Clinical and Genetic Investigations of 109 Index Patients With Dilated Cardiomyopathy and 445 of Their Relatives

Thomas M Hey; Torsten B Rasmussen; Trine Madsen; Mads Malik Aagaard; Maria Harbo; Henning Mølgaard; Søren K Nielsen; Jan Haas; Benjamin Meder; Jacob E Møller; Hans Eiskjær; Jens Mogensen

doi:10.1161/CIRCHEARTFAILURE.119.006701

Clinical and Genetic Investigations of 109 Index Patients With Dilated Cardiomyopathy and 445 of Their Relatives

Thomas M Hey, Torsten B Rasmussen, Trine Madsen, Mads Malik Aagaard, Maria Harbo, Henning Mølgaard, Søren K Nielsen, Jan Haas, Benjamin Meder, Jacob E Møller, Hans Eiskjær, Jens Mogensen

Publikation: Bidrag til tidsskrift › Tidsskriftartikel › Forskning › peer review

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Abstract

BACKGROUND: It was the aim to investigate the frequency and genetic basis of dilated cardiomyopathy (DCM) among relatives of index patients with unexplained heart failure at a tertiary referral center.

METHODS: Clinical investigations were performed in 109 DCM index patients and 445 of their relatives. All index patients underwent genetic investigations of 76 disease-associated DCM genes. A family history of DCM occurred in 11% (n=12) while clinical investigations identified familial DCM in a total of 32% (n=35). One-fifth of all relatives (n=95) had DCM of whom 60% (n=57) had symptoms of heart failure at diagnosis, whereas 40% (n=38) were asymptomatic. Symptomatic relatives had a shorter event-free survival than asymptomatic DCM relatives (P<0.001).

RESULTS: Genetic investigations identified 43 pathogenic (n=27) or likely pathogenic (n=16) variants according to the American College of Medical Genetics and Genomics and the Association for Molecular Pathology criteria. Forty-four percent (n=48/109) of index patients carried a pathogenic/likely pathogenic variant of whom 36% (n=27/74) had sporadic DCM, whereas 60% (21/35) were familial cases. Thirteen of the pathogenic/likely pathogenic variants were also present in ≥7 affected individuals and thereby considered to be of sufficient high confidence for use in predictive genetic testing.

CONCLUSIONS: A family history of DCM identified only 34% (n=12/35) of hereditary DCM, whereas systematic clinical screening identified the remaining 66% (n=23) of DCM families. This emphasized the importance of clinical investigations to identify familial DCM. The high number of pathogenic/likely pathogenic variants identified in familial DCM provides a firm basis for offering genetic investigations in affected families. This should also be considered in sporadic cases since adequate family evaluation may not always be possible and the results of the genetic investigations may carry prognostic information with an impact on individual management.

Originalsprog	Engelsk
Artikelnummer	e006701
Tidsskrift	Circulation. Heart Failure
Vol/bind	13
Udgave nummer	10
ISSN	1941-3289
DOI	https://doi.org/10.1161/CIRCHEARTFAILURE.119.006701
Status	Udgivet - okt. 2020

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10.1161/CIRCHEARTFAILURE.119.006701

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Hey, T. M., Rasmussen, T. B., Madsen, T., Aagaard, M. M., Harbo, M., Mølgaard, H., Nielsen, S. K., Haas, J., Meder, B., Møller, J. E., Eiskjær, H., & Mogensen, J. (2020). Clinical and Genetic Investigations of 109 Index Patients With Dilated Cardiomyopathy and 445 of Their Relatives. Circulation. Heart Failure, 13(10), Artikel e006701. Advance online publication. https://doi.org/10.1161/CIRCHEARTFAILURE.119.006701

