Post on 01-Apr-2015
LV NoncompactionEchocardiography Conference
Connie TsaoJan 21, 2009
Terms
•Left ventricular noncompaction in association with congenital abnormalities
•Isolated left ventricular noncompaction▫Left ventricular hypertrabeculation▫Persistent myocardial sinusoids▫Spongy myocardium
Outline• Definitions• Embryology• Pathophysiology• Associations with other disease • Isolated LV noncompaction• Epidemiology• Genetics• Pathology• Clinical Features• Diagnosis
▫ Echocardiography▫ Cardiovascular magnetic resonance
• Prognosis• Management
Definition• Congenital heart
disease• Myocardial wall
distortion▫ Prominent trabeculae▫ Deep intertrabecular
recesses
• Continuity between LV cavity and recesses
• Primary cardiomyopathy in 2006 World Heath Organization classification
Ritter M et al, Mayo Clin Proc 1997
Early Embryology, <5 weeksAnterolateral
mesoderm
Epithelium
Endocardium Myocardium
N-Cadherin
Cardiac Tube
Trabeculations
Neuregulin growth factors
3 weeks
↓N-Cadherin
Embryology, 5-8 weeks
Endocardium
Sub-epicardial space
Microvessels coronary
circulation
Vascular endothelial growth factorAngiopoietin-1
Compaction• Base apex
• Epi- endocardium• Intratrabecular
recesses myocardial capillaries
Srivastava D, Nature 2000; and RP, Nature Rev Genetics 2002
Pathogenesis of Noncompaction•Arrest of endomyocardial morphogenesis•Potential pathological processes
preventing regression of sinusoids (Weiford et
al, Circ 2004):▫Pressure overload▫Ischemia
•Not proven
History
•First described in association with other congenital abnormalities▫Obstruction of LVOT/RVOT
Pulmonary atresia with intact ventricular septum
▫Complex cyanotic congenital heart disease▫Anomalous coronary arteries
•Intertrabecular recesses communicate with ventricular cavity and coronary circulationLauer RM et al, NEJM 1964Dusek J et al, Arch Pathol 1975
Ebstein Anomaly and Noncompaction
Bagur RH, et al. Circ 2008
… in association with other disease• Neuromuscular disorders• Metabolic disease• Genetic syndromes
▫Barth syndrome X-linked, dilated CMP, neutropenia, skeletal
myopathy, mitochondrial abnormalities, lactic acidosis
G4.5 gene in Xq28: encodes tafazzins proteins: acyltransferase functions in mitochondria, expressed in heart/muscle cells
▫Charcot-Marie-Tooth▫Nail-patella
Similar phenotypes
•Dilated cardiomyopathy•HCM•Restrictive cardiomyopathy•Left-dominant arrhythmogenic
cardiomyopathy▫42 patients with unexplained IL TWI,
arrhythmia of LV origin, and/or LDAC or familial myocardial fibrosis
▫5 patients fulfilled echocardiographic criteria for LVNC
Sen-Chowdhry S et al., JACC 2008
1st Report of Isolated Noncompaction
Epidemiology of Isolated LV Noncompaction
•Children Adults, elderly•0.05% (Ritter M et al, Mayo Clin Proc 1997)
▫37,555 echocardiograms 17 cases▫Prominent, excessive trabeculations
•0.014% (Oechslin EN et al, JACC 2000)
▫242,857 echocardiograms 34 cases▫Noncompacted/compacted ≥ 2:1
•Men >> women
Genetics
• Sporadic or familial• Familial in 18-50% (Oechslin et al, JACC 2000, Chin et al,
Circ 1990, Xing et al, Mol Genet Metab 2006)• Autosomal dominant with incomplete penetrance >
X-linked or autosomal recessive• G4.5 gene of Xq28 region (Bleyl SB et al, Am J Med Genet
1997): taffazin• α-dystrobrevin gene (Ichida F et al, Circ 2001)
▫Links cytoskeleton of myocytes to extracellular matrix• LIM domain binding protein 3/ZASP• Sarcomere genes: β myosin heavy chain (MYH7), α
cardiac actin (ACTC), cardiac troponin T (TNNT2) (Klaassen S et al., Circ 2008)
