2. 1956
• Myocardial diseases classified
as myocarditis (inflammatory
heart muscle disease), and
myocardiosis (other heart
muscle diseases)
• Blankerhorn MA, Gall EA.
Myocarditis and myocardiosis:
a clinicopathologic appraisal.
Circulation 1956;13:217–23.
3. 1957
• The term cardiomyopathy
proposed for uncommon,
noncoronary heart muscle
diseases
• Bridgen W. Uncommon
myocardial diseases:the non-
coronary cardiomyopathies.
Lancet 1957;273:1179–84.
4. 1972
Cardiomyopathy described as
myocardial diseases of unknown
origin, and first classification
proposed as
dilated,hypertrophic, and
restrictive (or obliterative)
cardiomyopathy
• Goodwin JF, Oakley CM. The
cardiomyopathies.Br Heart J
1972;34:545–52.
5. 1980 WHO
Defines cardiomyopathies as
myocardial diseases of unknown
etiology. WHOISFC
adds specific heart muscle
diseases (cause of myocardial
affliction known) to the
classification
• Report of the WHO/ISFC Task
Force on the definition and
classification of
cardiomyopathies.Br Heart J
1980;44:672–3.
6. 1996
WHO-ISFC updates its
classification of
cardiomyopathies (diseases of
myocardium associated
withmyocardial dysfunction). The
update includes arrhythmogenic
right ventricular cardiomyopathy
and unclassified
cardiomyopathy, but excludes
specific heart muscle disease.
Richardson P, McKenna W,
Bristow M, et al.Report of the
1995 World Health
Organization/International
Society and Federation of
Cardiology Task Force on the
Definition and Classificationof
cardiomyopathies. Circulation
1996;93:841–2.
8. AHA 2006
Defines cardiomyopathies as diseases of myocardium associated
with mechanical and/or electrical dysfunction, which usually (but not
invariably) exhibit inappropriate ventricular hypertrophy or dilation,due
to a variety of causes that frequently are genetic, classified as
primary or secondary. Presents first visionary attempt to classify
primary cardiomyopathy by genetic origin (genetic, acquired, or
mixed)
9. ESC 2008
Defines cardiomyopathies as myocardial disorder in which the heart
muscle was structurally and functionally abnormal. Classified dilated,
hypertrophic, restrictive,arrhythmogenic right ventricular, or
unclassified cardiomyopathy subtypes as familial/genetic and
nonfamilial/nongenetic. Maintained the importance of phenotype
preceding genetic classification for clinical practice.
10. 2013 WHF-MOGE(S)
1. M: MORPHO-FUNCTIONAL
PHENOTYPE
2. O: INVOLVED ORGANS
3. G: GENETIC
4. E: ETIOLOGY
5. S: FUNCTIONAL STATUS
1.Arbustini E, Narula N, Dec WG, et al. The
MOGE(S) Classification for a phenotype–genotype
nomenclature of cardiomyopathy. Endorsed by the
World Heart Federation. J Am Coll Cardiol 2013;
62:2046–72.
2. Arbustini E, Narula N, Dec WG, et al. The
MOGE(S) classification for a phenotype–genotype
nomenclature of cardiomyopathy. endorsed by the
World Heart Federation. G Heart 2013;8:355–82.