Approach to patient with Dilated Cardiomyopathy
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Oct 18, 2017
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About This Presentation
Approach to patient with Dilated Cardiomyopathy
Slide Content
DCMDCM
An approach to Diagnosis and An approach to Diagnosis and
ManagementManagement
DR. MD. Saiful IslamDR. MD. Saiful Islam
MD (cardiology) Final part studentMD (cardiology) Final part student
Department of CardiologyDepartment of Cardiology
DMCHDMCH
An approach to Diagnosis and An approach to Diagnosis and
ManagementManagement
DR. MD. Saiful IslamDR. MD. Saiful Islam
MD (cardiology) Final part studentMD (cardiology) Final part student
Department of CardiologyDepartment of Cardiology
DMCHDMCH
CardiomyopathiesCardiomyopathies
Definition:Definition:
It is a heterogenous group of disease It is a heterogenous group of disease
of myocardium, of myocardium,
associated with mechanical or associated with mechanical or
electrical dysfunction,electrical dysfunction,
which is usually but not invariably which is usually but not invariably
exhibits inappropriate ventricular exhibits inappropriate ventricular
hypertrophy or dilation hypertrophy or dilation
& are due to variety of etiology that & are due to variety of etiology that
frequently are genetic.frequently are genetic.
Definition:Definition:
It is a heterogenous group of disease It is a heterogenous group of disease
of myocardium, of myocardium,
associated with mechanical or associated with mechanical or
electrical dysfunction,electrical dysfunction,
which is usually but not invariably which is usually but not invariably
exhibits inappropriate ventricular exhibits inappropriate ventricular
hypertrophy or dilation hypertrophy or dilation
& are due to variety of etiology that & are due to variety of etiology that
frequently are genetic.frequently are genetic.
WHO ClassificationWHO Classification
PrimaryPrimary
(those resulting from (those resulting from
genetic abnormalities genetic abnormalities
of cardiac muscle)of cardiac muscle)
–Dilated Dilated
–HypertrophicHypertrophic
–Restrictive Restrictive
Secondary Secondary
(those resulting from (those resulting from
infections, metabolic infections, metabolic
and nutritional diseases, and nutritional diseases,
endocrine disorders, endocrine disorders,
neuromuscular diseases, neuromuscular diseases,
blood diseases, tumors)blood diseases, tumors)
Br Heart J 1980; 44:672-673
Cardiomyopathies
PrimaryPrimary
(those resulting from (those resulting from
genetic abnormalities genetic abnormalities
of cardiac muscle)of cardiac muscle)
–Dilated Dilated
–HypertrophicHypertrophic
–Restrictive Restrictive
Secondary Secondary
(those resulting from (those resulting from
infections, metabolic infections, metabolic
and nutritional diseases, and nutritional diseases,
endocrine disorders, endocrine disorders,
neuromuscular diseases, neuromuscular diseases,
blood diseases, tumors)blood diseases, tumors)
Br Heart J 1980; 44:672-673
Cardiomyopathies
CardiomyopathyCardiomyopathy
WHO Classification
1.Dilated
•Enlarged
•Systolic dysfunction
2.Hypertrophic
•Thickened
•Diastolic dysfunction
3.Restrictive
•Diastolic dysfunction
3.Arrhythmogenic RV dysplasia
•Fibrofatty replacement
3.Unclassified
•Fibroelastosis
•LV noncompaction
Circ 93:841, 1996
WHO Classification
1.Dilated
•Enlarged
•Systolic dysfunction
2.Hypertrophic
•Thickened
•Diastolic dysfunction
3.Restrictive
•Diastolic dysfunction
3.Arrhythmogenic RV dysplasia
•Fibrofatty replacement
3.Unclassified
•Fibroelastosis
•LV noncompaction
Circ 93:841, 1996
ACC/AHA classificationACC/AHA classification
Dilated CardiomyopathyDilated Cardiomyopathy
•Dilation and impaired contraction of ventricles:
•Reduced systolic function with or without heart failure
•Characterized by myocyte damage
•Multiple etiologies with similar resultant pathophysiology
•Majority of cases are idiopathic
•In 20-50 % of cases, the disease is recognized as familial.
•Autosomal dominant inheritance is most commonly
encountered and mutations in several cardiac structural or
metabolic genes have been identified.
•
•Dilation and impaired contraction of ventricles:
•Reduced systolic function with or without heart failure
•Characterized by myocyte damage
•Multiple etiologies with similar resultant pathophysiology
•Majority of cases are idiopathic
•In 20-50 % of cases, the disease is recognized as familial.
•Autosomal dominant inheritance is most commonly
encountered and mutations in several cardiac structural or
metabolic genes have been identified.
•
DCMDCM
Main features:
dilatation of both
ventricles and atria
Mural thrombi are
frequently present
in LV
Scarring of the
mitral
and tricuspid
leaflets
and secondary
dilatation of their
Annuli
Reduced systolic
function
Main features:
dilatation of both
ventricles and atria
Mural thrombi are
frequently present
in LV
Scarring of the
mitral
and tricuspid
leaflets
and secondary
dilatation of their
Annuli
Reduced systolic
function
DCM: EtiologyDCM: Etiology
Idiopathic
Myocarditis
Ischemic
Infiltrative
Peripartum
Hypertension
Valvular
Familial
Inflammatory
Infectious
Viral – picornovirus, Cox B, CMV, HIV
Ricketsial - Lyme Disease
Parasitic - Chagas’ Disease, Toxoplasmosis