Pathology
Ritter et al, Mayo Clin Proc 1997
Jenni R et al, Heart 2001
Kaneda et al, Circ 2005
Cross section
Azan stain, fibrosis Van Gieson elastin stain
Ritter et al, Mayo Clin Proc 1997
Kaneda et al, Circ 2005
Clinical Features
•Heart failure▫Dyspnea▫Chest pain
•Arrhythmia▫Atrial fibrillation▫Ventricular tachycardia
•Thromboembolism▫CVA/TIA▫Pulmonary embolism
Heart Failure
Diastolic Systolic
• Restrictive hemodynamics on catheterization
• Initial presentation as restrictive cardiomyopathy
• Pathophysiology▫ Abnormal relaxation▫ Decreased compliance
due to volume of trabeculations
• No significant epicardial coronary disease
• Subendocardial hypoperfusion
• chronic microvascular ischemia
Ichida F et al, JACC 1999; Sen-Chowdhry et al, Curr Opin Card 2008
Microvascular dysfunctionThallium CMR- increased T2 signal
Hamamichi Y et al, Int J Cardiovas Imag 2001
Ichida F et al, JACC 1999
PET
Jenni R et al, Heart 2001
Jenni R et al, JACC 2002
Electrophysiology
• Atrial fibrillation• Ventricular tachycardia
ECG:• Left or right axis deviation• PR prolongation• Left ventricular hypertrophy• LBBB, RBBB, IVCD• Repolarization abnormalities• In pediatric population:
▫ Sinus bradycardia▫ WPW
Duru F et al, J Cardiovasc Electrophysiol 2000
LVH, T-wave abnormalities
McCrohon, J. A. et al. Circulation 2002;106:e22-e23
Thromboembolism• Stroke• TIA• Pulmonary embolus• Mesenteric infarction• Reported 21-38% • Etiology
▫ Stasis of blood in deep recesses/trabeculations
▫ Atrial fibrillation
Chin TK et al, Circ 1990Ritter M et al., Mayo Clin Proc 1997Oechslin E et al, JACC 2000
Oechslin et al, JACC 2000
Clinical Manifestations
• Largest comprehensive study in adults to date
• Review of all echocardiograms 1/84-12/98
• 34 adults with noncompaction
Oechslin et al, JACC 2000
Weiford et al, Circ 2004
Imaging for diagnosis
Chow C et al, Circ 2007
Diagnosis- Echocardiography I
• X/Y ≤ 0.5• Apex at end-diastole
▫ Subcostal▫ Apical 4Ch
0.59+0.05 0.20±0.040.92+0.07
Chin TK et al, Circ 1990
Diagnosis- Echocardiography II
• Compacted and noncompacted layers of ventricular wall▫ Thickened endocardial
layer▫ Prominent trabeculations▫ Deep recesses▫ Ratio noncompacted to
compacted >2:1▫ End-systole
• Trabecular meshwork in apex or midventricular segments of inferior and lateral wall Jenni R et al, Heart
2001
Noncompacted/ Compacted Ratio Mean±SD
Noncompacted/ Compacted RatioRange
Noncompaction (n=34)
3.5±0.8 2.3-5
Dilated CMP (n=10)
0.8±0.4 0.4-2.0
Hypertensive heart dz (n=9)
1.1±0.5 0.4-2.0
• All p <0.001 vs. noncompaction group • Autopsy validation in 7 of 34 noncompaction patients• Autopsy validation in all dilated cardiomyopathy patients
Jenni R et al, Heart 2001
Jenni R et al, Heart 2001
Jenni R et al, Heart 2001
Weiford et al, Circ 2004 Ichida F et al, JACC 1999
Diagnosis- Echocardiography III
•>3 trabeculations protruding from LV wall▫Apical to papillary muscles▫On single image plane
•Intertrabecular spaces in continuity with ventricular cavity▫Visualized on color doppler
Stollberger C et al, Am J Cardiol 2002
Validation of Jenni criteria
•Blinded retrospective review of records comparing patients with:▫LVNC (n=19)▫Dilated cardiomyopathy (n=31)▫Hypertensive heart disease (n=22)▫Chronic severe valvular disease (n=86)
Mitral regurgitation (n=22) Aortic regurgitation (n=20) Aortic stenosis (bi- and tri-leaflet valves,
n=44)Frischknecht B et al, J Am Soc Echocardiogr 2005
Frischknecht B et al, J Am Soc Echocardiogr 2005
