PROFILE is a cohort study evaluating the progression of fibromuscular dysplasia lesions. This study is the prospective dimension of ARCADIA registry (ClinicalTrials.gov Identifier: NCT02884141), which aims to document phenotypic and genetic traits in patients with renal and/or cervical artery fibromuscular dysplasia.
Background Fibromuscular dysplasia (FMD) is a group of nonatherosclerotic, noninflammatory arterial diseases that usually involve renal and carotid arteries. Patients with FMD may present with renovascular hypertension and/or with cerebrovascular symptoms. The prevalence of FMD in hypertensive patients is estimated at 4/1000. Angiographic classification includes the multifocal type, with multiple stenoses and the 'string-of-beads' appearance that is related to medial FMD, and tubular and focal types which are not clearly related to specific histological lesions. FMD may affect one or more vascular beds and progress to more severe stenosis and to renal or cerebrovascular complications. FMD appears to be familial in 10% of cases (OMIM #135580). Renal artery FMD may progress to more severe stenosis and to renal atrophy, and/or to stenoses affecting more arteries within or outside the renal vasculature. The risk of progression as assessed from available studies was probably overestimated because documentation of progression was obtained from angiography, a procedure which is not routinely undertaken in patients with favourable clinical and biological outcomes. The disease is progressive, however, and literature stated that patients with FMD should undergo yearly duplex ultrasonography to detect progression of disease, restenosis, or loss of kidney volume. There are very few data on prognosis of patients with symptomatic carotid or vertebral artery FMD. The risk of arterial disease progression over time is unknown. The risk of ischemic stroke ranged from 0 to about 3% per year in the few studies which assessed that issue. Objectives The primary objective is to estimate the incidence and risk factors for progression of FMD lesions. This will be assessed by comparison between initial and 3 years abdominal and supra-aortic trunks vascular imaging (angiography, CT-angiography or Magnetic Resonance (MR) angiography), monitoring of downstream consequences development of lesions progression and clinical events. The secondary objectives are: * to estimate rate of genetic polymorphism that may influence disease progression or be associated with complications * to assess the frequency of multi-site FMD (common objective with the ARCADIA study) * to collect standardized clinical, radiological, and biological data in patients with FMD through a national registry (common objective with the ARCADIA study) * to organize a clinical, radiological and biological database and a biobank that will constitute a unique resource to initiate further clinical research (common objective with the ARCADIA study).
Study Type
INTERVENTIONAL
Allocation
NA
Purpose
DIAGNOSTIC
Masking
NONE
Enrollment
340
Abdominal and supra-aortic trunks vascular imaging (angiography, CT-angiography or MR-angiography) will be performed 3 years after inclusion. This imaging will be compare to initial imaging (which is a part of usual care, not an intervention added by the study) in order to assess FMD progression.
A sample of blood will be taken to meet the objective of estimating the rate of genetic polymorphism that may influence disease progression or be associated with complications.
A sample of blood will be taken to biomarkers analysis to meet the primary objective of assessing the risk factors for progression of FMD lesions.
Cliniques universitaires Saint-Luc
Brussels, Brussels Capital, Belgium
CHU de Bordeaux hopital Saint-Andre
Bordeaux, Aquitaine-Limousin-Poitou-Charentes, France
Progression of fibromuscular dysplasia lesions confirmed by imaging
Time frame: 3 years
Glomerular filtration rate (GFR)
Time frame: Inclusion, 3 years
Kidney height
Time frame: Inclusion, 3 years
Clinical event: revascularization procedure in a lesion site
Time frame: Through study completion
Clinical event: renal infarction
Time frame: Through study completion
Clinical event: ischemic stroke
Time frame: Through study completion
Clinical event: arterial dissection in a lesion site or downstream from a lesion site
Time frame: Through study completion
Clinical event: aneurysm rupture in a lesion site or downstream from a lesion site
Time frame: Through study completion
Prevalence of multisite fibromuscular dysplasia confirmed by imaging
Time frame: Inclusion, 3 years
Single nucleotide polymorphisms
Assessed by genome-wide association
Time frame: Inclusion
Plasminogen/plasmin level
Time frame: Inclusion
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A sample of urine will be taken to biomarkers analysis to meet the primary objective of assessing the risk factors for progression of FMD lesions.
CHU de Clermont-Ferrand hopital Gabriel-Montpied
Clermont-Ferrand, Auvergne-Rhône-Alpes, France
CHU de Grenoble hopital Albert-Michallon
La Tronche, Auvergne-Rhône-Alpes, France
CHU de Nancy institut Louis-Mathieu
Vandeuvre-les-Nancy, Grand Est, France
CHRU de Lille hopital cardiologique
Lille, Hauts-de-France, France
CHRU de Lille hopital Roger-Salengro
Lille, Hauts-de-France, France
CHU de Caen hopital Cote de Nacre
Caen, Normandy, France
CHU de Toulouse hopital Rangueil
Toulouse, Occitanie, France
AP-HM hopital de la Timone
Marseille, Provence-Alpes-Côte d'Azur Region, France
...and 7 more locations
Matrix metalloproteinases level
Time frame: Inclusion