Non-infectious
Collagen Vascular Disease (SLE, RA)
Toxic
Alcohol, Anthracyclins (adriamycin), Cocaine
Metabolic
Endocrine –thyroid dz, pheochromocytoma, DM, acromegaly,
Nutritional
Thiamine, selenium, carnitine
Neuromuscular (Duchene’s Muscular Dystrophy--x-linked)
Idiopathic
Myocarditis
Ischemic
Infiltrative
Peripartum
Hypertension
Valvular
Familial
Inflammatory
Infectious
Viral – picornovirus, Cox B, CMV, HIV
Ricketsial - Lyme Disease
Parasitic - Chagas’ Disease, Toxoplasmosis
Non-infectious
Collagen Vascular Disease (SLE, RA)
Toxic
Alcohol, Anthracyclins (adriamycin), Cocaine
Metabolic
Endocrine –thyroid dz, pheochromocytoma, DM, acromegaly,
Nutritional
Thiamine, selenium, carnitine
Neuromuscular (Duchene’s Muscular Dystrophy--x-linked)
ETIOLOGIES OF DILATED CARDIOMYOPATHYETIOLOGIES OF DILATED CARDIOMYOPATHY
0
5
10
15
20
25
30
35
40
45
50
Disorder
IDCM
Myocarditis
Ischmic CM
Infiltrative
disease
Peripartum CM
Hypertension
HIV
CTD
Substance
abuse
Felker et al NEJM 2000
0
5
10
15
20
25
30
35
40
45
50
Disorder
IDCM
Myocarditis
Ischmic CM
Infiltrative
disease
Peripartum CM
Hypertension
HIV
CTD
Substance
abuse
Felker et al NEJM 2000
GeneticsGenetics
Some cardiomyopathies are monogenic disorders
Primary genetic – HCM, ARVC, LVNC
Mixed etiology – DCM (20-40 %), RCM (rare)
Great variability of genotype and phenotype
Hundreds and thousands of mutations
Many genes
Various types of inheritence
Different phenotypes in identical mutations
Some cardiomyopathies are monogenic disorders
Primary genetic – HCM, ARVC, LVNC
Mixed etiology – DCM (20-40 %), RCM (rare)
Great variability of genotype and phenotype
Hundreds and thousands of mutations
Many genes
Various types of inheritence
Different phenotypes in identical mutations
MOLECULAR DEFECTS IN DILATED MOLECULAR DEFECTS IN DILATED
CARDIOMYOPATHYCARDIOMYOPATHY
Fatkin D, et al. NEJM 1999;341Fatkin D, et al. NEJM 1999;341
GENES
Dystrophin
Desmin
Vinculin
Titin
Troponin-T
α-tropomyosin
ß-myosin heavy chain
Actin
Mitochondrial DNA
mutations
CARDIOMYOPATHYCARDIOMYOPATHY
Fatkin D, et al. NEJM 1999;341Fatkin D, et al. NEJM 1999;341
GENES
Dystrophin
Desmin
Vinculin
Titin
Troponin-T
α-tropomyosin
ß-myosin heavy chain
Actin
Mitochondrial DNA
mutations
Pathogenisis :DCMPathogenisis :DCM
PathophysiologyPathophysiology
Mutation Exogenous
insult
Contraction and relaxation
disorder
Ineffective energy utilization
Altered Ca ions handling
Activation of compensatory
neurohumoral mechanisms
Apoptosis
Fibrosis
Hypertrophy
Heart
failure
Arrhythmia, sudden
death
Thromboembolic
complication
Mutation Exogenous
insult
Contraction and relaxation
disorder
Ineffective energy utilization
Altered Ca ions handling
Activation of compensatory
neurohumoral mechanisms
Apoptosis
Fibrosis
Hypertrophy
Heart
failure
Arrhythmia, sudden
death
Thromboembolic
complication
PathophysiologyPathophysiology
•Initial Compensation for impaired myocyte contractility:
•Frank-Starling mechanism
•Neurohumoral activation
" intravascular volume
•Eventual decompensation
•ventricular remodeling
•myocyte death/apoptosis
•valvular regurgitation
•Initial Compensation for impaired myocyte contractility:
•Frank-Starling mechanism
•Neurohumoral activation
" intravascular volume
•Eventual decompensation
•ventricular remodeling
•myocyte death/apoptosis
•valvular regurgitation
Physiologic Physiologic
consequencesconsequences
consequencesconsequences
• Failure of the LV causes an increase in end-diastolicFailure of the LV causes an increase in end-diastolic
volume, which results in increase in LA, pulmonary volume, which results in increase in LA, pulmonary
venous and pulmonary capillary pressure. venous and pulmonary capillary pressure.
Mitral valve regurgitation may result from papillary muscle Mitral valve regurgitation may result from papillary muscle
dysfunction or severe dilatation of the valve annulus. dysfunction or severe dilatation of the valve annulus.
Idiopathic
Dilated
Cardiomyopathy
volume, which results in increase in LA, pulmonary volume, which results in increase in LA, pulmonary
venous and pulmonary capillary pressure. venous and pulmonary capillary pressure.
Mitral valve regurgitation may result from papillary muscle Mitral valve regurgitation may result from papillary muscle
dysfunction or severe dilatation of the valve annulus. dysfunction or severe dilatation of the valve annulus.
Idiopathic
Dilated
Cardiomyopathy
IDCMIDCM
EPIDEMIOLOGYEPIDEMIOLOGY
ANNUAL INCIDENCEANNUAL INCIDENCE 5- 8/100,0005- 8/100,000
INCREASED RISK ASSOCIATED WITH:INCREASED RISK ASSOCIATED WITH:
–MALE GENDERMALE GENDER
–BLACK RACEBLACK RACE
–HYPERTENSIONHYPERTENSION
–CHRONIC BETA-AGONIST USECHRONIC BETA-AGONIST USE
EPIDEMIOLOGYEPIDEMIOLOGY
ANNUAL INCIDENCEANNUAL INCIDENCE 5- 8/100,0005- 8/100,000
INCREASED RISK ASSOCIATED WITH:INCREASED RISK ASSOCIATED WITH:
–MALE GENDERMALE GENDER
–BLACK RACEBLACK RACE
–HYPERTENSIONHYPERTENSION
–CHRONIC BETA-AGONIST USECHRONIC BETA-AGONIST USE
IDCMIDCM
PATHOGENESISPATHOGENESIS
Familial/genetic factorsFamilial/genetic factors
Viral myocarditis and cytotoxic insultsViral myocarditis and cytotoxic insults
Immunologic abnormalitiesImmunologic abnormalities
–Beta-receptor auto-antibodiesBeta-receptor auto-antibodies
–Abnormal T-cell functionAbnormal T-cell function