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title = "Clinical and Genetic Investigations of 109 Index Patients With Dilated Cardiomyopathy and 445 of Their Relatives",

abstract = "BACKGROUND: It was the aim to investigate the frequency and genetic basis of dilated cardiomyopathy (DCM) among relatives of index patients with unexplained heart failure at a tertiary referral center.METHODS: Clinical investigations were performed in 109 DCM index patients and 445 of their relatives. All index patients underwent genetic investigations of 76 disease-associated DCM genes. A family history of DCM occurred in 11% (n=12) while clinical investigations identified familial DCM in a total of 32% (n=35). One-fifth of all relatives (n=95) had DCM of whom 60% (n=57) had symptoms of heart failure at diagnosis, whereas 40% (n=38) were asymptomatic. Symptomatic relatives had a shorter event-free survival than asymptomatic DCM relatives (P<0.001).RESULTS: Genetic investigations identified 43 pathogenic (n=27) or likely pathogenic (n=16) variants according to the American College of Medical Genetics and Genomics and the Association for Molecular Pathology criteria. Forty-four percent (n=48/109) of index patients carried a pathogenic/likely pathogenic variant of whom 36% (n=27/74) had sporadic DCM, whereas 60% (21/35) were familial cases. Thirteen of the pathogenic/likely pathogenic variants were also present in ≥7 affected individuals and thereby considered to be of sufficient high confidence for use in predictive genetic testing.CONCLUSIONS: A family history of DCM identified only 34% (n=12/35) of hereditary DCM, whereas systematic clinical screening identified the remaining 66% (n=23) of DCM families. This emphasized the importance of clinical investigations to identify familial DCM. The high number of pathogenic/likely pathogenic variants identified in familial DCM provides a firm basis for offering genetic investigations in affected families. This should also be considered in sporadic cases since adequate family evaluation may not always be possible and the results of the genetic investigations may carry prognostic information with an impact on individual management.",

keywords = "cardiomyopathy, dilated, family, genetic counseling, genetic testing, heart failure, prognosis",

author = "Hey, {Thomas M} and Rasmussen, {Torsten B} and Trine Madsen and Aagaard, {Mads Malik} and Maria Harbo and Henning M{\o}lgaard and Nielsen, {S{\o}ren K} and Jan Haas and Benjamin Meder and M{\o}ller, {Jacob E} and Hans Eiskj{\ae}r and Jens Mogensen",

year = "2020",

month = oct,

doi = "10.1161/CIRCHEARTFAILURE.119.006701",

language = "English",

volume = "13",

journal = "Circulation. Heart Failure",

issn = "1941-3289",

publisher = "Lippincott Williams & Wilkins",

number = "10",

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Hey, TM, Rasmussen, TB, Madsen, T, Aagaard, MM, Harbo, M, Mølgaard, H, Nielsen, SK, Haas, J, Meder, B, Møller, JE, Eiskjær, H & Mogensen, J 2020, 'Clinical and Genetic Investigations of 109 Index Patients With Dilated Cardiomyopathy and 445 of Their Relatives', Circulation. Heart Failure, bind 13, nr. 10, e006701. https://doi.org/10.1161/CIRCHEARTFAILURE.119.006701

TY - JOUR

T1 - Clinical and Genetic Investigations of 109 Index Patients With Dilated Cardiomyopathy and 445 of Their Relatives

