10147993536052Circ Cardiovasc ImagingCirc Cardiovasc ImagingCirculation. Cardiovascular imaging1941-96511942-008021576279346037710.1161/CIRCIMAGING.110.958751NIHMS305065ArticleHeterogeneity of Intramural Function in Hypertrophic Cardiomyopathy: Mechanistic Insights from MRI Late Gadolinium Enhancement and High-resolution DENSE Strain MapsAletras et al: Intramural Function in HCM using LGE and DENSE MRIAletrasAnthony H.PhDTilakGauri S.MD, PhD, MPHHsuLi-YuehDScAraiAndrew E.MDCardiovascular and Pulmonary Branch, National Heart, Lung and Blood Institute, National Institutes of Health, Department of Health and Human Services, Bethesda, MD, U.S.ADepartment of Computer Science and Biomedical Informatics University of Central Greece, Lamia, GreeceCorrespondence to: Andrew E. Arai, MD, Cardiovascular and Pulmonary Branch, National Heart, Lung, and Blood Institute, National Institutes of Health, Bldg 10, B1D-461, MSC 1061, 10 Center Drive, Bethesda, MD 20892-1061 USA, Phone: 301-496-3658, Fax: 301-402-2389, AraiA@nhlbi.nih.gov1772012165201172011289201244425434Background

In HCM, myocardial abnormalities are commonly heterogeneous. Two patterns of LGE have been reported: a bright “confluent” and an intermediate intensity abnormality termed “diffuse,” each representing different degrees of myocardial scarring. We used MRI to study the relation between intramural cardiac function and the extent of fibrosis in HCM. The aim of this study was to determine whether excess collagen or myocardial scarring, as determined by late gadolinium enhancement (LGE) MRI, are the primary mechanisms leading to heterogeneous regional contractile function in patients with hypertrophic cardiomyopathy (HCM).

Methods and Results

Intramural left ventricular (LV) strain, transmural LV function, and regions of myocardial fibrosis/scarring were imaged in 22 patients with HCM using displacement encoding with stimulated echoes (DENSE), cine MRI and LGE. DENSE systolic strain maps were qualitatively and quantitatively compared with LGE images. Intramural systolic strain by DENSE was significantly depressed within areas of confluent and diffuse LGE but also in the core of the most hypertrophic non-enhanced segment (all p<0.001 vs. non-hypertrophied segments). DENSE demonstrated an unexpected inner rim of largely preserved contractile function and a non-contracting outer wall within hypertrophic segments in 91% of patients.

Conclusions

LGE predicted some but not all of the heterogeneity of intramural contractile abnormalities. This indicates that myocardial scarring or excess interstitial collagen deposition does not fully explain the observed contractile heterogeneity in HCM. Thus, myofibril disarray or other non-fibrotic processes affect systolic function in a large number of patients with HCM.

hypertrophic cardiomyopathymagnetic resonance imagingDENSEdisplacement encoding with stimulated echoesmyocardial functionstrainlate gadolinium enhancementNational Heart, Lung, and Blood Institute : NHLBIZ01 HL004607-10 || HLNational Heart, Lung, and Blood Institute : NHLBIZ01 HL004607-09 || HL

Hypertrophic cardiomyopathy (HCM) is a genetic disease characterized by left ventricular (LV) hypertrophy1, 2 due to hyperplasia and hypertrophy of myocytes and hyperplasia of several other cell types. Myofiber disarray and interstitial fibrosis occur commonly 3, 4. Hypertrophy and fibrosis are associated with LV systolic and diastolic dysfunction, heart failure, arrhythmias, morbidity, and mortality 58. Myocardial ischemia, infarction and fibrosis occur in HCM despite widely-patent epicardial coronary artery vessels 9, 106. MRI late gadolinium enhancement (LGE) has revealed two types of abnormalities which may be related to infarction or fibrosis. Confluent LGE appears in most respects comparable to the type of bright gadolinium enhancement seen in the myocardial infarctions of patients with ischemic heart disease 11. Diffuse LGE likely represents less severe myocardial fibrosis or milder degrees of excess collagen deposition. It has also been postulated that the interstitial fibrosis may be a secondary and reversible phenotype 5, 12.

