTrials) | |||
Critères
Tous
Inclusion Criteria:
- Children, male and female, from 3 months to <18 years old
- Patient ≥ 5 kg
- Patient with KD according to the American Heart Association definition for complete
or incomplete KD. (Fever ≥ 5 days (or at least 3 days if KD with American Heart
Association criteria since the third days of fever) and ≥ 4 of 5 main clinical
signs: modification of the extremities, polymorphic exanthema, and bilateral bulbar
not exudative conjunctivitis, erythema of the lips or oral cavity, and cervical
lymph nodes usually unilateral > 1.5 cm in diameter.
- Patients who failed to respond to the standard therapy of KD, e.g. Persistence or
recrudescence of fever ≥ 38°C, 48 hours after the infusion of 2g/kg of IV Ig.
Patients may be screened 24h after the end of the first infusion if they remain
febrile 24h after the end of the first infusion.
- Patient, parents or legal guardian's written informed consent is required
- Patient with health insurance (SS or CMU).
- Efficient contraception for the duration of participation in the research for
childbearing aged women
- Children, male and female, from 3 months to <18 years old
- Patient ≥ 5 kg
- Patient with KD according to the American Heart Association definition for complete
or incomplete KD. (Fever ≥ 5 days (or at least 3 days if KD with American Heart
Association criteria since the third days of fever) and ≥ 4 of 5 main clinical
signs: modification of the extremities, polymorphic exanthema, and bilateral bulbar
not exudative conjunctivitis, erythema of the lips or oral cavity, and cervical
lymph nodes usually unilateral > 1.5 cm in diameter.
- Patients who failed to respond to the standard therapy of KD, e.g. Persistence or
recrudescence of fever ≥ 38°C, 48 hours after the infusion of 2g/kg of IV Ig.
Patients may be screened 24h after the end of the first infusion if they remain
febrile 24h after the end of the first infusion.
- Patient, parents or legal guardian's written informed consent is required
- Patient with health insurance (SS or CMU).
- Efficient contraception for the duration of participation in the research for
childbearing aged women
- Preterm and neonates, pregnancy, pregnancy and breast feeding
- Suspicion of another diagnosis
- Patient with overt concomitant bacterial, viral or fungal infection
- Patient previously treated with steroids and/or another biotherapy
- Patient with increased risk of tuberculosis infection
- Recent tuberculosis infection or with active tuberculosis
- Patient with any type of immunodeficiency or cancer
- Patients with severe renal impairment (CLcr < 30 ml/minute)
- Patients with hepatic insufficiency
- Patients with neutropenia (ANC<1.5 x109/l)
- Patients included in another interventional protocol
- Patient under the following treatments:
- Preventive Antipyretics (paracetamol, NSAIDs other than aspirin 30-50mg/kg given for
purpose of KD inflammation), as long as the patient receives the study medication
- Immunosuppressive medications given in a period less than twice of their half-life
prior the patient receives the study medication (systemic steroids, cyclosporine,
tacrolimus, azathioprine, cyclophosphamide, interferon, mycophenolate, other
anti-IL-1, anti IL-6, anti CD20 and anti TNF (Tumor Necrosis Factor)),
plasmapheresis)
- Hypersensitivity to anakinra or excipients (citric acid, sodium chloride, disodium
EDTA (Ethylene Diamine Tetra Acetic), polysorbate 80, sodium hydroxide, in water for
injection)
- Hypersensitivity to IV Ig, or excipients (L-proline and water for injection),
hypersensitivity to human normal immunoglobulin, in particular if the patient have
anti-IgA antibodies (IgA: Immunoglobulin A)
- Patients with type I or II hyperprolinemia
- Live vaccines within 1 month prior to enrollment
- Hypersensitivity to anakinra or to immunoglobulins or to excipients of Kineret® or
Privigen® or to E.coli proteins
- Contraindication for administration of anakinra or IVIG listed in the Summary of
Products Characteristics (SmPC) of Kineret® and Privigen®
- Ongoing or recent use of any other medication Known inhibitors/inducers of
cytochrome P450 as listed on the link below:
http://medicine.iupui.edu/clinpharm/ddis/main-table