AU - Hey, Thomas M

AU - Rasmussen, Torsten B

AU - Madsen, Trine

AU - Aagaard, Mads Malik

AU - Harbo, Maria

AU - Mølgaard, Henning

AU - Nielsen, Søren K

AU - Haas, Jan

AU - Meder, Benjamin

AU - Møller, Jacob E

AU - Eiskjær, Hans

AU - Mogensen, Jens

PY - 2020/10

Y1 - 2020/10

N2 - BACKGROUND: It was the aim to investigate the frequency and genetic basis of dilated cardiomyopathy (DCM) among relatives of index patients with unexplained heart failure at a tertiary referral center.METHODS: Clinical investigations were performed in 109 DCM index patients and 445 of their relatives. All index patients underwent genetic investigations of 76 disease-associated DCM genes. A family history of DCM occurred in 11% (n=12) while clinical investigations identified familial DCM in a total of 32% (n=35). One-fifth of all relatives (n=95) had DCM of whom 60% (n=57) had symptoms of heart failure at diagnosis, whereas 40% (n=38) were asymptomatic. Symptomatic relatives had a shorter event-free survival than asymptomatic DCM relatives (P<0.001).RESULTS: Genetic investigations identified 43 pathogenic (n=27) or likely pathogenic (n=16) variants according to the American College of Medical Genetics and Genomics and the Association for Molecular Pathology criteria. Forty-four percent (n=48/109) of index patients carried a pathogenic/likely pathogenic variant of whom 36% (n=27/74) had sporadic DCM, whereas 60% (21/35) were familial cases. Thirteen of the pathogenic/likely pathogenic variants were also present in ≥7 affected individuals and thereby considered to be of sufficient high confidence for use in predictive genetic testing.CONCLUSIONS: A family history of DCM identified only 34% (n=12/35) of hereditary DCM, whereas systematic clinical screening identified the remaining 66% (n=23) of DCM families. This emphasized the importance of clinical investigations to identify familial DCM. The high number of pathogenic/likely pathogenic variants identified in familial DCM provides a firm basis for offering genetic investigations in affected families. This should also be considered in sporadic cases since adequate family evaluation may not always be possible and the results of the genetic investigations may carry prognostic information with an impact on individual management.

AB - BACKGROUND: It was the aim to investigate the frequency and genetic basis of dilated cardiomyopathy (DCM) among relatives of index patients with unexplained heart failure at a tertiary referral center.METHODS: Clinical investigations were performed in 109 DCM index patients and 445 of their relatives. All index patients underwent genetic investigations of 76 disease-associated DCM genes. A family history of DCM occurred in 11% (n=12) while clinical investigations identified familial DCM in a total of 32% (n=35). One-fifth of all relatives (n=95) had DCM of whom 60% (n=57) had symptoms of heart failure at diagnosis, whereas 40% (n=38) were asymptomatic. Symptomatic relatives had a shorter event-free survival than asymptomatic DCM relatives (P<0.001).RESULTS: Genetic investigations identified 43 pathogenic (n=27) or likely pathogenic (n=16) variants according to the American College of Medical Genetics and Genomics and the Association for Molecular Pathology criteria. Forty-four percent (n=48/109) of index patients carried a pathogenic/likely pathogenic variant of whom 36% (n=27/74) had sporadic DCM, whereas 60% (21/35) were familial cases. Thirteen of the pathogenic/likely pathogenic variants were also present in ≥7 affected individuals and thereby considered to be of sufficient high confidence for use in predictive genetic testing.CONCLUSIONS: A family history of DCM identified only 34% (n=12/35) of hereditary DCM, whereas systematic clinical screening identified the remaining 66% (n=23) of DCM families. This emphasized the importance of clinical investigations to identify familial DCM. The high number of pathogenic/likely pathogenic variants identified in familial DCM provides a firm basis for offering genetic investigations in affected families. This should also be considered in sporadic cases since adequate family evaluation may not always be possible and the results of the genetic investigations may carry prognostic information with an impact on individual management.

KW - cardiomyopathy, dilated

KW - family

KW - genetic counseling

KW - genetic testing

KW - heart failure

KW - prognosis

UR - http://www.scopus.com/inward/record.url?scp=85094221648&partnerID=8YFLogxK

U2 - 10.1161/CIRCHEARTFAILURE.119.006701

DO - 10.1161/CIRCHEARTFAILURE.119.006701

M3 - Journal article

C2 - 33019804

SN - 1941-3289

VL - 13

JO - Circulation. Heart Failure

JF - Circulation. Heart Failure

IS - 10

M1 - e006701

ER -

Clinical and Genetic Investigations of 109 Index Patients With Dilated Cardiomyopathy and 445 of Their Relatives

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