The CADRE study is a multinational observational cohort of patients with sickle-cell disease (SCD) in five west and central sub-Saharan African countries. The aim of this project is to describe the incidence and assess the predictive factors of SCD-related micro- and macro-vascular complications in sub-Saharan Africa.
Sickle cell disease (SCD), one of the lost common genetic diseases worldwide, is caused by a mutation in the β globin gene. Most patients with this disease are homozygous for the βS allele (SS), whereas others have inherited a βS allele with another mutation in the β globin gene. In addition to repeated acute ischemic insults due to the red blood cells sickling in the microcirculation, a chronic vasculopathy leads to organ injuries, such as kidney disease, stroke, pulmonary hypertension, retinopathy, bone infarcts, and leg ulcers. CADRE is a multinational prospective observational study undertaken in five countries in sub-Saharan Africa. Patients with SCD will be recruited through outpatients' clinics in public, university and private hospitals and research centers in five countries. The CADRE protocol was approved by the relevant national ethics committee in each of the participating countries. Primary endpoint is to measure the prevalence and the incidence of the main vascular complications in the main types of SCD: glomerulopathy, nephropathy, cardiopathy, pulmonary hypertension, retinopathy, strokes, osteonecrosis and leg ulcers. Secondary endpoints are: * to define the clinical and biological predictors of SCD vasculopathy in Africa * to search for genetic risk factors for the SCD-related cardiovascular complications, in particular alpha thalassemia, persistence of foetal hemoglobin and other candidate genetic polymorphisms * to search for functional risk factors (pulse wave velocity, capillary vasodilatation, blood visosity) for the SCD-related cardiovascular complications * to search for new biological determinant of SCD-related cardiovascular complications, in particular alternative markers of hemolysis (microparticules, free heme) and inflammation (cytokines, leucocytes phenotyping, NET (neutrophile extracellular traps))
Study Type
OBSERVATIONAL
Enrollment
4,500
Central Hospital of Yaounde
Yaoundé, Cameroon
RECRUITINGCentre mère et enfant / fondation Chantal Biya
Yaoundé, Cameroon
Prevalence and 10 year-incidence of SCD-related vascular complications in different phenotypes of SCD: glomerulopathy
urinary albumin/creatinin ratio (mg/g)
Time frame: 10 years
Prevalence and 10 year-incidence of SCD-related vascular complications in different phenotypes of SCD: cardiopathy
left ventricular ejection fraction \< 60 %
Time frame: 10 years
Prevalence and 10 year-incidence of SCD-related vascular complications in different phenotypes of SCD: pulmonary hypertension
tricuspid regurgitation jet velocity (m/s)
Time frame: 10 years
Prevalence and incidence and the 10 year-incidence of the main SCD-related vascular complications in different phenotypes of SCD: retinopathy
retinal examination
Time frame: 10 years
Prevalence and 10 year-incidence of SCD-related vascular complications in different phenotypes of SCD:stroke
clinical diagnosis
Time frame: 10 years
Prevalence and 10 year-incidence of SCD-related vascular complications in different phenotypes of SCD:osteonecrosis
standard radiography
Time frame: 10 years
Prevalence and 10 year-incidence of SCD-related vascular complications in different phenotypes of SCD: leg ulcers
clinical diagnosis
Time frame: 10 years
Prevalence and 10 year-incidence of SCD-related vascular complications in different phenotypes of SCD: priapism
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Centre Pasteur du Cameroun
Yaoundé, Cameroon
RECRUITINGPediatrics unit, Centre Hospitalier d'Essos
Yaoundé, Cameroon
RECRUITINGHematology Unit, CHU Yopougon
Abidjan, Côte d’Ivoire
RECRUITINGInstitut de cardiologie
Abidjan, Côte d’Ivoire
ACTIVE_NOT_RECRUITINGCentre hospitalier Monkole
Kinshasa, Democratic Republic of the Congo
RECRUITINGCIRMF
Libreville, Gabon
COMPLETEDCardiology Unit, Centre gyneco-obstretrique
Bamako, Mali
ACTIVE_NOT_RECRUITINGCentre de Recherche et de Lutte contre la Drepanocytose
Bamako, Mali
RECRUITING...and 3 more locations
clinical diagnosis
Time frame: 10 years
Potential biological risk marker measured at baseline and follow up visits: carotid-femoral pulse wave velocity
measured by Pulsepen, m/s)
Time frame: 10 years
Potential biological risk marker measured at baseline and follow up visits: complete blood count
Time frame: 10 years
Potential biological risk marker measured at baseline and follow up visits: LDH level
Time frame: 10 years
Potential biological risk marker measured at baseline and follow up visits: bilirubin level
Time frame: 10 years
Potential biological risk marker measured at baseline and follow up visits: microparticules measure
Time frame: 10 years
Potential biological risk marker measured at baseline and follow up visits: free heme level
Time frame: 10 years
Potential biological risk marker measured at baseline and follow up visits: inflammatory cytokines
Time frame: 10 years
Potential biological risk marker measured at baseline and follow up visits: neutrophil extracellular traps
Time frame: 10 years