Extrapolations from transmural measurements of myocardial strain have led some investigators to postulate that patients with HCM may have preserved endocardial strain 13, 14 while others suggest there should be reduced endocardial strain 15, 16. A study by Tseng et al. 4 shows that myocardial fiber disarray is related to reduced myocardial strain. However, this study does not address the presence or absence of myocardial fibrosis within the hypokinetic regions. A more recent echocardiographic study by Popovic et al. 17 reports that non-fibrotic myocardial segments exhibit increased strain compared to segments with fibrosis. This finding suggests that perhaps some function is preserved in non-fibrotic hypertrophic segments. However, this could also reflect partial volume effects since average midwall strain measurements were studied in a 12 segment model.

High resolution imaging of intramural strain might provide insight into the relative contribution of myocardial fiber disarray and myocardial fibrosis as distinct mechanisms causing regional LV dysfunction. DENSE 18, 19 (Displacement Encoding with Stimulated Echoes) MRI can quantify short axis regional systolic function at high spatial resolution. DENSE allows direct measurement of intramural myocardial strain expressed in terms of circumferential shortening (CS) and radial thickening (RT) - a significant advance over transmural measures of regional function such as absolute systolic change in wall thickness (in mm) or percent wall thickening.

This study aimed to determine whether excess collagen or myocardial scarring, as determined by gadolinium enhanced MRI, are the primary mechanisms leading to heterogeneous regional contractile function in patients with HCM. We hypothesized that if intramural contractile function in HCM is heterogeneous due to excess collagen deposition or myocardial scarring, then hypokinesis will be localized primarily in areas with LGE. However, if extensive hypokinesis is observed outside the areas of LGE, then excess collagen or myocardial scarring is unlikely to be the only mechanism leading to heterogeneous regional contractile function in patients with HCM. Finally, it is possible that severely hypertrophic myocardium has diffusely abnormal function regardless of regional fibrosis. This possibility is sometimes referred to as “muscle bound”. We also hypothesized that high resolution intramyocardial DENSE strain maps would be able to image these functional abnormalities. Such imaging should be able to resolve these three possibilities.

An unexpected finding of this work was the presence of largely preserved inner wall strain in hypertrophic segments with overall low transmural strain. While an endocardial ring of preserved contractility in HCM has been postulated to exist, 17 no direct visualization has been provided to date. Therefore, additional analysis of this pattern of intramural strain was performed since it was not predicted by geometric models of myocardial hypertrophy.

MethodsStudy Population

Twenty-two patients with HCM were studied under research protocol 09-H-N237 approved by the National Heart Lung and Blood Institute’s review board. The diagnosis of HCM was established by echocardiography (>15 mm LV wall thickness in the absence of another cause for the increased cardiac mass). Patients with a history of alcohol septal ablation or cardiac surgery were excluded. Only patients who underwent both DENSE and LGE imaging were included. LV outflow tract gradients at rest were obtained by cardiac catheterization.

MRI Studies

Subjects were scanned in a 1.5 T MRI scanner using a cardiac phased array coil. LV systolic function and mass were imaged with cine MRI along contiguous short axis slices (typically with 1.4×1.4 mm/pixel and 8 mm slice thickness). Intramural circumferential shortening (CS) and radial thickening (RT) measurements were made with DENSE with a volumetric preparation. Displacement was mapped for every pixel of the end-systolic image allowing systolic strain (CS and RT) maps to be computed. End-systole was determined from the cine MRI. LGE imaging was performed with an inversion recovery method 20 after a dose of 0.2 mmol/kg gadopentetate dimeglumine (typical resolution of 1.4×1.4 mm/pixel, slice thickness of 8 mm) with the inversion time optimized to null normal myocardium.

