High spatial resolution free-breathing 3D late gadolinium enhancement cardiac magnetic resonance imaging in ischaemic and non-ischaemic cardiomyopathy: quantitative assessment of scar mass and image quality

Navigated free-breathing LGE-CMR validation against standard breath-hold LGE-CMR was performed within the frame of clinical CMR protocol development. This retrospective study was considered a chart review. Therefore, written informed consent was waived by the hospital institutional review board.

From May 2012 until November 2013, breath-hold and free-breathing sequences were acquired in patients that were referred for LGE-CMR, if there was enough time in the clinical scanning slot. Of the 54 patients in which both BH and FB were performed, there were two incomplete free-breathing datasets (one acquisition was stopped due to allergic contrast reaction; one was stopped because of very low navigator efficiency). In one patient there was no LGE detectable. The remaining 51 patients were included (38 male; 13 female; mean age ± standard deviation: 59.9 years ± 11.4 years).

All CMR examinations were performed in our institution on a 3T unit (Ingenia, Philips Healthcare, Best, The Netherlands) with the patient in supine position. The body coil was used for transmission, and a 16-element anterior and 12-element posterior phased-array coil were used for signal reception. Following a standard clinical CMR protocol including 2D cine imaging in all cardiac axis views, the gadolinium-based contrast agent gadoterate meglumine (Dotarem, Guerbet, Villepinte, France) was administered intravenously at a dose of 0.15 mmol/kg. Ten minutes after contrast administration, a 2D gradient-echo T1 weighted sequence was used (i.e. Look-Locker) to visually determine the optimal inversion time (TI) of healthy myocardium. Approximately 10–15 min post-contrast, a whole heart high spatial resolution 3D gradient echo (T1 fast field echo) PSIR sequence was acquired during free breathing with diaphragmatic pencil-beam navigation. Image parameters were as follows: repetition time (TR) 4.15 ms; echo time (TE) 2.02 ms; TI was set at the null point plus 50 ms and ranged from 250 to 400 ms; flip angle (FA) 10°; field of view (FOV) 350 × 350 mm; matrix size 208 × 208; acquired pixel size 1.68 × 1.68 mm; reconstructed pixel size 0.91 × 0.91 mm; 71 transverse slices with 3.4 mm thickness and slice gap -1.7 mm; sensitivity encoding (SENSE) factor 3. The 2D pencil beam respiratory navigator was planned on the right hemidiaphragm. The acceptance window was set at 5 mm with a constant correction of 0.6. Saturation bands were planned on the navigator, vertebrae and thoracic subcutaneous adipose tissue to suppress residual motion artefacts. Acquisition time was 3 min 4 s assuming 100 % navigator efficiency and heart rate of 60 beats per minute (bpm). Directly after free-breathing LGE-CMR, BH was acquired using a 3D gradient echo PSIR sequence in short-axis slice orientation in two equal stacks during two breath-holds of 10–20 s duration. Subsequently, left two-chamber and four-chamber cardiac views were acquired using the same sequence. Typical scan parameters were: TR 4.31 ms; TE 2.09 ms; TI 250–400 ms (same as free-breathing); flip angle 10°; FOV 350 × 350 mm; matrix size 188 × 125 mm; acquired pixel size 1.86 × 2.8 mm; reconstructed pixel size 1.46 × 1.46 mm; 24 slices with 10 mm thickness and – 5 mm slice gap; SENSE factor 3.

MASS research software (Department of Radiology, Leiden University Medical Centre, Leiden, The Netherlands) was used for multiplanar reformatting and image analysis. BH data were analysed after offline fusion of data of the two breath-hold 3D stacks. Free-breathing 3D datasets were reformatted into two multiplanar reconstructions with identical geometry as BH: one with normal spatial resolution (FB-NR: 1.46 × 1.46 × 10 mm), matching BH, and one with high spatial resolution isotropic voxel reconstruction (FB-HR: 0.91 × 0.91 × 0.91 mm). (See Online Supplementary Material for a description of reconstruction method.) Images were analysed in random order. First, endocardial and epicardial contours were drawn manually. Second, regions with maximally hyperenhanced and hypoenhanced healthy myocardium were identified visually and a small region of interest was drawn. Third, myocardial scar was identified automatically using the validated full-width half maximum (FWHM) algorithm [2, 13, 14]. For this algorithm, maximal signal intensity (SI_max) was defined as the mean signal intensity of the manually annotated hyperenhanced region, and minimal signal intensity (SI_min) was defined as the mean signal intensity of the manually annotated hypoenhanced region. Myocardial scar was defined as voxels with signal intensity higher than 50 % (SI_min + 0.5 × (SI_max – SI_min). Grey zone (only reported for ICM patients) was defined as voxels with signal intensity between 35 % (SI_min + 0.35 × (SI_max – SI_min) and 50 % (SI_min + 0.5 × (SI_max – SI_min). Fourth, manual adjustments to the automatically determined areas of scar were made only in cases of evident misinterpretation by the algorithm, for example in case of microvascular obstruction. Finally, scar and grey zone masses were calculated (in grams: specific weight of scar was set at 1.05 g/ml) using an in-house developed MATLAB script (Version R2012A, Natick, MA, USA).

