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Cardiomyopathy in neonates and children

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Title: Cardiomyopathy in neonates and children

1
Cardiomyopathy in neonates and children

Dr Rajesh Kumar
MD (PGI), DM (Neonatology) PGI, Chandigarh, India
Rani Children Hospital, Ranchi

Some cardiomyopathies are treatable
Cardiomyopathy may presents as recurrent wheeze

3
Classification of Cardiomyopathy

Dilated
Chronic
Acute Viral myocarditis (Inflammatory
Cardiomyopathy)
Hypertrophic
Restrictive

4
Epidemiology

Incidence 11,00,000
1 of all pediatric cardiac disease
During infancy incidence is 10 times higher than
older children
40 die within 2 years of life
Idiopathic is 70-80

5
CardiomyopathyPathophysiologic Classification

Dilated Cardiomyopathy
Insult to the myocardium
tissue necrosis/interstitial fibrosis
impaired systolic contractility/diastolic
compliance
ventricular dilation to maintain function
Left /- right sides

Hypertrophic Cardiomyopathy
Myocyte hypertrophy disarray
Increased mass thickness
Increased mass/volume ratio
Poor diastolic chamber compliance Left ventricle
High systolic pressure gradient
Restrictive Cardiomyopathy
Rare, very small L ventricular cavity
Impaired diastolic function initially
Unclassified cardiomyopathy

6
Causes of dilated Cardiomyopathy
7
Causes of dilated Cardiomyopathy
8
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9
Pathogenesis of idiopathic DCM

preceding viral myocarditis
autoimmunity
Underlying genetic predisposition

10
DCM History

Insidious onset, may be acute in up to 25 of
patients, exacerbated by a complicating LRTI
Cough, poor feeding, irritability, and shortness
of breath are usually the initial presenting
symptoms.
Pallor, sweating, easy fatigability, failure to
gain weight, and decreased urine output may be
present.
Wheezing may be an important clinical sign,
suggesting congestive heart failure (CHF)
manifestation in infants.
Chest pain, palpitations, orthopnea, hemoptysis,
frothy sputum, sudden death, abdominal pain,
syncope, and neurologic deficit are other modes
of presentation (20).
Cardiomegaly detected incidentally on a chest
radiograph or an arrhythmia detected incidentally
on an ECG may be the basis for initial cardiac
referral.
Approximately 50 of patients with dilated
cardiomyopathy (DCM) have a history of preceding
viral illness. A detailed family history for
familial cardiomyopathy is revealing in up to 25
of cases.

11
DCM physical findings

In established disease, features of CCF are
dominant.
Major cardiac findings include cardiomegaly,
quiet precordium, tachycardia, gallop rhythm (S3
and/or S4), accentuated P-2, and murmurs of
mitral and tricuspid regurgitation. Murmurs may
be inconspicuous initially when presenting in
acute heart failure.
Infants often present with predominantly
respiratory signs and, in the absence of a
precordial heave or prominent murmur, the
underlying cardiac disease may remain undiagnosed
until cardiomegaly is detected on chest
radiograph.

12
Diagnostic Evaluation

Step 1 Initial Evaluation
EKG
CXR
ECHO
Step 2 Screening Evaluation
CBC
EnzymesSGOT, SGPT, CPK,
ABG
Fractionated serum carnitine
Urine organic amino acids
Urine muco/oligosacharides
Skeletal survey

Step 3 Specific Testing
Cardiac catheterization
Myocardial biopsy
Holter monitoring
Carnitine levels (skeletal, cardiac tissue,
urine)
Serum ketone bodies, ammonia, pyruvate, lactate
Fibroblast studies
Chromosomes

13
ECG

Presence of Q waves and inversion of T waves in
leads I, II, aVL, and V4 through V6
(anterolateral infarction pattern) ALCAPA
Significant arrhythmia Arrythmia causing DCM
Low Voltage complexes Pericardial effusion

14
ECHO

Dilated left ventricle (gt95th percentile) with
global hypokinesia (fractional shortening lt25,
ejection fraction lt50), and no demonstrable
structural heart disease DCM
Left ventricular posterior wall hypokinesia with
hyper-echoic papillary muscles, retrograde
continuous flow into proximal pulmonary artery
ALCAPA
Significant pericardial effusion with
satisfactory left ventricular ejection fraction
Pericardial effusion

