A novel TTN deletion in a family with skeletal myopathy, facial weakness, and dilated cardiomyopathy

Background Pathogenic variants in TTN (OMIM 188840), encoding the largest human protein, are known to cause dilated cardiomyopathy and several forms of skeletal myopathy. The clinical interpretation of TTN variants is challenging, however, due to the frequency of missense changes, variable testing a...

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Bibliographic Details
Published in:Molecular genetics & genomic medicine 2019-11, Vol.7 (11), p.e924-n/a
Main Authors: Roggenbuck, Jennifer, Rich, Kelly, Morales, Ana, Tan, Christopher A., Eck, Douglas, King, Wendy, Vatta, Matteo, Winder, Thomas, Elsheikh, Bakri, Hershberger, Ray E., Kissel, John T.
Format: Article
Language:English
Subjects:
Adolescent
Adult
Age
Algorithms
Asymmetry
Cardiomyopathy
Cardiomyopathy, Dilated - etiology
Cardiomyopathy, Dilated - pathology
Clinical Report
Connectin - genetics
Dilated cardiomyopathy
Face - physiopathology
Facial Paralysis - etiology
Facial Paralysis - pathology
Families & family life
Female
Gait
Gene Deletion
Genomes
Genotype & phenotype
Heart failure
Humans
Laboratories
Male
Middle Aged
Muscle, Skeletal - physiopathology
Muscular Diseases - etiology
Muscular Diseases - pathology
Muscular dystrophy
Myopathy
Pedigree
Phenotypes
Prognosis
Signs and symptoms
TTN
Ultrasonic imaging
variant interpretation
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Summary:Background Pathogenic variants in TTN (OMIM 188840), encoding the largest human protein, are known to cause dilated cardiomyopathy and several forms of skeletal myopathy. The clinical interpretation of TTN variants is challenging, however, due to the frequency of missense changes, variable testing and reporting practices in commercial laboratories, and incomplete understanding of the spectrum of TTN‐related disease. Methods We report a heterozygous TTN deletion segregating in a family with an unusual skeletal myopathy phenotype associated with facial weakness, gait abnormality, and dilated cardiomyopathy. Results A novel 16.430 kb heterozygous deletion spanning part of the A‐ and M‐bands of TTN was identified in the proband and his symptomatic son, as well as in an additional son whose symptoms were identified on clinical evaluation. The deletion was found to be de novo in the proband. Conclusion Pathogenic variants in TTN may be an unrecognized cause of skeletal myopathy phenotypes, particularly when accompanied by dilated cardiomyopathy. We report a heterozygous TTN deletion segregating in a family with an unusual skeletal myopathy phenotype associated with facial weakness, gait abnormality, and dilated cardiomyopathy. Pathogenic variants in TTN may be an unrecognized cause of skeletal myopathy phenotypes, particularly when accompanied by dilated cardiomyopathy.
ISSN:2324-9269
2324-9269
DOI:10.1002/mgg3.924