Titin mutation segregates with hereditary myopathy with early respiratory failure

Pfeffer, Gerald; Elliott, Hannah R; Griffin, Helen; Barresi, Rita; Miller, James; Marsh, Julie A.; Evilä, Anni; Vihola, Anna; Hackman, Peter; Straub, Volker; Dick, D J; Horvath, Rita; Santibanez‐Koref, Mauro; Udd, Bjarne; Chinnery, Patrick F.

doi:10.1093/brain/aws102

Cited by 113 publications

(148 citation statements)

References 49 publications

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“…11,[26][27][28][29][30][31] Based on these reasons, we hypothesized that the TTN mutations present in our 5 patients with CNM were likely to be causative for the disease. Although occasional fibers with internal nuclei have been reported in other muscle diseases with TTN mutations, 19 patients had a noteworthy cardiac phenotype, although the ages at last examination only ranged from 5 to 19 years. In addition, ophthalmoplegia, a common finding in the previously defined CNM cases, was not present.…”

Section: Indirect Immunofluorescence Analysis Of Muscle Biopsiesmentioning

confidence: 90%

“…[10][11][12] Encompassing 363 exons, TTN includes several regions subject to extensive differential splicing, producing a number of different isoforms in cardiac and skeletal muscles. 10,13,14 TTN mutations have previously been implicated in various cardiac and skeletal muscle diseases including adult-onset tibial muscular dystrophy, [15][16][17] limb-girdle muscular dystrophy 2J, 15,18 hereditary myopathy with early respiratory failure, 19,20 and earlyonset myopathy with fatal cardiomyopathy. 21 Heterozygous truncating mutations in TTN have also been shown to be a common cause of dilated cardiomyopathy, accounting for ;25% of cases in one large series.…”

Section: Indirect Immunofluorescence Analysis Of Muscle Biopsiesmentioning

confidence: 99%

“…11,21 Binding of calpain 3 to the M-line region of titin is required for its stabilization, as mutations in this region of titin cause a decrease in the amount of calpain 3 in the muscle. 19,21,36 figure 2C). Altogether, these results suggested that all patient muscles analyzed had truncated titin proteins lacking a significant portion of their Cterminal regions.…”

Section: Indirect Immunofluorescence Analysis Of Muscle Biopsiesmentioning

confidence: 99%

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Recessive truncating titin gene, TTN , mutations presenting as centronuclear myopathy

et al. 2013

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Objective: To identify causative genes for centronuclear myopathies (CNM), a heterogeneous group of rare inherited muscle disorders that often present in infancy or early life with weakness and hypotonia, using next-generation sequencing of whole exomes and genomes.Methods: Whole-exome or -genome sequencing was performed in a cohort of 29 unrelated patients with clinicopathologic diagnoses of CNM or related myopathy depleted for cases with mutations of MTM1, DNM2, and BIN1. Immunofluorescence analyses on muscle biopsies, splicing assays, and gel electrophoresis of patient muscle proteins were performed to determine the molecular consequences of mutations of interest.Results: Autosomal recessive compound heterozygous truncating mutations of the titin gene, TTN, were identified in 5 individuals. Biochemical analyses demonstrated increased titin degradation and truncated titin proteins in patient muscles, establishing the impact of the mutations.Conclusions: Our study identifies truncating TTN mutations as a cause of congenital myopathy that is reported as CNM. Unlike the classic CNM genes that are all involved in excitation-contraction coupling at the triad, TTN encodes the giant sarcomeric protein titin, which forms a myofibrillar backbone for the components of the contractile machinery. This study expands the phenotypic spectrum associated with TTN mutations and indicates that TTN mutation analysis should be considered in cases of possible CNM without mutations in the classic CNM genes.

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Section: Indirect Immunofluorescence Analysis Of Muscle Biopsiesmentioning

confidence: 90%

Section: Indirect Immunofluorescence Analysis Of Muscle Biopsiesmentioning

confidence: 99%

Section: Indirect Immunofluorescence Analysis Of Muscle Biopsiesmentioning

confidence: 99%

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Recessive truncating titin gene, TTN , mutations presenting as centronuclear myopathy

et al. 2013

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“…The Mex6 (exon 363) TMDmutation homozygous LGMD2J is childhood onset and shows a secondary calpain deficiency, but the clinical presentation is different, without contractures. [24][25][26][27] Overall, the presentation described here is unique among titinopathies.…”

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confidence: 99%

A new titinopathy

et al. 2015

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Objective: To identify the genetic defects present in 3 families with muscular dystrophy, contractures, and calpain 3 deficiency.Methods: We performed targeted exome sequencing on one patient presenting a deficiency in calpain 3 on Western blot but for which mutations in the gene had been excluded. The identification of a homozygous truncating mutation in the M-line part of titin prompted us to sequence this region in 2 additional patients presenting similar clinical and biochemical characteristics.Results: The 3 patients shared similar features: coexistence of limb-girdle weakness and earlyonset diffuse joint contractures without cardiomyopathy. The biopsies showed rimmed vacuoles, a dystrophic pattern, and secondary reduction in calpain 3. We identified a novel homozygous mutation in the exon Mex3 of the TTN gene in the first patient. At protein level, this mutation introduces a stop codon at the level of Mex3. Interestingly, we identified truncating mutations in both alleles in the same region of the TTN gene in patients from 2 additional families. Molecular protein analyses confirm loss of the C-ter part of titin. Conclusions:

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“…Originellement considérée comme très rare et restreinte aux pays scandinaves, cette titinopathie est en fait relativement fréquente et surtout universelle. Des études récentes ont identifié des mutations de TTN à l'origine de HMERF dans au moins 30 familles d'origines différentes [6][7][8][9][10][11][12]. Certaines mutations retrouvées dans des cas d'HMERF paraissent plus fréquentes en Espagne ou en Grande-Bretagne.…”

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