Data analysis

LV ejection fraction and total myocardial mass were measured using computer assisted planimetry. The signal intensity was quantified in confluent and diffuse lesions21, from normal myocardium and the LV blood pool. In short, confluent lesions were defined as qualitatively having bright signal similar to that found in non-viable myocardium in patients with CAD. Diffuse lesions were defined as qualitatively having signal brighter than that of nulled myocardium and signal less bright than that of confluent lesions. The “most hypertrophic non-enhancing segment” was defined as the thickest segment (as seen on end-diastolic cine images) without LGE. To mitigate potential through-plane motion misregistration issues between DENSE and LGE, the adjacent slices to the one containing the “most hypertrophic non-enhancing segment” were examined for absence of LGE. Remote myocardium was defined as myocardium diametrically opposite to the hypertrophic segments. Following endocardial and epicardial segmentation, DENSE displacement maps were automatically processed to produce circumferential shortening (CS) and radial thickening (RT) strain maps 22. CS and RT maps were scaled using a standardized color scale that displayed quantitative regional function on a pixel-by-pixel basis. Region of Interest (ROI) analysis was performed to measure CS and RT within confluent, diffuse and most hypertrophic non-enhanced areas. Only one slice per patient was analyzed in order to preserve the independence of the samples. Apical slices were excluded from data analysis to avoid partial volume effects 23.

Statistical Analysis

Continuous measurements are expressed as mean ± standard deviation (SD) for descriptive purposes. Standard error of the mean (SEM) was used in figures where the primary purpose was to depict differences between two average values. Comparisons used a paired t-test with Bonferroni correction for multiple comparisons (p-values are presented unadjusted and the appropriate level of significance is used within each group of comparisons).

ResultsDemographics

Six patients (Table 1) had severe symptoms related to LV outflow obstruction while others had mild or no symptoms. Four were asymptomatic, seven presented with shortness of breath (SOB), three with chest pain (CP) and eight with a combination of SOB and CP. The average pulmonary capillary wedge pressure (PCWP) was 12±5 mmHg but 6 patients had significantly elevated PCWP. The maximum wall thickness averaged 25±5 mm. Median value of LV mass was 185 grams (range: 76 to 567) and the ejection fraction averaged 66±6%. Median value of LGE was 5.8% of the left ventricle (range:1.8 to 41.5). Nineteen of the patients had asymmetric septal hypertrophy (ASH), two with severe concentric hypertrophy (CON) and one with hypertrophy localized to the mid-ventricle (MID). Of the 22 individuals evaluated, only 4 had identified mutations after an unbiased screening of the Beta-Myosin head (exons 1–23) (Table 1). Patient numbers 1 and 20 are related and have the R403Q mutation. Patient number 5 has the K847E mutation. Patient number 15 has a Val95Ala mutation in Alpha-tropomyosin. On the basis of the unbiased screening, it can be concluded that the other patients are very unlikely to have mutations in the Beta- Myosin head.

DENSE Detects Patterns of Intramural Contractile Function associated with LGE

DENSE strain maps and LGE images can directly show that LGE is not a prerequisite for the presence of intramural functional abnormalities. DENSE functional abnormalities that are either more extensive than LGE imaging predicts or that are present in the absence of LGE can directly disprove the primary hypotheses. Figures 14 summarize the relationship between LGE and intramural cardiac function as depicted by DENSE CS and RT color strain maps. The color scale represents intramural percent circumferential shortening and percent radial thickening respectively. Normal CS and RT are generally mapped white to bright orange. Dark orange and purple hues represent mild and severe strain abnormalities. The transition from blue to green represents zero systolic strain. Green to black represents dyskinetic strain (i.e. systolic circumferential stretching or systolic radial thinning). Figures 14 also show diastolic and systolic frames from cine MRI (first and second images on the top row respectively) as well as LGE (third image on the top row).

An example that supports the concept that myocardium with confluent LGE does not contract normally in HCM is shown in Figure 1. This patient has a confluent abnormality of LGE in the inferior septum which corresponds to a severe focal abnormality in systolic strain as represented by the blue and purple patches corresponding to less than 10% circumferential shortening and radial thickening. Note that the signal intensity on the LGE is similar to what is typically observed in patients with myocardial infarction due to coronary artery disease (i.e. the myocardial enhanced zone and the left ventricular blood pool present with similar signal intensity) except that the abnormality is not located in the subendocardium.

Diffusely enhancing myocardium also does not contract in HCM (Figure 2). In this example, a diffuse pattern of LGE, which corresponds to a severe intramural strain abnormality on color-coded DENSE, can be seen in the anterior wall and anteroseptum. The myocardial signal intensity in the late gadolinium enhanced zone is much lower than in cases with confluent LGE. The DENSE CS and RT maps show normal strain (orange to white) in the septum, inferior and lateral walls as well as in the inner 1/3 of the anterior and anteroseptal segments. Thus, there is a substantial amount of myocardium in all segments with normal strain and a zone of very low strain in the outer half of the segment with diffuse gadolinium enhancement. Cine MRI showed normal systolic endocardial excursion and ejection fraction in this patient but could not assess intramural function.