Metabolic, energetic, and contractile Metabolic, energetic, and contractile
abnormalitiesabnormalities
CaCa
2+2+
-ATPase-ATPase
Myofibrillar ATPaseMyofibrillar ATPase
Creatine KinaseCreatine Kinase
PATHOGENESISPATHOGENESIS
Familial/genetic factorsFamilial/genetic factors
Viral myocarditis and cytotoxic insultsViral myocarditis and cytotoxic insults
Immunologic abnormalitiesImmunologic abnormalities
–Beta-receptor auto-antibodiesBeta-receptor auto-antibodies
–Abnormal T-cell functionAbnormal T-cell function
Metabolic, energetic, and contractile Metabolic, energetic, and contractile
abnormalitiesabnormalities
CaCa
2+2+
-ATPase-ATPase
Myofibrillar ATPaseMyofibrillar ATPase
Creatine KinaseCreatine Kinase
IDCMIDCM
Pathological consequencePathological consequence
Four chamber dilatationFour chamber dilatation
Varying degrees of interstitial fibrosis and Varying degrees of interstitial fibrosis and
myocyte hypertrophymyocyte hypertrophy
““Functional” atrioventricular regurgitation is Functional” atrioventricular regurgitation is
commoncommon
Normal epicardial coronary arteriesNormal epicardial coronary arteries
Pathological consequencePathological consequence
Four chamber dilatationFour chamber dilatation
Varying degrees of interstitial fibrosis and Varying degrees of interstitial fibrosis and
myocyte hypertrophymyocyte hypertrophy
““Functional” atrioventricular regurgitation is Functional” atrioventricular regurgitation is
commoncommon
Normal epicardial coronary arteriesNormal epicardial coronary arteries
IDCMIDCM
PATHOLOGIC FINDINGSPATHOLOGIC FINDINGS
PATHOLOGIC FINDINGSPATHOLOGIC FINDINGS
IDCMIDCM
CLINICAL PRESENTATIONSCLINICAL PRESENTATIONS
Heart failure symptomsHeart failure symptoms 75%-85%75%-85%
Anginal chest painAnginal chest pain 8%-20% 8%-20%
Emboli Emboli (systemic or pulmonary)(systemic or pulmonary) 1%-4%1%-4%
SyncopeSyncope <1% <1%
Sudden cardiac deathSudden cardiac death <1% <1%
CLINICAL PRESENTATIONSCLINICAL PRESENTATIONS
Heart failure symptomsHeart failure symptoms 75%-85%75%-85%
Anginal chest painAnginal chest pain 8%-20% 8%-20%
Emboli Emboli (systemic or pulmonary)(systemic or pulmonary) 1%-4%1%-4%
SyncopeSyncope <1% <1%
Sudden cardiac deathSudden cardiac death <1% <1%
DCM: FamilialDCM: Familial
30% of ‘idiopathic’30% of ‘idiopathic’
Inheritance patternsInheritance patterns
–Autosommal dom/rec, x-linked, mitochondrial Autosommal dom/rec, x-linked, mitochondrial
mutationmutation
DiagnosisDiagnosis
–Three generation family history Three generation family history is essential for is essential for
diagnosisdiagnosis
–Screening of family member & genetic testing Screening of family member & genetic testing
Mechanism:Mechanism:
–Abnormalities in:Abnormalities in:
Energy productionEnergy production
Contractile force generationContractile force generation
–Specific genes coding for:Specific genes coding for:
Myosin, actin, dystophinMyosin, actin, dystophin
30% of ‘idiopathic’30% of ‘idiopathic’
Inheritance patternsInheritance patterns
–Autosommal dom/rec, x-linked, mitochondrial Autosommal dom/rec, x-linked, mitochondrial
mutationmutation
DiagnosisDiagnosis
–Three generation family history Three generation family history is essential for is essential for
diagnosisdiagnosis
–Screening of family member & genetic testing Screening of family member & genetic testing
Mechanism:Mechanism:
–Abnormalities in:Abnormalities in:
Energy productionEnergy production
Contractile force generationContractile force generation
–Specific genes coding for:Specific genes coding for:
Myosin, actin, dystophinMyosin, actin, dystophin
DCM : IschemicDCM : Ischemic
Defined as -cardiomyopathy in the Defined as -cardiomyopathy in the
presence of:presence of:
–Prior extensive myocardial infractionPrior extensive myocardial infraction
–Severe coronary artery diseaseSevere coronary artery disease
ICM- ICM- causes 60% to 70% cases of systolic causes 60% to 70% cases of systolic
heart failure in industrilized countriesheart failure in industrilized countries
Defined as -cardiomyopathy in the Defined as -cardiomyopathy in the
presence of:presence of:
–Prior extensive myocardial infractionPrior extensive myocardial infraction
–Severe coronary artery diseaseSevere coronary artery disease
ICM- ICM- causes 60% to 70% cases of systolic causes 60% to 70% cases of systolic
heart failure in industrilized countriesheart failure in industrilized countries
DCM: PeripartumDCM: Peripartum
Diagnostic CriteriaDiagnostic Criteria
1 mo pre, 5 mos post1 mo pre, 5 mos post
Echo: LV dysfunction Echo: LV dysfunction
–LVEF < 45% LVEF < 45%
–FS < 30%FS < 30%
EpidemiologyEpidemiology
1:4000 women1:4000 women
–JAMA 2000;283:1183JAMA 2000;283:1183
Proposed mechanisms: Proposed mechanisms:
–Inflammatory Cytokines: Inflammatory Cytokines:
TNFa, IL6TNFa, IL6
–JACC 2000 35(3):701.JACC 2000 35(3):701.
Diagnostic CriteriaDiagnostic Criteria
1 mo pre, 5 mos post1 mo pre, 5 mos post
Echo: LV dysfunction Echo: LV dysfunction
–LVEF < 45% LVEF < 45%
–FS < 30%FS < 30%
EpidemiologyEpidemiology
1:4000 women1:4000 women
–JAMA 2000;283:1183JAMA 2000;283:1183
Proposed mechanisms: Proposed mechanisms:
–Inflammatory Cytokines: Inflammatory Cytokines:
TNFa, IL6TNFa, IL6
–JACC 2000 35(3):701.JACC 2000 35(3):701.
