Interpreting Genetic Variants in Titin in Patients With Muscle Disorders

Savarese, Marco; Maggi, Lorenzo; Vihola, Anna; Jonson, Per Harald; Tasca, Giorgio; Ruggiero, Lucia; Bello, Luca; Magri, Francesca; Giugliano, Teresa; Torella, Annalaura; Evilä, Anni; Fruscio, Giuseppina Di; Vanakker, Olivier; Gibertini, Sara; Vercelli, Liliana; Ruggieri, Alessandra; Antozzi, Carlo; Luque, H.; Janssens, Sandra; Pasanisi, Maria Barbara; Fiorillo, Chiara; Raimondi, Maria Chiara; Ergoli, Manuela; Politano, Luisa; Bruno, Claudio; Rubegni, Anna; Pane, Marika; Santorelli, Filippo M.; Minetti, Carlo; Angelini, C.; Bleecker, Jan De; Moggio, Maurizio; Mongini, Tiziana; Comi, Giacomo Pietro; Santoro, Lucio; Mercuri, Eugenio; Pegoraro, Elena; Mora, Marina; Hackman, Peter; Udd, Bjarne

doi:10.1001/jamaneurol.2017.4899

Cited by 70 publications

(88 citation statements)

References 47 publications

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“…Clinically, four patients younger than five years old presented with delayed motor development since early infancy. Except for the 1‐year‐old infant who had basically normal muscle strengths, neck flexion weakness was prominent in the three other patients, which was in keeping with previous reports . Furthermore, rigid spine, contractures of Achilles, and high‐arched palate were all observed in these three patients, showing high clinical consistency in clinical phenotypes with a higher prevalence than previous reports .…”

Section: Discussionsupporting

confidence: 89%

Novel TTN mutations and muscle imaging characteristics in congenital titinopathy

Zhu

Xie

et al. 2019

Ann Clin Transl Neurol

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Objective We present clinical features, muscle imaging findings, and genetic characteristics of five unrelated Chinese patients with congenital titinopathy, emphasizing the diagnostic role of muscle MRI. Methods Five patients who recessive titinopathies were recruited. All patients received muscle biopsies. Mutations were detected by panel massively parallel sequencing and confirmed by Sanger sequencing. Western blotting of muscle proteins was performed. Leg muscle MRIs were performed in four patients. Results Four patients aged 1–4 years old showed delayed motor development from early infancy, while a 17‐year‐old boy showed only a 1‐year history of exercise intolerance. Physical examination showed proximal weakness in three patients. Muscle biopsies demonstrated multiple myopathological changes, including increased internalized nuclei, multicores, central cores, and dystrophic changes. Genetic sequencing revealed compound heterozygous or homozygous novel TTN mutations, including six frameshift mutations, one nonsense mutation, two missense mutations, one splicing mutation, and one small nonframeshift deletion. Protein analyses revealed significant decrease of full‐length titin in all patients. Thigh muscle MRIs in four patients showed prominent fatty infiltration in the upper portion of semitendinosus and the peripheral portion of gluteus medius, while the sartorius and gracilis were relatively preserved. Interpretation These cases provided further evidence that TTN mutations are likely responsible for an increasing proportion of congenital myopathies than currently recognized. The novel mutations reported expand the mutation spectrum of the TTN gene. There is a characteristic pattern of muscle involvement in congenital titinopathy regardless of clinical or pathological phenotype, providing valuable clues for guiding a genetic diagnosis workup.

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Section: Discussionsupporting

confidence: 89%

Novel TTN mutations and muscle imaging characteristics in congenital titinopathy

Zhu

Xie

et al. 2019

Ann Clin Transl Neurol

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“…In the study by Savarese et al, 10 homology structural modeling analyses suggested deleterious consequence of missense variants 10 . The substitution p.(Thr6324Pro) is located on the external surface of a β strand in an Ig‐domain of the I‐band region, probably affecting the protein stability 10 . The missense variant p.(Thr31339Ala), located in an Fn3 domain within the A‐band, could affect hydrogen bonding with other molecules and may influence the interaction with titin ligands 10 .…”

Section: Discussionmentioning

confidence: 93%

“…In silico analyses suggested that the two missense mutations had deleterious consequences, based on their absence in the general population and the TITINdb predictions. In the study by Savarese et al, 10 homology structural modeling analyses suggested deleterious consequence of missense variants 10 . The substitution p.(Thr6324Pro) is located on the external surface of a β strand in an Ig‐domain of the I‐band region, probably affecting the protein stability 10 .…”

Section: Discussionmentioning

confidence: 99%

“…The substitution p.(Thr6324Pro) is located on the external surface of a β strand in an Ig‐domain of the I‐band region, probably affecting the protein stability 10 . The missense variant p.(Thr31339Ala), located in an Fn3 domain within the A‐band, could affect hydrogen bonding with other molecules and may influence the interaction with titin ligands 10 . Moreover, Thr31339 is in a myosin‐binding domain, 17 and the missense variant could alter titin‐myosin interactions.…”

Section: Discussionmentioning

confidence: 99%

“…Here, we describe three TTN variants, one frameshift mutation (c.79683dupA; p.(Arg26562Thrfs*12)) and two missense mutations (p.(Thr31339Ala) and p.(Thr6324Pro)), in two siblings with congenital multicore myopathy. This family was previously included in the study by Savarese et al 10 who analyzed 93 neuromuscular genes and provided a workflow for interpreting TTN variants. In this report, we present additional phenotypical and molecular data that establish the pathogenicity of these TTN variants.…”

Section: Introductionmentioning

confidence: 99%

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A new congenital multicore titinopathy associated with fast myosin heavy chain deficiency

Perrin

Métay

Villanova³

et al. 2020

Ann Clin Transl Neurol

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Congenital titinopathies are myopathies with variable phenotypes and inheritance modes. Here, we fully characterized, using an integrated approach (deep phenotyping, muscle morphology, mRNA and protein evaluation in muscle biopsies), two siblings with congenital multicore myopathy harboring three TTN variants predicted to affect titin stability and titin-myosin interactions. Muscle biopsies showed multicores, type 1 fiber uniformity and sarcomeric structure disruption with some thick filament loss. Immunohistochemistry and Western blotting revealed a marked reduction of fast myosin heavy chain isoforms. This is the first observation of a titinopathy suggesting that titin defect leads to secondary loss of fast myosin heavy chain isoforms. 846

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Understanding Titin Variants in the Age of Next-Generation Sequencing—A Titanic Challenge

Bönnemann

2018

JAMA Neurol

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Interpreting Genetic Variants in Titin in Patients With Muscle Disorders

Cited by 70 publications

References 47 publications

Novel TTN mutations and muscle imaging characteristics in congenital titinopathy

Novel TTN mutations and muscle imaging characteristics in congenital titinopathy

A new congenital multicore titinopathy associated with fast myosin heavy chain deficiency

Understanding Titin Variants in the Age of Next-Generation Sequencing—A Titanic Challenge

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