Intramural functional abnormalities can be more extensive than predicted by the extent of LGE. Figure 3 shows a patient with more severe septal hypertrophy but a similar sized abnormality of confluent LGE to the one seen in Figure 1. Despite severely depressed strain in the two thirds of the septum near the right ventricle, DENSE maps of intramural strain again showed a nearly circumferential inner ring of largely normal contraction. The amount of myocardium with normal strain (orange-white) is comparable in all segments around this short axis slice despite large functional abnormalities in the remainder of the septum. Systolic strain in this patient is more heterogeneous than LGE would predict. Cine MRI shows global systolic function (corresponding to an EF of 64%) that almost obliterates the mid left ventricular cavity.

Intramural functional abnormalities in HCM also exist in the absence of significant LGE. Figure 4 shows an example where the DENSE maps of intramural strain show two large distinct contractile abnormalities (purple to blue/black patches) separated by a zone of nearly normally contracting myocardium in the mid-septum. In this patient, there is only a small region of confluent LGE within the inferoseptum. Cine MRI showed hyperdynamic global systolic function in this patient.

The examples shown in Figures 24 indicate that reduced contractile function is not necessarily associated with LGE. In most of the patients (17 out of 22) the LGE was not localized to the inner third of the heart consistent with viable myocardium in the regions where strain appeared normal in most of these patients (Table 1).

Heterogeneous Intramural Function Irrespective of Pattern or Presence of Enhancement

Intramural function by DENSE was not only depressed within areas of both confluent and diffuse LGE but also at the core of the most hypertrophic non-enhanced segment (Figure 5). Specifically, CS was significantly reduced within the confluent late gadolinium enhanced regions compared to a normal remote non-enhanced non-hypertrophic region (6.1±1.6 vs. 20.4±1.8% CS respectively, p<0.001). Diffuse late gadolinium enhanced regions exhibited disproportionally reduced intramural CS compared to a normal remote non-enhanced non-hypertrophic region (7.5±0.9 vs. 18.4.8±2.1% CS respectively, p<0.001). Interestingly, the most hypertrophic non-enhanced segment also had significantly reduced intramural strain when compared to a normal remote non-enhanced non-hypertrophic region (9.3±1.5 vs. 19.1±2.2% CS respectively, p<0.001). Radial thickening DENSE data showed similar results (confluent enhancement 7.6±1.3 vs. normal 29.5±1.3%, p<0.001; diffuse enhancement 9.1±0.9 vs. normal 23.4±1.9%, p<0.001; most hypertrophic non-enhanced 9.5±1.2 vs. normal 28.3±1.4%, p<0.001).

On late gadolinium enhanced images, the signal intensity was significantly different for confluent and diffusely enhancing versus normal myocardium (Figure 6, both p<0.001). The signal intensity in the most hypertrophic non-enhancing myocardium was not significantly different than normal myocardium, an important control measurement that indicates the qualitative characterization of amount of gadolinium in these regions was not simply due to the way the images were displayed.

Preserved Absolute Wall Thickening and Inner wall Contractile Function

DENSE intramural contractile function demonstrated a complete circumferential inner rim of largely normal contracting myocardium in 77% of the patients (17 out of 22). This group of patients had on average a normal ejection fraction (66.8%±4.3). Predominantly transmural hypokinesis in the hypertrophic zone was observed in 2 out of 22 patients. These two patients had reduced ejection fractions (<55%). The remaining 3 out of 22 patients presented with a mixture of both patterns of intramural contractile function within the hypertrophic zones (ejection fraction 67.7%±5.8). Thus, 91% of patients had a complete or significant amount of myocardium with normal strain in the inner layers of the left ventricle.