DCM: toxicDCM: toxic
Alcoholic cardiomyopathyAlcoholic cardiomyopathy
Chronic useChronic use
Reversible with abstinenceReversible with abstinence
Continued use is associated with a 3 Continued use is associated with a 3
to 6 year mortility excedding 50%to 6 year mortility excedding 50%
Mechanism?:Mechanism?:
–Directly inhibits:Directly inhibits:
mitochondrial oxidative phosphorylationmitochondrial oxidative phosphorylation
Fatty acid oxidationFatty acid oxidation
– Myocyte cell death and fibrosisMyocyte cell death and fibrosis
Alcoholic cardiomyopathyAlcoholic cardiomyopathy
Chronic useChronic use
Reversible with abstinenceReversible with abstinence
Continued use is associated with a 3 Continued use is associated with a 3
to 6 year mortility excedding 50%to 6 year mortility excedding 50%
Mechanism?:Mechanism?:
–Directly inhibits:Directly inhibits:
mitochondrial oxidative phosphorylationmitochondrial oxidative phosphorylation
Fatty acid oxidationFatty acid oxidation
– Myocyte cell death and fibrosisMyocyte cell death and fibrosis
DCM: InfectiousDCM: Infectious
Acute viral myocarditisAcute viral myocarditis
Coxasackie B or echovirusCoxasackie B or echovirus
Self-limited infection in young peopleSelf-limited infection in young people
Mechanism?:Mechanism?:
–Myocyte cell death and fibrosisMyocyte cell death and fibrosis
–Immune mediated cell injuryImmune mediated cell injury
Acute viral myocarditisAcute viral myocarditis
Coxasackie B or echovirusCoxasackie B or echovirus
Self-limited infection in young peopleSelf-limited infection in young people
Mechanism?:Mechanism?:
–Myocyte cell death and fibrosisMyocyte cell death and fibrosis
–Immune mediated cell injuryImmune mediated cell injury
Difference betweenDifference between
DCM and ICMDCM and ICM
DCMDCM
1.1.Global hypokinesiaGlobal hypokinesia
2.2.RWMA and the RWMA and the
coronary territory coronary territory
do not conformdo not conform
3.3.Dyskinesia not Dyskinesia not
seenseen
4.4.RV involvement is RV involvement is
oftenoften
ICMICM
1.1.Regional Regional
hypokinesiahypokinesia
2.2.RWMA follows RWMA follows
coronary territorycoronary territory
3.3.Dyskinesia is seenDyskinesia is seen
4.4.RV involvement is RV involvement is
rarerare
DCM and ICMDCM and ICM
DCMDCM
1.1.Global hypokinesiaGlobal hypokinesia
2.2.RWMA and the RWMA and the
coronary territory coronary territory
do not conformdo not conform
3.3.Dyskinesia not Dyskinesia not
seenseen
4.4.RV involvement is RV involvement is
oftenoften
ICMICM
1.1.Regional Regional
hypokinesiahypokinesia
2.2.RWMA follows RWMA follows
coronary territorycoronary territory
3.3.Dyskinesia is seenDyskinesia is seen
4.4.RV involvement is RV involvement is
rarerare
Diagnosis of DCMDiagnosis of DCM
HistoryHistory
Clinical examinationClinical examination
Chest x-rayChest x-ray
12-lead ECG12-lead ECG
Echocardiography Echocardiography
Blood testsBlood tests
Family screening and genetic testingFamily screening and genetic testing
Endomyocardial biopsyEndomyocardial biopsy
Cardiac CT ScanCardiac CT Scan //
MRI (magnetic resonance imaging)MRI (magnetic resonance imaging)
Cardiac catheterizationCardiac catheterization
HistoryHistory
Clinical examinationClinical examination
Chest x-rayChest x-ray
12-lead ECG12-lead ECG
Echocardiography Echocardiography
Blood testsBlood tests
Family screening and genetic testingFamily screening and genetic testing
Endomyocardial biopsyEndomyocardial biopsy
Cardiac CT ScanCardiac CT Scan //
MRI (magnetic resonance imaging)MRI (magnetic resonance imaging)
Cardiac catheterizationCardiac catheterization
Associated history with Associated history with
DCMDCM
Alcohol consumptionAlcohol consumption
Peripartum statusPeripartum status
IHDIHD
MalnutritionMalnutrition
Hereditary involvement-3 generation Hereditary involvement-3 generation
of family history is essentialof family history is essential
Diabetes mellitusDiabetes mellitus
Endocrine disorder(thyroid)Endocrine disorder(thyroid)
Valvular disorder( eg. AR , MR)Valvular disorder( eg. AR , MR)
DCMDCM
Alcohol consumptionAlcohol consumption
Peripartum statusPeripartum status
IHDIHD
MalnutritionMalnutrition
Hereditary involvement-3 generation Hereditary involvement-3 generation
of family history is essentialof family history is essential
Diabetes mellitusDiabetes mellitus
Endocrine disorder(thyroid)Endocrine disorder(thyroid)
Valvular disorder( eg. AR , MR)Valvular disorder( eg. AR , MR)
Clinical ManifestationsClinical Manifestations
Symptoms:Symptoms:
All age group may be affectedAll age group may be affected
May be asymptomatic May be asymptomatic
The onset is insidious, but sometimes symptoms of heart The onset is insidious, but sometimes symptoms of heart
failure occur suddenlyfailure occur suddenly
DyspneaDyspnea
PalpitationPalpitation
Chest painChest pain
Dizziness and syncopeDizziness and syncope
CVA,Hemiplegia,ParaplegiaCVA,Hemiplegia,Paraplegia
Systemic embolismSystemic embolism
Infants and younger children have Infants and younger children have respiratory symptoms respiratory symptoms
and failure to thriveand failure to thrive. .
Symptoms:Symptoms:
All age group may be affectedAll age group may be affected
May be asymptomatic May be asymptomatic
The onset is insidious, but sometimes symptoms of heart The onset is insidious, but sometimes symptoms of heart
failure occur suddenlyfailure occur suddenly
DyspneaDyspnea
PalpitationPalpitation
Chest painChest pain
Dizziness and syncopeDizziness and syncope
CVA,Hemiplegia,ParaplegiaCVA,Hemiplegia,Paraplegia
Systemic embolismSystemic embolism
Infants and younger children have Infants and younger children have respiratory symptoms respiratory symptoms
and failure to thriveand failure to thrive. .
Clinical ManifestationsClinical Manifestations
Signs:Signs:
Pulse : Sinus tachycardia, Irregular in AF or in Pulse : Sinus tachycardia, Irregular in AF or in
extrasystol, Bradycardia in CHBextrasystol, Bradycardia in CHB
BP : Low BP , Narrow pulse pressureBP : Low BP , Narrow pulse pressure
JVP : ElevatedJVP : Elevated
Precordium:Precordium:
–Apex shifted, forceful and ill sustainedApex shifted, forceful and ill sustained
–S2 may be palpable due to PHS2 may be palpable due to PH
–May be parasternal liftMay be parasternal lift