15
Cardiomyopathy Management

Supportive Therapy
Non specific therapy for heart failure, to
improve survival alleviate symptoms
ACE inhibitors (captopril, enalpril)
Reduce afterload
Improve cardiac ejection
Reduce catecholamine drive prolonging cardiac
survival
Careful titration necessary
B blockers (metoprolol, carvedilol)
Digoxin
Diuretics

Specific Therapy
Depends on the underlying disease condition
Most have no effective Rx
Carnitine supplements
Surgery
Correction of aberrant vessels
Implanable defibrillators
Partial left venticulectomy
Cardiac transplant

16
Digoxin

Inotropic agent
Loading dose
Premature neonate20-30 mg/kg
Term neonate 30-40 mg/kg
Schedule for loading ½, ¼, ¼ 8hours apart
Maintanance dose
Premature neonate 5-10 mg/kg/day BD
Term neonate 10 mg/kg/day BD

17
Digoxin

Route IV, IM, oral
Injection 1ml ampoule, 250 mg /ml
1unit 6.25 mg 10 mg /kg 1.5units/kg
Oral (Digoxin Paed elixir) 1ml 0.05 mg
Maintenance dose 0.01 mg/kg/day
Wt in kg /10 ml twice daily
3 kg 0.3 ml twice daily

18
Alteration of preload

Fluid retention due to low cardiac output and
renal perfusion
Ventricular contractility is compromised due to
massive volume overload
Diuretics
Acute diuresis Furosemide 1-4 mg/kg/dose
Chronic diuresis Furosemide potassium sparing
diuretics

19
Maximum diuretic therapy

Frusamide upto 2mg/kg/dose TDS
Frusamide Thiazide diuretic
Frusamide Metolazone
Metolazone 0.2 mg/kg/dose OD
Hydrochlortiazid 2-4 mg/kg/day
Chlorthiazide 20-40 mg/kg/day

20
Alteration of afterload

Precaution Do not use in hypovolumic condition
and in pt with fixed left ventricular outflow
obstruction
Effective in Regurgitant lesions(ECD,
Cardiomyopathy) and left to right shunts (VSD)
Acute Nitroprusside, Dobutamine, amrinone
Chronic ACE inhibitors
Enalapril 0.1 mg/kg /day OD or BD ( 5 kg ¼ tab
OD)

21
ACE inhibitors

Captopril
Neonate 0.1 0.4 mg/kg/dose 1-4 times a day
Infant 0.1 1 mg /kg/dose 1-4 times a day
Child 12.5 mg/dose 1-2 times a day
Enalapril 0.1 mg/kg 1-2 times a day never gt0.5
mg/kg/day

22
K concerns

If using Furesamide gt2mg/kg/day
add oral potassium
Add spironolactone
If using ACE inhibitors do not use spironolactone
Electrolytes should be monitored monthly
Hyponatremia should be managed with decreasing
diuretic and restricting fluid, not by
supplementing sodium

23
Carvedilol in cardiomyopathy
24
Tab CARDIVAS 3.125 mg
25
Role of beta blocker

Adrenergic stimulation happens in CCF
Increases HR and contractility
Alpha stimulation leads to peripheral and
coronary constriction, increase O2 demand and
after load
Beta1 receptor stimulation causes calcium
accumulation in cells and cell death
Carvedilol is beta and alpha blocker

26
K concerns

If using Furesamide gt2mg/kg/day
add oral potassium
Add spironolactone
If using ACE inhibitors do not use spironolactone
Electrolytes should be monitored monthly
Hyponatremia should be managed with decreasing
diuretic and restricting fluid, not by
supplementing sodium

27
Treatment

Carnitine 25-50 mg / kg/dose BD or TDS, Max
200mg/kg/day
Coenzyme Q10 variable result

28
Hypertrophic Cardiomyopathy

Clinical Sudden death, Syncope, Presyncope,
dizziness, palpitation
Murmur, S3
ECG Arrythmia
ECHO septal thickness is gt 1.4 times the
posterior wall thickness
Treatment propanalol, Verapamil, amiodarone