Absolute systolic wall thickening by CINE MRI was overall preserved in these HCM patients (Figure 7A). In particular, absolute systolic wall thickening averaged more than 6 mm even with an end-diastolic wall thickness of 20 mm. Even the most hypertrophic segments (end-diastolic thickness greater than 25 mm) exhibited normal absolute systolic wall thickening defined as >3 mm 24. On average, more than 5 mm of absolute systolic wall thickening was observed by CINE MRI for both hypertrophic and non-hypertrophic segments independent of the extent of LGE. These findings of overall preserved absolute systolic wall thickening are concordant with the observed preserved ejection fractions (Table 2). Conversely, a normal ejection fraction or significant regional wall thickening did not preclude large patches of severely depressed intramural systolic function.

On average, percent systolic wall thickening (Figure 7B) was inversely related to end-diastolic wall thickness suggesting that transmural contractile function in the most hypertrophic myocardial segments is very low.

In non-hypertrophic segments (Figure 8, EDWth < 12 mm), percent wall thickening was inversely related to increasing extent of segment LGE. In hypertrophic segments (Figure 8, EDWth >=12 mm), percent wall thickening was low irrespective of extent of LGE.

Discussion

The DENSE systolic strain maps show heterogeneous myocardial function in HCM which requires a heterogeneous mechanism rather than a diffuse or global process. LGE predicts some but not all of the heterogeneity of intramural contractile abnormalities. Since LGE is a highly sensitive method 11, 25, myocardial scar and excess collagen deposition cannot explain the spectrum of heterogeneous intramural function encountered in HCM. Myofiber disarray is one mechanism that could impair function without showing abnormalities on late enhancement images4. The frequently observed pattern of an inner ring of normal intramural strain provides a mechanism that can explain preserved global left ventricular function despite severe strain abnormalities in the remainder of that segment. That observation could not be predicted by “uniform models” or assumptions about cardiac contraction. There are several factors that lead to heterogeneity of intramural function in patients with HCM and most of these mechanisms cannot be visualized with transmural or low resolution methods. Thus, the ability to spatially register high resolution strain maps with LGE images allows interrogation of the relationships between function and myocardial scar/collagen at an unprecedented level.

Histopathological studies have identified more than one kind of intramural heterogeneity in HCM that could relate to contractile abnormalities. Sarcomeric disarray is highly heterogeneous 26, 27 and not even confined within hypertrophic segments 26. Sarcomeric hypertrophy occurs in the endocardium and the mid-wall 28, 29. Diffuse interstitial fibrosis and myocardial scarring are common in HCM 28, 30, 31. Moreover, a high fraction of young patients with HCM but no coronary artery disease have patchy signs of acute-subacute ischemia postmortem 31.

At a clinical level, HCM is characterized by many types of heterogeneous abnormalities. Resting myocardial blood flow is heterogeneous despite metabolic demands similar to that of normal myocardium 32 and is related to LGE 10. Multi-focal patterns of LGE have also been identified in asymptomatic and mildly symptomatic HCM patients 23. These patterns, which may represent infarction, fibrosis, or excess collagen deposition 33, 34, were later correlated with progressive dilation of the ventricle and risk of sudden death 21.

Characterization of intramural left ventricular strain based on simple geometrical models does not apply in HCM since the assumption of a homogeneously contracting medium is not valid. Based on such models, there is a largely linear endocardial to epicardial gradient of circumferential strain and HCM 35. Pioneering myocardial tagging studies may have masked the intramural strain heterogeneity due to the coarse spatial resolution (tag spacing of 7mm) 35. Other MRI tagging studies in patients with HCM have previously reported abnormal contractile function in the left ventricle. Both radial displacement 36 and circumferential shortening are reduced in the septum 37. Similar results were also obtained for total systolic strain recently with methods that allow full cardiac cycle interrogations 38 whereas diastolic strain was reduced in all segments.

Late gadolinium enhancement is not as closely linked to the full range of contractile abnormalities detected in HCM whereas in coronary artery disease regional function varies inversely with the transmural extent of gadolinium delayed enhancement 20. In patients with HCM, the extent of delayed enhancement is inversely related to systolic segmental percent wall thickening 23. While the current study also found an inverse relationship between percent wall thickening and the extent of LGE, this only applied to the less severely hypertrophic segments (Figure 8). In the thickest regions of the heart, transmural systolic contraction was independent of the extent of LGE (Figure 8). While not addressed by this dataset, myocardial edema or inflammation may also explain the discrepancy between regional contractile function and LGE 39, 40.

