Impact of MIgalastat TheRApy on CaRdiac Function in patiEnts With Fabry's Cardiomyopathy (MIRACRE-Fabry Trial)

Yonsei University

Status

Enrolling

Conditions

Fabry Disease

Treatments

Other: Echocardiography

Study type

Observational

Funder types

Other

Identifiers

NCT04639999

4-2020-1038

Details and patient eligibility

About

This is an observational study. No treatment or intervention will be assigned to the subjects. All patients will receive full standard of care concomitant medication for the treatment of their cardiac condition. 20 patients with genetically confirmed Anderson-Fabry disease who have a plan to start Migalastat will undergo 2D strain, diastolic stress echocardiography, LV vortex flow analysis, and CMR at baseline and after 2 year of treatment with Migalastat for follow-up.

Full description

Objectives - to evaluate the impact of chaperone therapy on LV diastolic function and flow in patients with Fabry's cardiomyopathy using LV 2D strain, diastolic stress echocardiography, LV vortex flow and CMR.
Primary/Secondary Endpoint

A. Primary endpoint:
- Change of peak exercise E/E' by diastolic stress echocardiography, global longitudinal strain and LV vortex flow parameters at 2 year follow up.
B. Secondary endpoints:
- Changes of extracellular volume by CMR (T1 mapping) at 2 year follow up
- Evaluation of the degree of the resting LV diastolic function
- Evaluation of global and regional LV strain
- Other echo-parameters; LV mass index at baseline, 2 year follow up, reduction of peak exercise E/E prime at 2 year follow up
- Changes of quality of life using questionnaire
- Change of peak VO2, exercise time, AT by diastolic stress echocardiography at 2 year follow up
- Change in T1 baseline (myo, ms) & T1 baseline (blood, ms) T1 postcontrast (myo, ms) & T1 baseline (blood, ms) by CMR
Study Methods -Study Design: This is an observational study. No treatment or intervention will be assigned to the subjects. All patients will receive full standard of care concomitant medication for the treatment of their cardiac condition. 20 patients with genetically confirmed Anderson-Fabry disease who have a plan to start Migalastat will undergo 2D strain, diastolic stress echocardiography, LV vortex flow analysis, and CMR at baseline and after 2 year of treatment with Migalastat for follow-up.

Enrollment

20 estimated patients

Sex

All

Ages

16 to 70 years old

Volunteers

No Healthy Volunteers

Inclusion criteria

Patients aged 16 ~ 70 years with Fabry's disease who were confirmed by enzyme assay and gene study
Patients who have LV hypertrophy in 2D echocardiography (end diastolic septum and posterior wall thickness ≥12mm) or Patients who present with cardiac changes (indicative of disease progression such as decreased global longitudinal strain on 2D strain echocardiography or low native T1 mapping on cardiac MRI) even without LV wall thickness of ≥12mm
Patients provided with the written, informed consent to participate in this study

Exclusion criteria

Contraindication for chaperone therapy (Migalastat)
Patients who cannot perform supine bicycle stress echocardiography, contrast echocardiography or cardiac MRI
Hemodynamically significant valvular heart disease or arrythmias
History of acute myocardial infarction or congestive heart failure with reduced LV ejection fraction of less than 35%
CVA in the prior 6 months
Scheduled or planned surgery in the next 6 months
Chronic liver cirrhosis
Allergy to contrast agent (Definity®, Lantheus Medical Imaging, North Billerica, MA, USA)