Cardiomyopathy


Cardiomyopathy Classification and external resources
Opened left ventricle of heart shows a thickened, dilated left ventricle with subendocardial fibrosis manifested as increased whiteness of endocardium. Autopsy.
ICD-10	I42.0
ICD-9	425.4
DiseasesDB	2137
MeSH	D009202

Cardiomyopathy, which literally means "heart muscle disease," is the deterioration of the function of the myocardium (i.e., the actual heart muscle) for any reason. People with cardiomyopathy are often at risk of arrhythmia or sudden cardiac death or both.^[1]

Cardiomyopathies can generally be categorized into two groups, based on World Health Organization guidelines: extrinsic cardiomyopathies and intrinsic cardiomyopathies.^[2]

1 Extrinsic cardiomyopathies
- 1.1 Ischemic cardiomyopathy
- 1.2 Cardiomyopathy due to systemic diseases
2 Intrinsic cardiomyopathies
3 Treatment
4 Famous cases
5 Genetic causes of cardiomyopathy
6 References
7 External links

Extrinsic cardiomyopathies

These are cardiomyopathies where the primary pathology is outside the myocardium itself. Most cardiomyopathies are extrinsic, because by far the most common cause of a cardiomyopathy is ischemia. The World Health Organization calls these specific cardiomyopathies:^[2]

Coronary artery disease
Congenital heart disease
Nutritional diseases
Ischemic (or ischaemic) cardiomyopathy
Hypertensive cardiomyopathy
Valvular cardiomyopathy
Inflammatory cardiomyopathy
Cardiomyopathy secondary to a systemic metabolic disease
Alcoholic cardiomyopathy
Diabetic cardiomyopathy

Ischemic cardiomyopathy

Ischemic cardiomyopathy is a weakness in the muscle of the heart due to inadequate oxygen delivery to the myocardium with coronary artery disease being the most common cause. Anemia and sleep apnea are relatively common conditions that can contribute to ischemic myocardium and hyperthyroidism can cause a 'relative' ischemia secondary to high output heart failure. Individuals with ischemic cardiomyopathy typically have a history of myocardial infarction (heart attack), although longstanding ischemia can cause enough damage to the myocardium to precipitate a clinically significant cardiomyopathy even in the absence of myocardial infarction. In a typical presentation, the area of the heart affected by a myocardial infarction will initially become necrotic as it dies, and will then be replaced by scar tissue (fibrosis). This fibrotic tissue is akinetic; it is no longer muscle and cannot contribute to the heart's function as a pump. If the akinetic region of the heart is substantial enough, the affected side of the heart (i.e. the left or right side) will go into failure, and this failure is the functional result of an ischemic cardiomyopathy.

Cardiomyopathy due to systemic diseases

Many diseases can result in cardiomyopathy. These include diseases like hemochromatosis, (an abnormal accumulation of iron in the liver and other organs), amyloidosis (an abnormal accumulation of the amyloid protein), diabetes, hyperthyroidism, lysosomal storage diseases and the muscular dystrophies.

Intrinsic cardiomyopathies

An intrinsic cardiomyopathy is weakness in the muscle of the heart that is not due to an identifiable external cause. To make a diagnosis of an intrinsic cardiomyopathy, significant coronary artery disease should be ruled out (amongst other things). The term intrinsic cardiomyopathy does not describe the specific etiology of weakened heart muscle. The intrinsic cardiomyopathies are a mixed-bag of disease states, each with their own causes.

Intrinsic cardiomyopathy has a number of causes including drug and alcohol toxicity, certain infections (including Hepatitis C), and various genetic and idiopathic (i.e., unknown) causes.