The DENSE MRI acquisition has many advantages in producing cardiac strain measurements. DENSE has been used to measure post-infarct recovery of function 41. Myocardial tagging 42, harmonic phase image processing 43 and DENSE have yield comparable strain measurements 4346 and have been recently shown to rely on the same physics for mapping motion 47. As implemented in this study, DENSE provided approximately 250 measurements of intramural contractile function per short axis slice -- an order of magnitude more measurements than conventional tagged MRI. Therefore, fitting the strain measurements to a predetermined model of the heart 48 was not necessary -- a significant advantage for the irregularly shaped heart in patients with HCM. Since a volumetric preparation is used to sensitize the image to motion, the method intrinsically avoids through-plane motion artifacts.

Regional wall motion assessment by cine MRI and echocardiography can potentially be misleading depending on whether one chooses to report percent wall thickening (i.e. transmural strain) or absolute systolic change in wall thickness (in mm). Percent wall thickening is inversely proportional to end diastolic wall thickness yet the average amount of wall thickening in mm remains normal or hypercontractile in the same hearts. However, the greatest hazard of interpreting percent wall thickening data is the extrapolation to infer the mechanisms leading to abnormalities in regional contractile function in HCM. High-resolution images of intramural systolic function can properly address this issue. The fact that LGE and intramural strain show abnormalities with different spatial distributions suggests that the information may be complementary. Larger studies will need to be performed to determine the prognostic significance of these findings.

Limitations

The current data do not address right ventricular involvement specifically since it was not possible to delineate the RV-LV border within the septum. Multi-slice analysis with appropriate statistical methods to correct for data dependence could have provided insight into intra-subject heterogeneity. However, single slice analysis was favored both for simplicity sake and for preserving the statistical significance lever, which degrades by testing multiple hypotheses (e.g. through the use of the Bonferroni correction). LGE images were acquired during diastole while DENSE images during systole. Despite all efforts to properly place the relevant regions of interest, some partial volume averaging may have influenced the results. Further histopathological studies are needed to shed light on how abnormalities by DENSE may indicate diffuse, interstitial fibrosis in visually-negative LGE regions.

Conclusions

In conclusion, just as high resolution LGE images allowed intramural assessments of myocardial infarction and fibrosis, high-resolution DENSE strain maps provide the most detailed view of intramural function obtained to date in patients with HCM. These results show that LGE as a measure of myocardial fibrosis does not fully explain the observed contractile heterogeneity in these patients. Direct visualization of an inner rim of preserved strain in the endocardium and mid-wall along with otherwise hypokinetic regions is a contractile pattern unique to HCM that has not been previously visualized with other methods.

Sources of Funding

This study was supported by the Intramural Research Program of the National Heart, Lung and Blood Institute at the National Institutes of Health.

Disclosures

None.

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Patient with confluent late gadolinium enhancement in the inferior septum which colocalizes with a severe focal abnormality in radial DENSE (see Results for details).

The diffuse pattern of late gadolinium enhancement seen in the anterior septum matches the contractile abnormality seen with DENSE (see Results for details).

Patient where the systolic strain deficit extends well beyond the two clearly defined confluent lesions on the late gadolinium enhanced images (see Results for details).

Patient with extensive systolic intramural strain abnormality despite minimal late gadolinium gadolinium enhancement (see Results for details).

Abnormal systolic strain is seen not only in areas of confluent and diffuse late gadolinium enhancement but also in the most hypertrophic non-enhanced segment. Intramural function is reduced irrespective of type or presence of late gadolinium enhancement pattern in hypertrophic segments indicating that myocardial scarring and interstitial fibrosis cannot predict the entire spectrum of functional abnormalities.

Signal intensities in late gadolinium enhancement images varied depending on presence and type of late gadolinium enhancement. Confluent and diffuse patterns had significantly higher signal intensity than normal myocardium. The signal intensity in the most hypertrophic non-enhancing segment was not significantly different from that of normal myocardium.

