Affiliation:
1. Department of Cardio‐Thoraco‐Vascular Sciences and Public Health University of Padua Italy
2. Department of Medicine Institute of Radiology University of Padua Italy
3. Institute of Cardiovascular Science University College London London United Kingdom
Abstract
Background
This study assessed the prevalence of left ventricular (
LV
) involvement and characterized the clinical, electrocardiographic, and imaging features of
LV
phenotype in patients with arrhythmogenic right ventricular cardiomyopathy (
ARVC
). Differential diagnosis between
ARVC
‐
LV
phenotype and dilated cardiomyopathy (
DCM
) was evaluated.
Methods and Results
The study population included 87
ARVC
patients (median age 34 years) and 153
DCM
patients (median age 51 years). All underwent cardiac magnetic resonance with quantitative tissue characterization. Fifty‐eight
ARVC
patients (67%) had
LV
involvement, with both
LV
systolic dysfunction and
LV
late gadolinium enhancement (
LGE
) in 41/58 (71%) and
LV
‐
LGE
in isolation in 17 (29%). Compared with
DCM
, the
ARVC
‐
LV
phenotype was statistically significantly more often characterized by low
QRS
voltages in limb leads, T‐wave inversion in the inferolateral leads and major ventricular arrhythmias.
LV
‐
LGE
was found in all
ARVC
patients with
LV
systolic dysfunction and in 69/153 (45%) of
DCM
patients. Patients with
ARVC
and
LV
systolic dysfunction had a greater amount of
LV
‐
LGE
(25% versus 13% of
LV
mass;
P
<0.01), mostly localized in the subepicardial
LV
wall layers. An
LV
‐
LGE
≥20% had a 100% specificity for diagnosis of
ARVC
‐
LV
phenotype. An inverse correlation between
LV
ejection fraction and
LV
‐
LGE
extent was found in the
ARVC
‐
LV
phenotype (
r
=−0.63;
P
<0.01), but not in
DCM
(
r
=−0.01;
P
=0.94).
Conclusions
LV
involvement in
ARVC
is common and characterized by clinical and cardiac magnetic resonance features which differ from those seen in
DCM
. The most distinctive feature of
ARVC
‐
LV
phenotype is the large amount of
LV
‐
LGE
/fibrosis, which impacts directly and negatively on the
LV
systolic function.
Publisher
Ovid Technologies (Wolters Kluwer Health)
Subject
Cardiology and Cardiovascular Medicine
Cited by
107 articles.
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