–On auscultation:S1 and S2 soft, S2 loud from PH On auscultation:S1 and S2 soft, S2 loud from PH
, Pansystolic murmur at mitral and tricuspid , Pansystolic murmur at mitral and tricuspid
area,S3 and S4 are common area,S3 and S4 are common
Signs:Signs:
Pulse : Sinus tachycardia, Irregular in AF or in Pulse : Sinus tachycardia, Irregular in AF or in
extrasystol, Bradycardia in CHBextrasystol, Bradycardia in CHB
BP : Low BP , Narrow pulse pressureBP : Low BP , Narrow pulse pressure
JVP : ElevatedJVP : Elevated
Precordium:Precordium:
–Apex shifted, forceful and ill sustainedApex shifted, forceful and ill sustained
–S2 may be palpable due to PHS2 may be palpable due to PH
–May be parasternal liftMay be parasternal lift
–On auscultation:S1 and S2 soft, S2 loud from PH On auscultation:S1 and S2 soft, S2 loud from PH
, Pansystolic murmur at mitral and tricuspid , Pansystolic murmur at mitral and tricuspid
area,S3 and S4 are common area,S3 and S4 are common
Other peripheral signs:Other peripheral signs:
Liver : Enlarged , tender and pulsatileLiver : Enlarged , tender and pulsatile
Edama : at dependent partEdama : at dependent part
Lung base: Basal crepitationLung base: Basal crepitation
Others: Signs of systemic and Others: Signs of systemic and
pulmonary embolism may be foundpulmonary embolism may be found
Liver : Enlarged , tender and pulsatileLiver : Enlarged , tender and pulsatile
Edama : at dependent partEdama : at dependent part
Lung base: Basal crepitationLung base: Basal crepitation
Others: Signs of systemic and Others: Signs of systemic and
pulmonary embolism may be foundpulmonary embolism may be found
ACC/AHA HEART FAILURE EVALUATION GUIDELINESACC/AHA HEART FAILURE EVALUATION GUIDELINES
CLASS I & II RECOMMENDATIONSCLASS I & II RECOMMENDATIONS
Laboratory StudiesLaboratory Studies
–Blood count, urinalysis, electrolytes, renal function, Blood count, urinalysis, electrolytes, renal function,
glucose, LFTs glucose, LFTs (class I; level C)(class I; level C)
–Thyroid stimulating hormone Thyroid stimulating hormone (class I; level C)(class I; level C)
–Fe/TIBC, ferritin Fe/TIBC, ferritin (class IIa, level C)(class IIa, level C)
–Urinary screening for hemochromatosis Urinary screening for hemochromatosis (class IIa; (class IIa;
level C)level C)
–Measurement of ANA, rheumatoid factor, urinary Measurement of ANA, rheumatoid factor, urinary
VMA and metanepherines in selected patients VMA and metanepherines in selected patients
(class IIa; level C)(class IIa; level C)
–HIV testingHIV testing (class IIb; level C) (class IIb; level C)
Electrocardiogram Electrocardiogram (class I; level C)(class I; level C)
Chest x-ray Chest x-ray (class I; level C)(class I; level C)
Echocardiogram/Doppler or radioventriculogram Echocardiogram/Doppler or radioventriculogram (class (class
I;level C)I;level C)
-Adapted from Hunt SA et al. Circulation 2001;104:2996-3007
CLASS I & II RECOMMENDATIONSCLASS I & II RECOMMENDATIONS
Laboratory StudiesLaboratory Studies
–Blood count, urinalysis, electrolytes, renal function, Blood count, urinalysis, electrolytes, renal function,
glucose, LFTs glucose, LFTs (class I; level C)(class I; level C)
–Thyroid stimulating hormone Thyroid stimulating hormone (class I; level C)(class I; level C)
–Fe/TIBC, ferritin Fe/TIBC, ferritin (class IIa, level C)(class IIa, level C)
–Urinary screening for hemochromatosis Urinary screening for hemochromatosis (class IIa; (class IIa;
level C)level C)
–Measurement of ANA, rheumatoid factor, urinary Measurement of ANA, rheumatoid factor, urinary
VMA and metanepherines in selected patients VMA and metanepherines in selected patients
(class IIa; level C)(class IIa; level C)
–HIV testingHIV testing (class IIb; level C) (class IIb; level C)
Electrocardiogram Electrocardiogram (class I; level C)(class I; level C)
Chest x-ray Chest x-ray (class I; level C)(class I; level C)
Echocardiogram/Doppler or radioventriculogram Echocardiogram/Doppler or radioventriculogram (class (class
I;level C)I;level C)
-Adapted from Hunt SA et al. Circulation 2001;104:2996-3007
ECG Finding:ECG Finding:
Sinus tachycardia, BradycardiaSinus tachycardia, Bradycardia
Low voltage ECGLow voltage ECG
LVHLVH
Rt or Lt Atrial hypertrophyRt or Lt Atrial hypertrophy
Atrial or Ventricular arrythmia Atrial or Ventricular arrythmia
Pseudo infraction pattern(Deep but narrow ‘q’ Pseudo infraction pattern(Deep but narrow ‘q’
suggestive of antero-septal MI)suggestive of antero-septal MI)
Shallow invesion of ‘T’ wave Shallow invesion of ‘T’ wave
LBBB, RBBB ,LAHB, LPHB, Bifascicular or LBBB, RBBB ,LAHB, LPHB, Bifascicular or
Trifascicular blockTrifascicular block
AV block( 1’or 2’ or 3’degree)AV block( 1’or 2’ or 3’degree)
Sinus tachycardia, BradycardiaSinus tachycardia, Bradycardia
Low voltage ECGLow voltage ECG
LVHLVH
Rt or Lt Atrial hypertrophyRt or Lt Atrial hypertrophy
Atrial or Ventricular arrythmia Atrial or Ventricular arrythmia
Pseudo infraction pattern(Deep but narrow ‘q’ Pseudo infraction pattern(Deep but narrow ‘q’
suggestive of antero-septal MI)suggestive of antero-septal MI)
Shallow invesion of ‘T’ wave Shallow invesion of ‘T’ wave
LBBB, RBBB ,LAHB, LPHB, Bifascicular or LBBB, RBBB ,LAHB, LPHB, Bifascicular or
Trifascicular blockTrifascicular block
AV block( 1’or 2’ or 3’degree)AV block( 1’or 2’ or 3’degree)
ECGECG
X-rayX-ray
Cardiomegally ,simulting pericardial effusion Cardiomegally ,simulting pericardial effusion
or multi vaivular disease or Ischemic or multi vaivular disease or Ischemic
cardiomyupathycardiomyupathy
Pulmonary edema with Kerley’ B linePulmonary edema with Kerley’ B line
Pleural effusion may be present Pleural effusion may be present
Pulmonary infraction is not uncommonPulmonary infraction is not uncommon
Usually no LA enlargement so single right Usually no LA enlargement so single right
border. No calcified valve and normal aortaborder. No calcified valve and normal aorta
Cardiomegally ,simulting pericardial effusion Cardiomegally ,simulting pericardial effusion
or multi vaivular disease or Ischemic or multi vaivular disease or Ischemic
cardiomyupathycardiomyupathy
Pulmonary edema with Kerley’ B linePulmonary edema with Kerley’ B line
Pleural effusion may be present Pleural effusion may be present
Pulmonary infraction is not uncommonPulmonary infraction is not uncommon