Left panel 7A: Irrespective of segmental end-diastolic thickness, the myocardium exhibits on average more than 3 mm absolute systolic change in wall thickness. Note that excluding the most hypertrophic segments, absolute systolic change in wall thickness is on average more than 6 mm. In normal subjects, >3 mm represents normal absolute systolic change in wall thickness. Right panel 7B: With increasing end-diastolic thickness the myocardium exhibits reduced percent systolic wall thickening, which is a measure of transmural systolic strain. This seems paradoxical given that these patients have preserved ejection fractions and fairly extensive left ventricular hypertrophy.

(Sample size per category was <6:572, 6–12:1272, 12–15:327, 15–20:449, 20–25:306, >25:134)

Gadolinium delayed enhancement does not fully explain the observed functional abnormalities. For segments with end-diastolic wall thickness (EDWTh) < 12mm percent wall thickening was inversely proportional to the extent of delayed enhancement. However, for segments with EDWTh ≥ 12mm, transmural percent wall thickening was depressed irrespective of the extent of gadolinium delayed enhancement.

Demographics, clinical and hemodynamic findings

PatientAgeGenderNYHASymptomsHCMPatternSAMLVOTGradientPCWPMutationEP inducibleArrhythmias, other findings
135F3CP, SOBASHNo1419BMHC, R403QNoSVT, AF
248M1NoneCONYes410NANA1st deg AVB, SVT
351F2SOBASHNo616NANoVT
450M3CP, SOBASHNo012NANASVT, VT
549F2CPASHNo2210BMHC, K847ENAPAT
666F2CP, SOBASHYes124NANAVT, Provocable LVOT obstruction
732F2SOBASHNo68NANA
841M1SOBASHNo09NANoVT
949F3CP, SOBASHNo514NANAAF, incomplete LBBB, VT
1023M1NoneASHNo88NANABrief run NSVT during EP testing, Negative holter
1127F1SOBASHYes129NANoNegative holter
1226M2CP, SOBASHNo07NANoNegative holter
1332M1NoneMIDNo208NANAProvocable LVOT obstruction
1415M1NoneASHNo011NANoProvocable RVOT obstruction
1533F3SOBASHNo026a trop, Val95AlaNA
1635M2CP, SOBASHYes10NANAVTAT, VT
1724F2CPASHYes10410NANAProvocable LVOT obstruction
1844M3CP, SOBASHNo010NANoVT
1934F2SOBASHYes620NANA
2049F3CP, SOBASHNo219BMHC, R403QNA
2152M2SOBCONNo010NANoTIA, Paroxysmal AF, NSVT
2219M1CPASHNoNANANANANear syncope while driving, Negative holter

NYHA = New York Heart Association classification; M = male; F = female; CP = Chest Pain; SOB = Shortness of Breath; HCM = Hypertrophic Cardiomyopathy; SAM = Systolic Anterior Motion of the mitral valve; LVOT = Left Ventricular Outflow Tract; RVOT = right ventricular outflow tract; EP = Electrophysiology; NA = not available; AF = atrial fibrillation; AVB = atrioventricular block; PAT = paroxysmal atrial tachycardia; VT = ventricular tachycardia; NSVT = non-sustained VT; TIA = transient ischemic attack

CMR findings

PatientMax WTh (mm)LGE (% of LV)LGE patternsStrain patternsLVEF (%)LV Mass (g)
11713.0ConfluentBoth65107
2285.1ConfluentEndo63567
3258.1DiffuseEndo67179
4239.9DiffuseTrans55240
5243.8DiffuseEndo73111
6224.3DiffuseEndo67129
72510.5BothBoth64107
82112.3BothEndo61192
9205.8ConfluentBoth74136
10282.2DiffuseEndo68190
11285.8DiffuseEndo72161
123314.6ConfluentEndo64219
132711.1DiffuseEndo59207
14282.2DiffuseEndo65267
15224.6ConfluentEndo73144
16345.5BothEndo73367
17333.5DiffuseEndo66263
182517.9BothEndo68135
19253.5ConfluentEndo65213
201712.5ConfluentEndo6276
212441.5ConfluentTrans53224
22211.8DiffuseEndo70167

LV = Left Ventricle; Max WTh = Maximum Wall Thickening; LGE = Late Gadolinium Enhancement; LVEF = Left Ventricular Ejection Fraction, Endo=endocardial, Trans=transmural.