Subclinical myocardial injury in patients with Facioscapulohumeral muscular dystrophy 1 and preserved ejection fraction – assessment by cardiovascular magnetic resonance

The study was approved by the local ethic committee (EA1/169/15) and all subjects gave written informed consent.

We prospectively screened 64 patients with FSHD1 of which 58 patients could be included in the study. CMR could not be completely performed in 6 patients: 3 due to arrhythmia (2 patients were excluded due to ventricular bigeminy and one patient due to atrial fibrillation), 1 claustrophobia, 1 obesity, 1 known allergy to contrast media. Finally, 52 patients (age 48 ± 15y, 36 men) were analyzed.

The diagnosis of FSHD1 was defined as partial loss of D4Z4 macrosatellite repeats units in the subtelomeric region of chromosome 4. While patients with FSHD1 present 1–10 repeats, there are 11–110 repeats in the general population [4]. Exclusion criteria were pre-existing cardiovascular diseases, malignancies or contraindication for CMR.

Patients underwent a cardiological work-up including physical examination and echocardiography to confirm a preserved LVEF. A LVEF lower than 55% was defined as an exclusion criterion [10].

A detailed patient medical history was recorded. Laboratory hematocrit was assessed just before CMR for quantification of extracellular volume fraction (ECV). Blood pressure was taken before and after CMR. Assessment of heart rhythm abnormalities was based on a 12-lead electrocardiogram (ECG) and an ambulatory electrocardiography monitoring for 24 h (Holter-ECG). Patients were also considered at risk of sudden death according to the Groh-criteria [11]. Following the criteria, patients were ranked positive if one of the following criteria was given: no sinus rhythm, PR interval ≥ 240 ms, QRS duration≥120 ms, second- or third-degree atrioventricular block. Screening for conduction abnormalities and arrhythmias was performed using a Holter. Low atrial rhythm is defined as inverted P waves in lead II, III, and aVF.

The group of patients was compared to 29 healthy subjects. The healthy population has been previously published [7, 12]. They underwent CMR and ECG. The protocol was exactly the same for both groups. Exclusion criteria were similar to the patient group. Details are given in Table 1.

Image analysis was performed using cvi⁴² version 5.3.2 (Circle Cardiovascular Imaging, Calgary, Canada).

Short axis cine images were used to determine LV volumes, mass and function by drawing endo- and epicardial contours (papillary muscles as part of the mass) at the end of the systolic and diastolic phases [17].

Both, the values of T2 and T1 maps were quantified as previously reported [7]. The qualitative survey implied the exclusion of segments in case of artifacts (e.g., caused by susceptibility effects or unintended thoracic motion) or wrong motion correction as described recently [7, 12]. In addition, we calculated the ECV by means of native and post-contrast T1 values and the hematocrit as published [18]. The hematocrit was assessed just before CMR, when the patient was already in the scanner (about 5 min before scan was started).

The quantitative analysis of mapping was performed as average value for slice and for each segment separately. The ROI was defined by the delineation of the endocardial and epicardial border of the myocardium. To ensure that blood or extramyocardial tissue are not included, safety rim of 5% was used. The segments were defined following the American Heart Association (AHA) segment model [19]. The visual evaluation of the LGE images was performed by two independent, experienced readers (SCMR Level III) to assess the presence, number and location of focal scar.

The detection of tiny fatty spots was possible applying fat/water separated imaging. Imaging was analyzed using pre-defined criteria [20]. A suspected region was considered positive if the intramyocardial fat could be either assured coexistent in the fat-separated image (hyperintense) and in the water-separated image (hypointense) or detected in one of the separated images and in the cine images and the LGE. That approach was verified by two experienced readers as recently published [7].

Focal fat infiltration was observed in 7/52 patients (13%, 5 men), always located in the apical part of the interventricular septal wall (Fig. 4), whereas focal fibrosis was never shown in this region. None of the healthy subjects presented fat infiltration. Three FSHD1 patients had evidence of both focal fibrosis and fat infiltration.

The medial and basal slices were analyzed. Reliability was high for both inter- and intra-observer evaluations (r = 0.93 and 0.94, ICC = 0.82 and 0.92). Apical segments were excluded due to the high exclusion rate (in 62% artifacts and/or inaccurate motion-correction).

Basal and medial T2 maps of 52 patients were evaluated. 6/624 segments had to be excluded due to artifacts. T2 values did not differ between FSHD1 patients and the control group (basal: FSHD1 50.0 ± 3.5 ms vs. controls 49.5 ± 2.2 ms, p = 0.159; medial: FSHD1 51.0 ± 2.8 ms vs. controls 49.8 ± 2.4 ms, p = 0.108).

T2 values did not differ between LGE-positive and LGE-negative FSHD1 patients (basal: LGE(+) 50.1 ± 2.2 ms vs. LGE(−) 50.0 ± 3.9 ms, p = 0.932; medial: LGE(+) 50.4. ± 3.1 ms vs. LGE(−) 51.2 ± 2.8 ms, p = 0.391). There were also no gender differences within the FSHD1 group (basal: FSHD1 men:49.7 ± 3.7 vs. women:50.7 ± 2.9 ms, p = 0.058; medial: FSHD1 men:50.4 ± 2.6 vs. women:52.0 ± 2.7 ms, p = 0.054).

Basal and medial native T1 maps of 52 patients were evaluated. 56/624 segments had to be excluded due to artifacts and incorrect motion correction. Global native myocardial T1 values were significantly longer in FSHD1 patients compared to healthy subjects, both in the basal (FSHD1:1012 ± 26 ms vs. healthy:985 ± 28 ms, p < 0.01) and the medial slices (FSHD1:994 ± 37 vs. controls:982 ± 28 ms, p = 0.028). Compared to healthy subjects, native myocardial T1 values were longer in segments with focal fibrosis (basal inferolateral: p < 0.01, basal inferior: p = 0.033, basal anteroseptal: p < 0.01). Interestingly, Native myocardial T1 values were also increased within the adjacent medial segments (inferolateral: p = 0.032, inferior: p = 0.041, anteroseptal: p < 0.01) (Fig. 5). The same could be observed for ECV. ECV of the basal and medial slices was higher in patients than healthy subjects (basal: FSHD1: 26.3 ± 2.9% vs. healthy: 23.7 ± 2.2%, p < 0.01, medial: FSHD1:26.4 ± 3.1% vs. controls:24.2 ± 2.4%, p < 0.01). ECV was higher not only in segments with focal fibrosis (basal inferolateral: p < 0.01, basal inferior: p < 0.01, basal anteroseptal: p < 0.01, basal inferoseptal: p = 0.027), but also within the adjacent regions (medial inferolateral: p = 0.048, medial inferior: p = 0.021, medial anteroseptal: p < 0.01, medial inferoseptal: p = 0.024) (Fig. 6).

This is a single center cross-sectional study and the sample size of the matched groups is relatively small, but all of the subjects have a genetically confirmed diagnosis and all patients are well characterized in our department of neurology. In the view of the prevalence of the disease, it should be considered as representative.

ECG as well as Holter-ECG was not available in all patients due to hyperaesthesia or logistic patient related reasons. Patients with arrhythmias that could influence the CMR scan quality were excluded from the study.

The potential impact of the significant, but small differences in T1-mapping related values have to be elucidated in further long-term follow-up trials.

We could not identify a relation between arrhythmia and native T1 mapping. But we have investigated only patients with preserved LVEF. One could expect that a larger sample size and an inclusion of all FSHD1 patients would lead to different results.

The capability of prolonged monitoring and inclusion of all FSHD1 patients to influence clinical outcomes should be evaluated in following studies.