29
Restrictive Cardiomyopathy

Restriction of diastolic filling
Causes amyloidosis, hemosiderosis,
hypereosinophilia, and endocardial fibroelastosis
Treatment unhelpful, Only diuretic

30
MI in children

ALCAPA
Post TGA operation coronary ostia stenosis,
kinking of coronary artery
Thrombotic occlusion in KD
Takayashu arteritis
SCD

31
Aspirin in KD

Acute intervention for Kawasaki disease80-100
mg/kg/d PO divided q6h until afebrile for 2-3 d
Subsequent antiplatelet dose3-5 mg/kg/d PO
Duration of treatment is 6-8 wk from onset of
illness or until erythrocyte sedimentation rate
and platelet count return to reference range
may require indefinite continuation if coronary
artery abnormalities are observed

32
MI in ALCAPA

Infant develops irritability with dyspnea,
tachycardia, diaphoresis, and vomiting while
feeding. Irritability is secondary to anginal
pain caused by a coronary artery steal phenomenon
to the anomalous origin of the left coronary
artery. The flow in this vessel, which has its
distribution over the left ventricular
myocardium, is retrograde to the main pulmonary
artery.
The diagnosis of ALCAPA is suspected in irritable
anxious infants presenting with pain while
feeding. ECG demonstrates classic findings of
deep Q waves, peaked T waves, and/or ST segment
changes consistent with ischemia, injury, or
infarction.

33
MI in KD

Coronary artery involvement occurs in 15-25 of
children with Kawasaki disease within 1-3 weeks
of onset. In patients with untreated Kawasaki
disease, sudden death has resulted from acute
myocardial infarction caused by ruptured coronary
artery aneurysms or thromboses.
Detrimental changes in arterial wall hemodynamics
are present and persist after acute Kawasaki
disease which may predispose to long-term
cardiovascular events.

34
Neonatal Cardiomyopathy
35
Neonatal Cardiomyopathy Etiologic
classification

HYPERTROPHIC
Familial
Idiopathic Hypertrophic
Maternal disease
Diabetes
Myocarditis
Infectious
endotoxins, exotoxicins
Drugs /Iatrogenic
Dexamathasone (BPD)( case report)
ECMO (case report)
Adriamycin
Chloramphenicol
Malformation syndromes
Beckwith wiedemann

DILATED
Perinatal insult/ maladjustment
Asphyxia
Persistent fetal circulation
Congenital anomalies
Anomalous origin of Left coronary
Inborn errors of metabolism
Glycogen storage dses (Pompes dse)
Mucopolysaccharidosis
Disorders of fatty acid metabolism (Carnitine
deficiency)
Amino organic acidiurias
Maternal connective Tissue dse
SLE

36
Neonatal Cardiomyopathy Asphyxia induced

Hypoxia leads to myocardial ischemia/dilation
Term infant with delivery complicated by hypoxic
stress
Apgars usually lt3 _at_ 1
Metabolic acidosis/ multi system ischemia
Severe cases Hypotension/shock
Murmur of mitral/tricuspid regurg may be present
EKG Diffuse ST -T changes, R atrial hypertrophy
Prognosis Good without cardiogenic shock

37
Neonatal Cardiomyopathy From Maternal Diabetes

Asymmetric hypertrophic cardiomyopathy
Mechanism not clearly understood ?
Hyperinsulinemia
Prevalence unrelated to diabetic control of
mother
Puffy, Plethoric infant, with signs and symptoms
of CCF
SEM common and related to degree of outflow
obstruction
RXUsually symptomatic
Prognosis Usually good, resolves in months
Digitalis and other inotropics agents are
contraindicated
except in very severe depression of myocardial
contractility

38
Neonatal Cardiomyopathy Carnitine deficiency

Autosomal recessive inheritance
Plasma memb carnitine transport defect Impairs
fatty acid oxidation
Metabolic acidosis, intractable hypoglycemia,
severe non-immune hydrops, /-muscle weakness
EKG Giant T waves(pathognomonic)
Subnormal carnitine level 1-2 , heterozygous
parents have 50 levels
Symptomatic Rx for the cardiac failure gives
minimal benefits
Definitive Rx Oral carnitine supplements
Prognosis Usually good with early diagnosis and
Rx
Risk of growth and mental retardation

39
Neonatal Cardiomyopathy Myocarditis