Frischknecht B et al, J Am Soc Echocardiogr 2005
Accuracy of Combined Echocardiographic criteria
• 199 patients referred to heart failure clinic• Compared with 60 normal controls• Evaluated all 3 echo criteria• 47 patients (24%) fulfilled any echo criteria
▫Chin et al, 19%▫ Jenni et al, 15%▫Stollberger et al, 13%▫Combined: 7% fulfilled all 3 criteria
• 5 controls (8%) fulfilled echo criteria▫4 controls African-American
• Current criteria too sensitive?Kohli S et al, EHJ 2008
An underdiagnosed disease?•27 pediatric patients with noncompaction
(Ichida F et al, JACC 1999)
▫Diagnosis missed in 89% patients▫Alternative diagnoses: dilated cardiomyopathy,
apical hypertrophic cardiomyopathy, restrictive cardiomyopathy, myocarditis
• 17 adults identified with noncompaction of 37,555 echos screened (Ritter M et al., Mayo Clin Proc 1997)
▫Onset of symptoms to diagnosis: 3.5±5.7 years
Routine 2D TTE With Definity
Chow et al, Circ 2007
•7 patients with clinical noncompaction by echo or CMR (5M, 14-46 years)▫At least 1 of following: similar appearance in 1st
degree relatives, assoc neuromuscular d/o, thromboembolic disease, regional WMA
•Comparison to: Healthy volunteers (n=45), athletes (n=25), HCM (n=39), dilated CMP (n=14), Hypertensive heart dz (n=17), AS (n=30)
JACC 2005
Methods
•17 segment model▫Excluded true apex as thinner wall
•Noncompacted segment▫2 myocardial layers with different tissue
compaction▫Segment of most pronounced
trabeculations•Ratio of noncompacted to compacted
myocardium in diastole measured
• Healthy volunteers: 91% subjects w/ NC in apex, 78% mid, 21% base. • Most common anterior• Similar distribution in other groups
• Noncompaction patients significantly greater # segments involved (10±3) than all other groups
CMR criteria
• NC/C ratio >2.3 in diastole▫Sensitivity 86%▫Specificity 99%▫PPV 75%▫NPV 99%
Oechslin et al, JACC 2000
Weiford et al, Circ 2004
Not so poor prognosis?•45 patients referred for cardiomyopathy
▫28M, 17F▫37±17 yrs (13-83)▫Majority in NYHA Class I-II CHF (64%)▫20% NSVT, no sustained arrhythmias▫Medical rx:
60% anticoagulation for EF <25% or thromboembolism 90% ACE-I 47% beta blockers
▫At 46 month followup, 97% mean survival from death or transplantation
Murphy RT et al, EHJ 2005
• 65 pts with suspected noncompaction• 74% symptom-based referral, 26% asymptomatic• Followed for mean 46 ± 44 mos (6-193 mos)• Non-symptom group more benign characteristics
▫Younger, fewer ECG abnormalities, greater LVEF, lower left atrial size
• No difference in extent of noncompaction• No major CV events in asymptomatic group• 31% symptomatic group CV death, transplantation• Independent predictors of CV death, transplantation:
▫NYHA III-IV, ventricular arrhythmias, LA size
Management• Screening 1st degree family members• Treatment of heart failure
▫Medical rx: Improved LVEF, decreased LVM in infant rx with
carvedilol (Toyono M et al, Heart 2001)
▫Consideration of biventricular PPM/ICD• Screening for arrhythmias
▫Consideration of ICD• Anticoagulation
▫Atrial fibrillation and/or LVEF <40%• Heart transplantation
Conclusions
•Rare congenital heart disease thought to result from an arrest in early cardiac embryogenesis▫Genetic and sporadic forms
•Clinical manifestations:▫Heart failure▫Arrhythmias▫Thromboembolism
•Diagnosis by echocardiography or CMR▫Advances in imaging increased recognition
•Variable prognosis, likely long natural history•Treatment based on clinical manifestations