Usually no LA enlargement so single right Usually no LA enlargement so single right
border. No calcified valve and normal aortaborder. No calcified valve and normal aorta
X-rayX-ray
EchocardiographyEchocardiography
Typical FeaturesTypical Features
2D Echo of DCM2D Echo of DCM
1.1.All four chambers are dilatedAll four chambers are dilated
2.2. LV wall thin with hypokinesiaLV wall thin with hypokinesia
M mode echo of DCMM mode echo of DCM
1.1.Valve-Normal in morphology with reduced excursionValve-Normal in morphology with reduced excursion
2.2. EPSS is increasedEPSS is increased
3.3. Mitral valve shows Penguin appearance in the sea shore Mitral valve shows Penguin appearance in the sea shore
Color dopplerColor doppler
1.1. Functional MR and TR with trivial ARFunctional MR and TR with trivial AR
Comment : DCMComment : DCM
Typical FeaturesTypical Features
2D Echo of DCM2D Echo of DCM
1.1.All four chambers are dilatedAll four chambers are dilated
2.2. LV wall thin with hypokinesiaLV wall thin with hypokinesia
M mode echo of DCMM mode echo of DCM
1.1.Valve-Normal in morphology with reduced excursionValve-Normal in morphology with reduced excursion
2.2. EPSS is increasedEPSS is increased
3.3. Mitral valve shows Penguin appearance in the sea shore Mitral valve shows Penguin appearance in the sea shore
Color dopplerColor doppler
1.1. Functional MR and TR with trivial ARFunctional MR and TR with trivial AR
Comment : DCMComment : DCM
EchocardiographyEchocardiography
INDICATIONS FOR ENDOMYOCARDIAL INDICATIONS FOR ENDOMYOCARDIAL
BIOPSYBIOPSY
AcuteAcute dilated cardiomyopathy with dilated cardiomyopathy with refractory heart refractory heart
failure failure symptomssymptoms
Rapidly progressive Rapidly progressive ventricular dysfunction in an ventricular dysfunction in an
unexplained unexplained cardiomyopathy of cardiomyopathy of recent onsetrecent onset
New onset New onset cardiomyopathy with cardiomyopathy with recurrentrecurrent ventricular ventricular
tachycardia or high grade heart blocktachycardia or high grade heart block
Heart failure in the setting of fever, rash, and peripheral Heart failure in the setting of fever, rash, and peripheral
eosinophiliaeosinophilia
Dilated cardiomyopathy in setting of Dilated cardiomyopathy in setting of systemic diseases systemic diseases
known to affect the myocardium known to affect the myocardium (systemic lupus (systemic lupus
erythematosus, polymyositis, sarcoidosis)erythematosus, polymyositis, sarcoidosis)
Wu LA, et al. Mayo Clin Proc 2001;76:1030-8
BIOPSYBIOPSY
AcuteAcute dilated cardiomyopathy with dilated cardiomyopathy with refractory heart refractory heart
failure failure symptomssymptoms
Rapidly progressive Rapidly progressive ventricular dysfunction in an ventricular dysfunction in an
unexplained unexplained cardiomyopathy of cardiomyopathy of recent onsetrecent onset
New onset New onset cardiomyopathy with cardiomyopathy with recurrentrecurrent ventricular ventricular
tachycardia or high grade heart blocktachycardia or high grade heart block
Heart failure in the setting of fever, rash, and peripheral Heart failure in the setting of fever, rash, and peripheral
eosinophiliaeosinophilia
Dilated cardiomyopathy in setting of Dilated cardiomyopathy in setting of systemic diseases systemic diseases
known to affect the myocardium known to affect the myocardium (systemic lupus (systemic lupus
erythematosus, polymyositis, sarcoidosis)erythematosus, polymyositis, sarcoidosis)
Wu LA, et al. Mayo Clin Proc 2001;76:1030-8
RIGHT
VENTRICULAR
BIOPSY
ENDOMYOCARDIAL BIOPSY IN DILATED
CARDIOMYOPATHY
VENTRICULAR
BIOPSY
ENDOMYOCARDIAL BIOPSY IN DILATED
CARDIOMYOPATHY
NON-INVASIVE EVALUATION OF MYOCARDITISNON-INVASIVE EVALUATION OF MYOCARDITIS
MRI IMAGINGMRI IMAGING
Friedrich MG et al. Circulation 1998;97:1802-9.
EnhancedEnhanced
MRI IMAGINGMRI IMAGING
Friedrich MG et al. Circulation 1998;97:1802-9.
EnhancedEnhanced
INDICATIONS FORINDICATIONS FOR CORONARY ANGIOGRAPHY IN CORONARY ANGIOGRAPHY IN
NEW ONSET CARDIOMYOPATHYNEW ONSET CARDIOMYOPATHY
ACC/AHA CONSENSUS GUIDELINES ACC/AHA CONSENSUS GUIDELINES
Patients with Known Coronary Artery Disease/Angina PectorisPatients with Known Coronary Artery Disease/Angina Pectoris
–Revascularization recommended in vast majority of such Revascularization recommended in vast majority of such
individuals with multivessel disease. Little role for non-invasive individuals with multivessel disease. Little role for non-invasive
testing.testing.
–Coronary angiography considered Coronary angiography considered Class I Class I Recommendation Recommendation
(Level of evidence: B)(Level of evidence: B)
Patients with Known Coronary Artery Disease Who Lack AnginaPatients with Known Coronary Artery Disease Who Lack Angina
–No controlled trials have examined whether coronary No controlled trials have examined whether coronary
revascularization can improve outcomes in this populationrevascularization can improve outcomes in this population
–Many centers first evaluate patient for myocardial hibernationMany centers first evaluate patient for myocardial hibernation
–Coronary angiography considered Coronary angiography considered Class IIa Class IIa Recommendation Recommendation
(Level of Evidence:C) (Level of Evidence:C)
Patients with or without Chest Pain in Whom Coronary Artery Patients with or without Chest Pain in Whom Coronary Artery
Disease has Not Been EvaluatedDisease has Not Been Evaluated
–Approximately 35% of patients with IDCM will report angina-like Approximately 35% of patients with IDCM will report angina-like
painpain
–Coronary angiography should be considered Coronary angiography should be considered Class IIa Class IIa
recommendation (Level of Evidence: C) recommendation (Level of Evidence: C) Hunt SA,et al. Circulation 2001;104:2996
NEW ONSET CARDIOMYOPATHYNEW ONSET CARDIOMYOPATHY
ACC/AHA CONSENSUS GUIDELINES ACC/AHA CONSENSUS GUIDELINES
Patients with Known Coronary Artery Disease/Angina PectorisPatients with Known Coronary Artery Disease/Angina Pectoris
–Revascularization recommended in vast majority of such Revascularization recommended in vast majority of such
individuals with multivessel disease. Little role for non-invasive individuals with multivessel disease. Little role for non-invasive
testing.testing.
