The aim of the study is to assess the diagnostic sensitivity of MRI to detect changes in Helbich-Bhalla scoring over time in patients with cystic fibrosis
Cystic fibrosis (CF) is caused by the cystic fibrosis transmembrane conductance regulator (CFTR) gene mutation and represents one of the most frequent and lethal inherited disease in Caucasian. However, thanks to better treatments that slow down the progression of pulmonary disease, the median life expectancy has reached 41 years and there are nowadays more CF patients older than 18-year-old than younger. Chronic lung disease is the main manifestation and represents more than 90% of CF morbidity and mortality. However, there is a need for biomarkers more sensitive than clinical and functional findings for a personalized management of patients. Computed tomography (CT), owing to its high spatial resolution and contrast, is the standard of reference in imaging for depicting lung structural alterations. But CT is an ionizing technique, rising concern in cancer risk associated to cumulated radiation dose. To date, Magnetic Resonance Imaging (MRI) is a radiation-free technique which has been demonstrated to add meaningful functional information that cannot be reached using CT. Recent advances in 3-dimensional ultra-short echo time (3D-UTE) imaging have been shown promising to improve lung MR imaging quality. A clear delineation between airway wall and lumen was obtained, thanks to submillimeter voxel size, enabling readers to estimate both bronchial thickening and dilatation with very good concordance with CT, independently from the magnitude of score. The combination of pulse sequence may rather benefit from the potential of MRI to get more complete insight into inflammatory processes by combining several contrasts, as compared to other ionizing methods. Novel MR methods have been shown promising in assessing lung changes with high resolution and therefore could be proposed instead of CT for radiation- free repeated, life-long follow-up
Study Type
INTERVENTIONAL
Allocation
NA
Purpose
PREVENTION
Masking
NONE
Enrollment
212
lung MRI without contrast injection
University Hospital of Bordeaux
Bordeaux, France
University Hospital of Bordeaux
Bordeaux, France
Hôpital Henri Mondor
Créteil, France
CHRU de Grenoble
Grenoble, France
Sensitivity of MRI to detect lung changes
deterioration or improvement measured by the Helbich-Bhalla scoring with CT as gold standard
Time frame: Month 36
Sensitivity of MRI to Helbich-Bhalla scoring change
Sensitivity of MRI to Helbich-Bhalla scoring change in various subgroups of patients according to age, centers and MR scan manufacturers, and new treatment drug use (Ivacaftor/lumicaftor: Orkambi Ø or Ivacaftor : Kalydeco Ø ) from CT and MR examinations
Time frame: Month 0 and Month 36
CT / MR concordance
Concordance between CT and MR in amplitude of Helbich-Bhalla scoring variations at M0 and M36
Time frame: Month 0 and Month 36
Sensitivity of the 3D-UTE MR sequence
Sensitivity of the 3D-UTE MR sequence alone to detect change in Helbich-Bhalla scoring as compared to CT performed at M0 and M36
Time frame: Month 0 and Month 36
Imaging quality of the 3D-UTE MR
using a likert scale
Time frame: Month 0, Month 12, Month 24 and Month 36
Correlation between a specific Helbich-Bhalla MR score and the amplitude of change
Correlation between a specific Helbich-Bhalla MR score with clinical and functional data, and concordance with the amplitude of change between M0 and M36
Time frame: Month 0 and Month 36
Accuracy of a lung MR protocol
Accuracy of a lung MR protocol including T1-weighted and T2-weighted sequences to diagnose allergic broncho-pulmonary aspergillosis (ABPA) in CF patients
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CHRU de Lille
Lille, France
Hopital Nord
Marseille, France
Hopital Universitaire de la Timone
Marseille, France
Fondation Lenval
Nice, France
Hôpital Armand-Trousseau
Paris, France
Hôpital Necker Enfant Malades
Paris, France
...and 1 more locations
Time frame: Month 0 and Month 36
Reproducibility in detecting lung structural abnormality
MR and CT reproducibility in detecting lung structural abnormality at the segmental level
Time frame: Month 0 and Month 36
Reproducibility in overall Helbich-Bhalla scoring
MR and CT reproducibility in overall Helbich-Bhalla scoring
Time frame: Month 0 and Month 36
Correlations between Helbich-Bhalla scoring and clinical questionnaire
Correlations between Helbich-Bhalla scoring measured with MRI and CT and clinical questionnaire
Time frame: Month 0 and Month 36
Correlations between Helbich-Bhalla scoring and exacerbation rate
Correlations between Helbich-Bhalla scoring measured with MRI and CT and exacerbation rate
Time frame: Month 0 and Month 36
Correlations between Helbich-Bhalla scoring and clinical pulmonary functional test
Correlations between Helbich-Bhalla scoring measured with MRI and CT and clinical pulmonary functional test
Time frame: Month 0 and Month 36