RaDiCo-ACOSTILL - Adult and pediatric cohort with Still's disease (RaDiCo-ACOSTILL)

Head :
Georgin-Lavialle Sophie , UMRS 938
Fautrel Bruno, UMR S 1136

Last update : 03/21/2024 | Version : 1 | ID : 74149

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Métadonnées
Identification
General Aspects
Scientific investigator(s) (Contact)
Collaborations
Funding
Governance of the database
Additional contact
Type of database
Database objective
Population type
Dates
Size of the database
Data
Procedures
Promotion
Access
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General
Identification
Detailed name Adult and pediatric cohort with Still's disease (RaDiCo-ACOSTILL)
Sign or acronym RaDiCo-ACOSTILL
CNIL registration number, number and date of CPP agreement, AFSSAPS (French Health Products Safety Agency) authorisation N° CCTIRS 16-088bis / N° CPP 14128 ND / N° MESR DC-2015-2479 / MR-001
General Aspects
Medical area Internal medicine
Pediatrics
Rare diseases
Rheumatology
Study in connection with Covid-19 No
Pathology (details) Adult Still's disease (AOSD) and systemic onset juvenile idiopathic arthritis (SoJIA) represent two rare multifactorial diseases associated with systemic inflammation. These two forms, AOSD and SoJIA, are considered two facets of the same syndrome, combining four cardinal symptoms [high fever > 39°C, arthralgia or arthritis, skin rash, leukocyte formula with more than 80% neutrophil polymorphonuclear cells]; lymphadenopathy and splenomegaly may also be present; there is significant biological inflammatory syndrome with elevated C-reactive protein, serum ferritin with a dramatic decrease in glycosylated fraction. The incidence of the disease is low, around 0.1 / 100,000 for adults and 0.6 / 100,000 for children. Its prevalence is approximately 1 to 3/100,000 and 3/100,000 for children, so there are approximately 500 to 1500 adults and 450 children affected in France. It is subdivided into pediatric and adult forms according to the age of onset before or after 16 years. The prognosis of the disease is functional and vital. Macrophage activation syndrome (MAS) is frequently associated, either at the onset of the disease, at the initiation of treatment, or concomitant with viral reactivation. The evolution over time has mainly been studied in children and is variable: regression, episodic progression with regression over time, and chronic joint evolution. In adults, these three evolutionary modes can also be observed. However, differences seem to exist between AOSD and SoJIA.
Scientific investigator(s) (Contact)
Name of the director Georgin-Lavialle
Surname Sophie
Address Hôpital TENON, 4 rue de la Chine, 75020 PARIS.
Phone 0033(0) 1 56 01 60 77
Email sophie.georgin-lavialle@aphp.fr
Unit UMRS 938
Organization National Institute of Health and Medical Research (Inserm)
Name of the director Fautrel
Surname Bruno
Address Groupe Hospitalier Universitaire Pitié-Salpêtrière
83 boulevard de l'Hôpital, 75651 Paris cedex 13, France
Phone +33(0) 1 421 77801
Email bruno.fautrel@aphp.fr
Unit UMR S 1136
Organization National Institute of Health and Medical Research (Inserm)
Collaborations
Funding
Funding status Public
Details The RaDiCRaDiCo-ACOSTILL cohort initially received funding from the state managed by the National Research Agency (ANR) as part of the "Investissements d'Avenir" cohorts program (PIA).
Governance of the database
Sponsor(s) or organisation(s) responsible National Institute of Health and Medical Research (Inserm)
Organisation status Public
Presence of scientific or steering committees Yes
Labelling and database evaluation Security audit certification of the database. Data management and continuous quality control of data.
Additional contact
Main features
Type of database
Type of database Morbidity registers
Study databases (details) Cohort study
Database recruitment is carried out by an intermediary A selection of health institutions and services
Database recruitment is is made on the basis of: Another treatment or procedure
Database recruitment is carried out as part of an interventional study No
Additional information regarding sample selection. All pediatric and adult patients already diagnosed and followed (prevalent patients) or newly diagnosed (incident patients) in one of the French Reference Centers for Rare Diseases or Rare Disease Competence Centers will be invited to participate in the study. In order to document the improvement in patient management, morbidity, and mortality through the implementation of the Still's Disease National Diagnostic and Care Guidelines (PNDS Still), deceased patients may be included in the cohort. The objective is to recruit a minimum of 200 adult patients and 300 pediatric patients to ensure that the study has sufficient statistical power.
Database objective
Main objective The main objective is to describe the natural history of the disease in adult and pediatric populations.
Inclusion criteria The inclusion criteria for the RaDiCo-ACOSTILL cohort are as follows:

- Patients aged over 16 years (age >16 years) meeting the Yamaguchi diagnostic criteria or Fautrel criteria.
- Patients aged 16 years or younger (age ≤16 years) fulfilling the 2001 criteria for systemic onset juvenile idiopathic arthritis according to the ILAR classification.
- Having signed consent to participate in the cohort and for the collection of clinical and biological data; in accordance with regulations, for deceased minors or adults under legal protection, non-opposition from legal representatives will be sought.
- Affiliated with the social security system.

The exclusion criteria are:
- Other causes of recurrent infectious fever (such as tuberculosis, toxoplasmosis, deep abscesses, viral infections, sepsis) or tumor-related fever (such as lymphomas).
- Other defined inflammatory rheumatic diseases such as rheumatoid arthritis, psoriatic arthritis, spondyloarthropathies.
- Autoimmune inflammatory diseases (systemic lupus erythematosus), granulomatosis (sarcoidosis, Blau syndrome), vasculitis (Behçet's disease, polyarteritis nodosa), polymyositis, and dermatomyositis.
- Well-defined autoinflammatory syndromes with unambiguous mutations, such as familial Mediterranean fever, cryopyrinopathies, TRAPS, mevalonate kinase deficiency.
- Known genetic macrophage activation syndromes.
- Patients unable to understand the information leaflet and sign the informed consent form.
- Patients not affiliated with the social security system.
Population type
Age Newborns (birth to 28 days)
Infant (28 days to 2 years)
Early childhood (2 to 5 years)
Childhood (6 to 13 years)
Adolescence (13 to 18 years)
Adulthood (19 to 24 years)
Adulthood (25 to 44 years)
Adulthood (45 to 64 years)
Elderly (65 to 79 years)
Great age (80 years and more)
Population covered Sick population
Pathology M05-M14 - Inflammatory polyarthropathies
Gender Male
Woman
Geography area National
Data collection
Dates
Date of first collection (YYYY or MM/YYYY) 2017
Date of last collection (YYYY or MM/YYYY) 2027
Size of the database
Size of the database (number of individuals) < 500 individuals
Details of the number of individuals 422
Data
Database activity Current data collection
Type of data collected Clinical data
Declarative data
Paraclinical data
Biological data
Clinical data (detail) Direct physical measures
Medical registration
Details of collected clinical data The main variables collected are: demographics, family and medical history, socio-economic data, clinical and biological data, clinical signs, symptoms, specific disease treatments, and quality of life self-assessment questionnaires.
Declarative data (detail) Paper self-questionnaire
Internet self-questionnaire
Details of collected declarative data HAQ/CHAQ child and parent / SF 36 - SF10 (adult - child) / Psychological impact (Hamilton, adult) / Impact on work productivity and activity (WPAI, adult) / Perceived impact (PASS MCII, adult)
Paraclinical data (detail) Imaging data (standard radiographs of painful joints when performed)
Biological data (detail) Biochemical, hematological, and immunological data
Presence of a biobank Yes
Contents of biobank Whole blood
Plasma
DNA
Details of biobank content This study includes a collection of biological samples conducted as part of research for future studies (DNA, RNA, plasma, peripheral blood mononuclear cells).
Health parameters studied Health event/morbidity
Health event/mortality
Health care consumption and services
Quality of life/health perception
Others
Care consumption (detail) Hospitalization
Medical/paramedical consultation
Medicines consumption
Procedures
Data collection method eCRF in secure web access, secure cloud and HADS hosting
Classifications used Drug Dictionary (DCIs)
Quality procedure(s) used Data Management Plan and Data Validation Plan. Continuous data management (automatic control rules and query system)
Participant monitoring Yes
Monitoring procedures Monitoring by convocation of the participant
Monitoring by contact with the referring doctor
Links to administrative sources No
Promotion and access
Promotion
Access
Presence of document that lists variables and coding procedures Yes
Terms of data access (charter for data provision, format of data, availability delay) Requests for access to RaDiCo-ACOSTILL data (aggregated or individual) will be reviewed by the Scientific Committee following the submission of a summary of a Specific Research Project, as defined in the Access Charter. Requests should be sent to the following address: acostill@radico.fr
Access to aggregated data Access on specific project only
Access to individual data Access on specific project only

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