Intrinsic cardiomyopathies are generally classified into four types,^[2]^[3] but additional types are also recognized:

Dilated cardiomyopathy (DCM), the most common form, and one of the leading indications for heart transplantation. In DCM the heart (especially the left ventricle) is enlarged and the pumping function is diminished. Approximately 40% of cases are familial, but the genetics are poorly understood compared with HCM. In some cases it manifests as peripartum cardiomyopathy, and in other cases it may be associated with alcoholism.
Hypertrophic cardiomyopathy (HCM or HOCM), a genetic disorder caused by various mutations in genes encoding sarcomeric proteins. In HCM the heart muscle is thickened, which can obstruct blood flow and prevent the heart from functioning properly.
Arrhythmogenic right ventricular cardiomyopathy (ARVC) arises from an electrical disturbance of the heart in which heart muscle is replaced by fibrous scar tissue. The right ventricle is generally most affected.
Restrictive cardiomyopathy (RCM) is an uncommon cardiomyopathy. The walls of the ventricles are stiff, but may not be thickened, and resist the normal filling of the heart with blood. A rare form of restrictive cardiomyopathy is the obliterative cardiomyopathy, seen in the hypereosinophilic syndrome. In this type of cardiomyopathy, the myocardium in the apices of the left and right ventricles becomes thickened and fibrotic, causing a decrease in the volumes of the ventricles and a type of restrictive cardiomyopathy.
Noncompaction cardiomyopathy has been recognized as a separate type since the 1980s. The term refers to a cardiomyopathy where the left ventricle wall has failed to grow properly from birth and has a spongy appearance when viewed during an echocardiogram.

Signs and symptoms Cardiomyopathy is usually found incidentally - "case finding" - by healthcare professionals during a routine checkup. The only test for hypertension is a blood pressure measurement. Hypertension in isolation usually produces no symptoms although some people report headaches, fatigue, wanting to sleep more than usual, dizziness, blurred vision, facial flushing or tinnitus. [10]

Malignant Cardiomyopathy (or accelerated Cardiomyopathy) is distinct as a late phase in the condition, and may present with headaches, blurred vision and end-organ damage.

Cardiomyopathy is often confused with mental tension, stress and anxiety. While chronic anxiety and/or irritability is associated with poor outcomes in people with hypertension, it alone does not cause it. Accelerated hypertension is associated with somnolence, confusion, visual disturbances, and nausea and vomiting (hypertensive encephalopathy)

Treatment

Treatment depends on the type of cardiomyopathy, but may include medication, implanted pacemakers, defibrillators, or ventricular assist devices (LVADs), or ablation. The goal of treatment is often symptom relief, and some patients may eventually require a heart transplant. Treatment of cardiomyopathy (and other heart diseases) using alternative methods such as stem cell therapy is commercially available but is not supported by convincing evidence.

Famous cases

Dave Williams (musician) of Drowning Pool died of this disease in 2002.

Dr. Robert Atkins, inventor of "The Atkins Diet" suffered from this disease in the years before his death from a fall.

Alexei Cherepanov, 19 year old professional ice hockey player, died of this during an ice hockey game in 2008.

Michael James Hegstrand aka Road Warrior Hawk an American professional wrestler.

Slash, guitarist for Velvet Revolver, survived this disease.

Reggie Lewis, captain and all-star of the Boston Celtics, died from either Hypertrophic or Cocaine Cardiomyopathy at age 27.

Genetic causes of cardiomyopathy

Phenotype	Inheritance pattern	Chromosomal locus	Gene	Protein	Skeletal myopathy
Dilated cardiomyopathy	X-linked	Xp21	dystrophin	Dystrophin	Duchenne / Becker muscular dystrophy
	X-linked	Xq28	G4.5	Tafazzin	Barth syndrome
	Autosomal dominant	15q14	actin	Actin	Nemaline myopathy
		2q35	desmin	Desmin	Desmin myopathy
		5q33	δ-sarcoglycan	δ-sarcoglycan	Limb girdle muscular dystrophy 2F
		1q32	Troponin T	Troponin T
		14q11	β-myosin heavy chain	β-myosin heavy chain
		15q2	α-tropomyosin	α-tropomyosin	Nemaline myopathy
		Midna	Mitochondrial respiratory chain	Mitochondrial respiratory chain	Mitochondrial myopathy
Dilated cardiomyopathy with conduction disease	Autosomal dominant	1q21	lamin A/C	Lamin A/C	Emery-Dreifuss muscular dystrophy
Hypertrophic cardiomyopathy	Autosomal dominant	14q11	β-myosin heavy chain	β-myosin heavy chain
		14q11	β-myosin heavy chain	β-myosin heavey chain
		1q32	Troponin T	Troponin T
		12q23	Troponin T	Troponin T
		15q2	α-tropomyosin	α-tropomyosin	Nemaline myopathy
		11q11	myosin-binding protein C	myosin-binding protein C
		3p21	myosin essential light chain	myosin essential light chain
		3p21	myosin regulatory light chain	myosin regulatory light chain
		2p31	titin	Titin
Hypertrophic cardiomyopathy with Wolf-Parkinson-White syndrome		7q3	AMPK	AMPK
		MIDINA	Mitochondrial respiratory chain	Mitochondrial respiratory chain	Mitochondrial myopathy
Left ventricular noncompaction	X-linked	Xq28	G4.5	Tafazzin	Barth syndrome
	Autosomal dominant	18q12	α-dystrobrevin	α-Dystrobrevin	Muscular dystrophy

