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C‐terminal titin deletions cause a novel early‐onset myopathy with fatal cardiomyopathy

245

Citations

36

References

2007

Year

Abstract

M-line titin homozygous truncations cause the first congenital and purely recessive titinopathy, and the first to involve both cardiac and skeletal muscle. These results expand the spectrum of early-onset myopathies and suggest that titin segments downstream of the kinase domain are dispensable for skeletal and cardiac muscle development, but are crucial for maintaining sarcomere integrity.

References

YearCitations

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