–Coronary angiography considered Coronary angiography considered Class I Class I Recommendation Recommendation
(Level of evidence: B)(Level of evidence: B)
Patients with Known Coronary Artery Disease Who Lack AnginaPatients with Known Coronary Artery Disease Who Lack Angina
–No controlled trials have examined whether coronary No controlled trials have examined whether coronary
revascularization can improve outcomes in this populationrevascularization can improve outcomes in this population
–Many centers first evaluate patient for myocardial hibernationMany centers first evaluate patient for myocardial hibernation
–Coronary angiography considered Coronary angiography considered Class IIa Class IIa Recommendation Recommendation
(Level of Evidence:C) (Level of Evidence:C)
Patients with or without Chest Pain in Whom Coronary Artery Patients with or without Chest Pain in Whom Coronary Artery
Disease has Not Been EvaluatedDisease has Not Been Evaluated
–Approximately 35% of patients with IDCM will report angina-like Approximately 35% of patients with IDCM will report angina-like
painpain
–Coronary angiography should be considered Coronary angiography should be considered Class IIa Class IIa
recommendation (Level of Evidence: C) recommendation (Level of Evidence: C) Hunt SA,et al. Circulation 2001;104:2996
Aim of ManagementAim of Management
•Heart failure therapy:
1.Drug therapy
2.Mechanical assist devices
3.Heart transplant
•Prevention of sudden cardiac death
•Prevention of thromboembolic complications
•Heart failure therapy:
1.Drug therapy
2.Mechanical assist devices
3.Heart transplant
•Prevention of sudden cardiac death
•Prevention of thromboembolic complications
Treatment of DCMTreatment of DCM
No specific treatmentNo specific treatment
Modification of contributory factor:Modification of contributory factor:
–Avoid alcoholAvoid alcohol
–Avoid pregnancyAvoid pregnancy
–Genetic counsellingGenetic counselling
–Limit exerciseLimit exercise
–Weight reductionWeight reduction
–Control of blood pressureControl of blood pressure
–Promt control of InfectionPromt control of Infection
–Correction of anaemia and malnutritionCorrection of anaemia and malnutrition
No specific treatmentNo specific treatment
Modification of contributory factor:Modification of contributory factor:
–Avoid alcoholAvoid alcohol
–Avoid pregnancyAvoid pregnancy
–Genetic counsellingGenetic counselling
–Limit exerciseLimit exercise
–Weight reductionWeight reduction
–Control of blood pressureControl of blood pressure
–Promt control of InfectionPromt control of Infection
–Correction of anaemia and malnutritionCorrection of anaemia and malnutrition
Supportive Supportive
medical treatment: medical treatment:
Treatment of HF:Treatment of HF:
–Rest Rest
–Salt and water restrictionSalt and water restriction
–Diuretics (eg. Frusemide)Diuretics (eg. Frusemide)
–DigoxinDigoxin
–Vasodilators (eg.ACE inhibitor , Nitrates, Vasodilators (eg.ACE inhibitor , Nitrates,
Prazocin )Prazocin )
-Potassium supplements-Potassium supplements
-Spironolactone-Spironolactone
-Vitamin: B1-Vitamin: B1
-Levocarnitine-Levocarnitine
medical treatment: medical treatment:
Treatment of HF:Treatment of HF:
–Rest Rest
–Salt and water restrictionSalt and water restriction
–Diuretics (eg. Frusemide)Diuretics (eg. Frusemide)
–DigoxinDigoxin
–Vasodilators (eg.ACE inhibitor , Nitrates, Vasodilators (eg.ACE inhibitor , Nitrates,
Prazocin )Prazocin )
-Potassium supplements-Potassium supplements
-Spironolactone-Spironolactone
-Vitamin: B1-Vitamin: B1
-Levocarnitine-Levocarnitine
Con..Con..
Anti arrythmic drugs:Anti arrythmic drugs:
–90% patient has complex ventricular 90% patient has complex ventricular
arrythmiaarrythmia
–IF AF: DigoxinIF AF: Digoxin
–If VT or VF :AmiodoroneIf VT or VF :Amiodorone
Long term anticoagulant therapy:Long term anticoagulant therapy:
–To prevent systemic and pulmonary To prevent systemic and pulmonary
embolismembolism
Consider adding beta blocker if symptoms Consider adding beta blocker if symptoms
persistpersist
Intravenous Dobutamine / DopamineIntravenous Dobutamine / Dopamine
Anti arrythmic drugs:Anti arrythmic drugs:
–90% patient has complex ventricular 90% patient has complex ventricular
arrythmiaarrythmia
–IF AF: DigoxinIF AF: Digoxin
–If VT or VF :AmiodoroneIf VT or VF :Amiodorone
Long term anticoagulant therapy:Long term anticoagulant therapy:
–To prevent systemic and pulmonary To prevent systemic and pulmonary
embolismembolism
Consider adding beta blocker if symptoms Consider adding beta blocker if symptoms
persistpersist
Intravenous Dobutamine / DopamineIntravenous Dobutamine / Dopamine
Con..Con..
•Intervension
• ICD: Patients with documented arrhythmias or a
history of unexplained syncope should be treated
aggressively, usually with an implantable
cardioverter-defibrillator (ICD). Prevention of
sudden death with implantable ICD is efficacious
•CRT: For heart failure in DCM-Using special
pacing technique (Bi ventricular)
•Surgery treatment
– ventricular septal myotomy (disabling angina, syncope
associated with LV outflow obstruction)
– mitral valve replacement (if obstruction cannot be
alleviated)
Cardiac transplantation
•Intervension
• ICD: Patients with documented arrhythmias or a
history of unexplained syncope should be treated
aggressively, usually with an implantable
cardioverter-defibrillator (ICD). Prevention of
sudden death with implantable ICD is efficacious
•CRT: For heart failure in DCM-Using special
pacing technique (Bi ventricular)
•Surgery treatment
– ventricular septal myotomy (disabling angina, syncope
associated with LV outflow obstruction)
– mitral valve replacement (if obstruction cannot be
alleviated)
Cardiac transplantation
Implantation of Implantation of cardiovertercardioverter--
defibrillatordefibrillator
Patients with severely
depressed myocardial
function should be
monitored for
arrhythmias and, if
present, treated
aggressively with
antiarrhythmic agents
or an
implantable
cardioverter-
defibrillator
(ICD).
defibrillatordefibrillator
Patients with severely
depressed myocardial
function should be
monitored for
arrhythmias and, if
present, treated
aggressively with
antiarrhythmic agents
or an
implantable
cardioverter-
defibrillator
(ICD).