Table from article *"The Failing Heart". Nature. Retrieved on June 15, 2007.

References

↑ Kasper, Denis L. et al (2005). Harrison's Principles of Internal Medicine, 16th edn. McGraw-Hill. ISBN 0-07-139140-1.
↑ ^2.0 ^2.1 ^2.2 Richardson, P. et al (1996). "Report of the 1995 World Health Organization/International Society and Federation of Cardiology Task Force on the Definition and Classification of cardiomyopathies". Circulation 93 (5): 841–2. PMID 8598070. (Full text)
↑ Cardiomyopathy Association. "About cardiomyopathy". Retrieved on 2006-09-28.

External links

[1] The Children's Cardiomyopathy Foundation is a non-profit that provides support to parents of affected children and accelerates research related to diagnosis, treatments and cures for all types of cardiomyopathies in children.
The Cardiomyopathy Association A site is designed to provide you with information on the main forms of the heart muscle disease known as cardiomyopathy. Great information for adults and young.
Cardiomyopathy information from Seattle Children's Hospital Heart Center
Information from the Stanford Hypertrophic Cardiomyopathy Center
Cardiomyopathy-related antibodies
Treatment Cardiomyopathy (Alternative Medicine)

Cardiovascular disease: heart disease - Circulatory system pathology (I00-I52, 390-429)

Ischaemic/
Acute coronary

CHD: CAD - Coronary thrombosis - Coronary vasospasm - Coronary artery aneurysm

Angina pectoris (Prinzmetal's angina) - Myocardial infarction (heart attack)

Myocardial rupture - Dressler's syndrome

Layers

Pericardium	Pericarditis (Acute, Constrictive) - Pericardial effusion - Cardiac tamponade - Hemopericardium

Myocardium	Myocarditis Cardiomyopathy: Dilated (Alcoholic) - Hypertrophic - Restrictive (Loeffler endocarditis, Cardiac amyloidosis) Arrhythmogenic right ventricular dysplasia

Endocardium/ valves	Endocarditis (Subacute bacterial endocarditis, Libman-Sacks endocarditis, Nonbacterial thrombotic endocarditis) mitral (regurgitation, prolapse, stenosis) - aortic (stenosis, insufficiency) - tricuspid (stenosis, insufficiency) - pulmonary (stenosis, insufficiency)

Conduction/
arrhythmia

Heart block	AV (1°, 2°, 3°) - Bundle branch (Left, Right) - Bifascicular/Trifascicular - Sinoatrial - Sick sinus syndrome - Adams-Stokes syndrome

Pre-excitation syndrome	Wolff-Parkinson-White - Lown-Ganong-Levine

Tachycardia	Paroxysmal - Supraventricular (AV nodal reentrant, Accelerated idioventricular rhythm, Sinus) - Ventricular (Torsades de pointes, Catecholaminergic polymorphic)

Premature contraction	Atrial - Ventricular

Flutter/fibrillation	Atrial flutter - Ventricular flutter - Atrial fibrillation (Familial) - Ventricular fibrillation

Pacemaker	Wandering pacemaker - Ectopic pacemaker - Parasystole - Multifocal atrial tachycardia

Long QT syndrome	Romano-Ward syndrome - Andersen-Tawil syndrome - Jervell and Lange-Nielsen syndrome

Cardiac arrest	Sudden cardiac death - Asystole - Pulseless electrical activity

Other

Cardiomegaly - Ventricular hypertrophy (Left, Right/Cor pulmonale)
Heart failure (Cardiac asthma) - Rheumatic fever

See also congenital, neoplasia