| Literature DB >> 31264822 |
Vandana Shashi1, Janelle Geist2, Youngha Lee3, Yongjin Yoo3, Unbeom Shin4, Kelly Schoch1, Jennifer Sullivan1, Nicholas Stong5, Edward Smith6, Joan Jasien6, Peter Kranz7, Yoonsung Lee8, Yong Beom Shin9, Nathan T Wright10, Murim Choi3, Aikaterini Kontrogianni-Konstantopoulos2.
Abstract
Encoding the slow skeletal muscle isoform of myosin binding protein-C, MYBPC1 is associated with autosomal dominant and recessive forms of arthrogryposis. The authors describe a novel association for MYBPC1 in four patients from three independent families with skeletal muscle weakness, myogenic tremors, and hypotonia with gradual clinical improvement. The patients carried one of two de novo heterozygous variants in MYBPC1, with the p.Leu263Arg variant seen in three individuals and the p.Leu259Pro variant in one individual. Both variants are absent from controls, well conserved across vertebrate species, predicted to be damaging, and located in the M-motif. Protein modeling studies suggested that the p.Leu263Arg variant affects the stability of the M-motif, whereas the p.Leu259Pro variant alters its structure. In vitro biochemical and kinetic studies demonstrated that the p.Leu263Arg variant results in decreased binding of the M-motif to myosin, which likely impairs the formation of actomyosin cross-bridges during muscle contraction. Collectively, our data substantiate that damaging variants in MYBPC1 are associated with a new form of an early-onset myopathy with tremor, which is a defining and consistent characteristic in all affected individuals, with no contractures. Recognition of this expanded myopathic phenotype can enable identification of individuals with MYBPC1 variants without arthrogryposis.Entities:
Keywords: MYBPC1; arthrogryposis; hypotonia; myopathy; myosin binding protein-C; tremor
Year: 2019 PMID: 31264822 PMCID: PMC6688907 DOI: 10.1002/humu.23760
Source DB: PubMed Journal: Hum Mutat ISSN: 1059-7794 Impact factor: 4.878