CRT: Cardiac CRT: Cardiac
Resynchronization TherapyResynchronization Therapy
1. Improved hemodynamics1. Improved hemodynamics
–Increased COIncreased CO
–Reduced LV filling Reduced LV filling
pressurespressures
–Reduced sympathetic Reduced sympathetic
activityactivity
–Increased systolic function Increased systolic function
2. Reverse LV 2. Reverse LV
remodeling/architectureremodeling/architecture
–Decreased LVES/ED Decreased LVES/ED
volumesvolumes
–Increased LVEFIncreased LVEF
–Circ ’02, JACC ’02, Circ ’02, JACC ’02,
JACC ’02, NEJM’02JACC ’02, NEJM’02
Resynchronization TherapyResynchronization Therapy
1. Improved hemodynamics1. Improved hemodynamics
–Increased COIncreased CO
–Reduced LV filling Reduced LV filling
pressurespressures
–Reduced sympathetic Reduced sympathetic
activityactivity
–Increased systolic function Increased systolic function
2. Reverse LV 2. Reverse LV
remodeling/architectureremodeling/architecture
–Decreased LVES/ED Decreased LVES/ED
volumesvolumes
–Increased LVEFIncreased LVEF
–Circ ’02, JACC ’02, Circ ’02, JACC ’02,
JACC ’02, NEJM’02JACC ’02, NEJM’02
Newly emerging treatment for DCMNewly emerging treatment for DCM
Immunosuppressive and Immunosuppressive and
immunomodulation therapyimmunomodulation therapy
Gene therapy Gene therapy
Cellular transplantationCellular transplantation
–Fetal cardiomyocytesFetal cardiomyocytes
–Skeletal myoblastsSkeletal myoblasts
–Adult stem cellsAdult stem cells
–Embryonic stem cellsEmbryonic stem cells
Immunosuppressive and Immunosuppressive and
immunomodulation therapyimmunomodulation therapy
Gene therapy Gene therapy
Cellular transplantationCellular transplantation
–Fetal cardiomyocytesFetal cardiomyocytes
–Skeletal myoblastsSkeletal myoblasts
–Adult stem cellsAdult stem cells
–Embryonic stem cellsEmbryonic stem cells
Complication of DCMComplication of DCM
Heart failureHeart failure
Arrythmias : AF ,SVT,PVCs ,VT VFArrythmias : AF ,SVT,PVCs ,VT VF
AV blocks:1’ 2’ and CHBAV blocks:1’ 2’ and CHB
BBB : RBBB ,LBBB, LAHB ,LPHBBBB : RBBB ,LBBB, LAHB ,LPHB
Systolic or pulmonary embolismSystolic or pulmonary embolism
SyncopeSyncope
Sudden cardiac deathSudden cardiac death
Heart failureHeart failure
Arrythmias : AF ,SVT,PVCs ,VT VFArrythmias : AF ,SVT,PVCs ,VT VF
AV blocks:1’ 2’ and CHBAV blocks:1’ 2’ and CHB
BBB : RBBB ,LBBB, LAHB ,LPHBBBB : RBBB ,LBBB, LAHB ,LPHB
Systolic or pulmonary embolismSystolic or pulmonary embolism
SyncopeSyncope
Sudden cardiac deathSudden cardiac death
PrognosisPrognosis
The course of disease is progressively downhill, The course of disease is progressively downhill,
although some patients may remain stable for although some patients may remain stable for
years.years.
Treatment of HF may result in temporary Treatment of HF may result in temporary
remission, but relapses are common and in time remission, but relapses are common and in time
– patients become resistant to therapy.– patients become resistant to therapy.
Prognosis for survival beyond a year is poor.Prognosis for survival beyond a year is poor.
50% die within 2 years of diagnosis50% die within 2 years of diagnosis
Nearly all die in 5 yearsNearly all die in 5 years
10% may recover10% may recover
25-40% survives for 10 years25-40% survives for 10 years
The course of disease is progressively downhill, The course of disease is progressively downhill,
although some patients may remain stable for although some patients may remain stable for
years.years.
Treatment of HF may result in temporary Treatment of HF may result in temporary
remission, but relapses are common and in time remission, but relapses are common and in time
– patients become resistant to therapy.– patients become resistant to therapy.
Prognosis for survival beyond a year is poor.Prognosis for survival beyond a year is poor.
50% die within 2 years of diagnosis50% die within 2 years of diagnosis
Nearly all die in 5 yearsNearly all die in 5 years
10% may recover10% may recover
25-40% survives for 10 years25-40% survives for 10 years
IDCM:PROGNOSTIC FEATURESIDCM:PROGNOSTIC FEATURES
VENTRICULOGRAPHIC FINDINGSVENTRICULOGRAPHIC FINDINGS
–Degree of impairment in LVEFDegree of impairment in LVEF
–Extent of left ventricular enlargementExtent of left ventricular enlargement
–Coexistent right ventricular dysfunctionCoexistent right ventricular dysfunction
–Ventricular mass/volume ratioVentricular mass/volume ratio
–Global wall motion abnormalitiesGlobal wall motion abnormalities
–Left ventricular sphericityLeft ventricular sphericity
CLINICAL FINDINGSCLINICAL FINDINGS
–Favorable prognosisFavorable prognosis:: NYHA < IV, younger age, female NYHA < IV, younger age, female
sexsex
–Poor prognosisPoor prognosis:: Syncope, persistent S3 gallop, right- Syncope, persistent S3 gallop, right-
sided heart failure, AV or bundle branch block, sided heart failure, AV or bundle branch block,
hyponatremia, troponin elevation, increased BNP, hyponatremia, troponin elevation, increased BNP,
maximum oxygen uptake < 12 mg/kg/minmaximum oxygen uptake < 12 mg/kg/min
VENTRICULOGRAPHIC FINDINGSVENTRICULOGRAPHIC FINDINGS
–Degree of impairment in LVEFDegree of impairment in LVEF
–Extent of left ventricular enlargementExtent of left ventricular enlargement
–Coexistent right ventricular dysfunctionCoexistent right ventricular dysfunction
–Ventricular mass/volume ratioVentricular mass/volume ratio
–Global wall motion abnormalitiesGlobal wall motion abnormalities
–Left ventricular sphericityLeft ventricular sphericity
CLINICAL FINDINGSCLINICAL FINDINGS
–Favorable prognosisFavorable prognosis:: NYHA < IV, younger age, female NYHA < IV, younger age, female
sexsex
–Poor prognosisPoor prognosis:: Syncope, persistent S3 gallop, right- Syncope, persistent S3 gallop, right-
sided heart failure, AV or bundle branch block, sided heart failure, AV or bundle branch block,
hyponatremia, troponin elevation, increased BNP, hyponatremia, troponin elevation, increased BNP,
maximum oxygen uptake < 12 mg/kg/minmaximum oxygen uptake < 12 mg/kg/min
SummarySummary
Cardiomyopathies are diseases of the heart Cardiomyopathies are diseases of the heart
muscle and are classified based on their muscle and are classified based on their
structural and functional phenotypestructural and functional phenotype
Disorders are frequently geneticDisorders are frequently genetic
Accurate differentiation is needed in order to Accurate differentiation is needed in order to
guide treatment and managementguide treatment and management
Cardiomyopathies are diseases of the heart Cardiomyopathies are diseases of the heart
muscle and are classified based on their muscle and are classified based on their
structural and functional phenotypestructural and functional phenotype
Disorders are frequently geneticDisorders are frequently genetic
Accurate differentiation is needed in order to Accurate differentiation is needed in order to
guide treatment and managementguide treatment and management
Thanks for paying Thanks for paying
attention! attention!
attention! attention!
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