SNR was calculated by dividing (SI_max – SI_reference) by the noise (standard deviation of signal outside the body). SI_max was subtracted by SI_reference to compensate for high signal intensity of the nulled healthy myocardium in PSIR (which is 0 in magnitude inversion recovery images) [15]. CNR was computed as the difference between SI_max and SI_min, divided by the noise (standard deviation of signal outside the body). Figure 1 is a 2D representation of 3D computation of SES, which was computed with an algorithm in the Matlab environment (v. R2012a, Mathworks, Natick, MA, USA). To account for differences in signal intensity between breath-hold and free-breathing datasets, the signal intensity of all voxels containing myocardium were normalised on a scale of 0 % (SI_min) to 100 % (SI_max): SI_normalised = (SI – SI_min) / (SI_max –SI_min). Then, at the edge of the scar, the steepness of the slope (expressed in ΔSI_normalised / mm) reflects SES. A SES of 1.0 reflects a full transition of scar to healthy myocardium over a 1.0-mm distance.

Data are presented as mean ± standard deviation. BH sequence was compared to FB-NR for validation purposes. Subsequently, FB-NR was compared with FB-HR. Outcome measures were compared using paired-samples t-test. Agreement of scar mass was compared using Pearson’s correlation coefficient and Bland Altman analysis. A p value of less than 0.05 was considered to indicate statistical significance. Statistical analyses were performed using SPSS software (version 20, SPSS, Chicago, IL, USA).

Scar mass was the same in BH versus FB-NR (mean ± SD: 15.5 g ± 18.0 g vs. 15.5 g ± 16.9 g, p = 0.997). Moreover, scar mass showed good correlation (r = 0.953) without systematic bias in Bland Altman analysis (mean difference ± SD: 0.00 g ± 5.47 g), as shown in the Online Supplementary Material. Limits of agreement were between −10.94 g and +10.93 g.

FB-NR yielded higher scar mass as compared with FB-HR (15.5 g ± 16.9 g vs. 14.4 g ± 15.6 g; p = 0.007). Although the data correlated well (r = 0.988), Bland Altman analysis demonstrated a systematic positive bias of + 1.15 g for FB-NR versus FB-HR (mean difference ± SD: + 1.15 g ± 2.84 g), as shown in the Online Supplementary Material. Limits of agreement were between –4.42 g and +6.72 g.

In the ICM subgroup, scar mass was 18.9 g ± 20.2 g in BH versus 19.3 g ± 18.7 g in FB-NR, which was not significantly different (p = 0.670). In parallel with scar mass in all patients, FB-NR overestimated scar mass as compared with FB-HR in the ICM subgroup (19.3 g ± 18.7 g vs. 17.9 g ± 17.2 g, p = 0.01).

Grey zone was not significantly different between BH versus FB-NR (6.5 g ± 5.4 g vs. 6.0 g ± 6.0 g, p=0.128), and between FB-NR vs. FB-HR (6.0 g ± 6.0 g vs. 6.2 g ± 6.0 g, p=0.329).

In NICM patients scar mass was similar in BH vs. FB-NR (7.3 ± 6.1 g vs. 6.3 g ± 4.3 g, p=0.312). The difference in scar mass between FB-NR and FB-HR was not significant in this subgroup (6.3 g ± 4.3 g vs. 5.9 g ± 4.8 g, p=0.457).

As shown in the Online Supplementary Material, SNR and CNR were significantly lower in BH as compared with FB-NR (207.6 ± 85.8 vs. 1052.2 ± 877.2, p < 0.01 and 221.9 ± 70.9 vs. 864.9 ± 692.5, respectively). As a result of higher spatial resolution, SNR and CNR decreased significantly in FB-HR as compared with FB-NR (258.3 ± 94.9 vs. 1052.2 ± 877.2, p < 0.01 and 232.4 ± 91.5 vs. 864.9 ± 692.5, p < 0.01, respectively). In the ICM subgroup, SNR and CNR were lower in BH as compared with FB-NR (224.7 ± 87.3 vs. 1125.0 ± 1010.9, p < 0.01 and 240.4 ± 66.8 vs. 935.1 ± 789.1, p < 0.01, respectively). In FB-HR, SNR and CNR were lower as compared with FB-NR (272.9 ± 93.4 vs. 1125.0 ± 1010.9, p < 0.01 and 250.6 ± 89.1 vs. 935.1 ± 789.1, p< 0.01, respectively). Also in the NICM subgroup, SNR and CNR were lower in BH as compared with FB-NR (165.9 ± 67.9 vs. 875.5 ± 374.4, p < 0.01 and 177.1 ± 61.4 vs. 694.3 ± 330.3, p < 0.01, respectively), and lower in FB-HR as compared to FB-NR (222.8 ± 92.1 vs. 875.5 ± 374.4, p < 0.01 and 188.2 ± 84.5 vs. 694.3 ± 330.3, p < 0.01, respectively).

SES was similar in BH versus FB-NR (0.176 ± 0.039 vs. 0.176 ± 0.036, p = 0.947), see Online Supplementary Material. FB-HR images had significantly higher SES as compared to FB-NR (0.216 ± 0.042 vs. 0.176 ± 0.036, p < 0.01). The absolute increase in sharpness was 0.040 with 95% confidence interval between 0.032 and 0.048, corresponding to a relative increase in SES of 22.7 % with 95 % confidence interval between 18.7 and 27.2. An example of the different signal intensity profiles across the edge of the scar of FB-NR vs. FB-HR is shown in Fig. 6. In the ICM subgroup, SES was the same in BH and FB-NR (0.176 ± 0.033 vs. 0.173 ± 0.036, p = 0.639), and statistically significantly higher in FB-HR as compared with FB-NR (0.212 ± 0.038 vs. 0.173 ± 0.036, p < 0.01). Also in the NICM subgroup, SES was the same in BH and FB-NR (0.176 ± 0.053 vs. 0.182 ± 0.039, p = 0.460), and statistically significantly higher in FB-HR as compared with FB-NR (0.227 ± 0.050 vs. 0.182 ± 0.039, p < 0.01).