Regional differences in prognostic value of cardiac valve plane displacement in systemic light-chain amyloidosis

We identified patients with cardiac biopsy-secured systemic AL amyloidosis who had undergone a CMR between February 2005 and October 2014 at our institution for a retrospective single-center post-hoc analysis. Patient selection is demonstrated in a flow chart (Fig. 1a). The mean interval between CMR and the start of chemotherapy was 23 days. The diagnosis was defined by the presence of monoclonal gammopathy by serum electrophoresis, immunofixation on serum and urine, and free light chain test, and confirmed by positive Congo red staining with birefringence under polarized light of any biopsy (periumbilical fat aspiration, rectum or target organ), positive immunohistology for kappa or lambda in the biopsy, and on the exclusion of hereditary forms of amyloidosis. The study population was referred to our imaging center for cardiologic work up with diagnosed light chain disorder. All 68 patients have signed a written informed consent for the retrospective analysis of clinical routine data. The use of de-identified patient data for research purposes was approved by the institutions ethics committee in accordance to the Declaration of Helsinki.

All CMR examinations were performed on a 1.5 Tesla scanner (Achieva, Philips Healthcare, Best, The Netherlands) equipped with a cardiac phased array 32-channel receiver coil. Cine images were obtained using a breath-hold segmented-k-space balanced fast-field echo sequence (bSSFP) employing retrospective electrocardiogram (ECG)- or pulse oximetric gating with 35 phases per cardiac cycle. Typical CMR imaging parameters were: field-of-view (FOV) = 350 × 350 mm², repetition time/echo time (TR/TE) = 2.8/1.4 ms, acquired voxel size = 2.2 × 2.2 × 8 mm³, flip angle (FA) = 60°, reconstructed voxel size = 1.3 × 1.2 × 8 mm³. Data were analyzed by a single examiner blinded to the patients’ clinical status. Routine analysis was performed on a commercially available workstation (IntelliSpace Portal (ISP) Version 7.0.1, Philips Healthcare, Best, The Netherlands) with a semi-automatic software for volumetric analysis. Ventricular volumes, ejection fraction and LV myocardial mass were acquired in short axis stacks by manually tracing epi- and endocardial borders, excluding papillary muscles from the myocardium. Relative LGE mass was measured using a 5-standard-deviation (SD) threshold in reference to visually unenhanced myocardium (Fig. 1b) [16]. LGE was graduated into (1) none, (2) subendocardial or (3) transmural involvement (qualitative LGE). Global longitudinal strain (GLS) derived from cine SSFP of 2-, 3-, and 4-chamber long axis views by delineating endo- and epicardial borders at end-diastole using CVI cmr⁴² version 5.6.1, (Circle Cardiovascular Imaging, Calgary, Canada). Regional longitudinal strains are presented for basal (mean longitudinal strain of American Heart Association segments 1 to 6), midventricular (mean longitudinal strain of segments 7 to 12) and apical slices (mean longitudinal strain of segments 13 to 16).

Regional systolic valve plane excursion was assessed at seven locations on anterior aortic plane systolic excursion (AAPSE), anterior, anterolateral, inferolateral, inferior and anterolateral mitral (MAPSE), and lateral tricuspid annulus (TAPSE) derived from cine bSSFP images in 2-, 3-, and 4-chamber views as previously described [15]. CVPD was defined as the distance from peak end-diastolic to peak end-systolic excursion of each annular region, where the endocardial insertion points of the aortic, mitral or tricuspid valve leaflets respectively served as anatomic landmarks.

Blood samples were drawn up to 14 days before the date of CMR examination. NT-proBNP (N-terminal prohormone of brain natriuretic peptide) and cTNT (cardiac troponin T) were obtained from a commercially available fully automated analyzer based on a sandwich immunoassay (ELECSYS, Roche Diagnostics, Mannheim, Germany). Glomerular filtration rate was estimated by the “Modified Diet in Renal Diseases” (MDRD) formula.

Primary combined endpoint was all-cause mortality or heart transplantation. Follow-up was obtained by review of patient’s electronic records or telephone interview with the patient or relative.

Data were analyzed using MedCalc, version 15.11.4 (MedCalc Software, Ostend, Belgium). Continuous and normal distributed variables (Kolmogorov-Smirnov test, p ≥ 0.05) were expressed as mean ± standard deviation. Group differences for continuous variables were tested using the independent t-test, and differences between nominal variables were assessed using the Fisher exact test. Continuous variables without normal distribution were stated as median and interquartile range (IQR), group differences were tested using the nonparametric Mann-Whitney U test. Kaplan-Meier curves were used to estimate the distribution of survival as a function of the follow-up duration. Optimal cut-off values were defined by Receiver operating characteristics (ROC) and Youden’s J statistic. The association of clinical, imaging and serological parameters with outcome was evaluated by uni- and multivariate Cox proportional-hazards regression models. Differences were considered statistically significant at p < 0.05.