Your search keyword '"telethonin"' showing total 203 results

1. Clinical and molecular characterization of limb‐girdle muscular dystrophy 2G/R7 in a large cohort of Brazilian patients.

Author

Gaviraghi, Tobias, Cavalcanti, Eduardo B. U., Lorenzoni, Paulo José, Cotta, Ana, de Souza, Paulo V. S., de Oliveira, André D., de Moraes, Maria T., Marques, Marcos V. O., Donis, Karina C., Winckler, Pablo B., Costa e Silva, Cynthia, Pinto, Wladimir B. V. R., Kay, Cláudia S. K., Ducci, Renata D., Rodrigues, Paula R. V. P., Fustes, Otto J. H., da Silva, André M. S., Zanoteli, Edmar, França, Marcondes C., and Sobreira, Cláudia F. R.

Subjects

*MUSCULAR dystrophy, *CONSCIOUSNESS raising, *NATURAL history, *ASIANS, *DISEASE duration

Abstract

Limb‐girdle muscular dystrophy type 2G/R7 (LGMD2G/R7) is an ultra‐rare condition initially identified within the Brazilian population. We aimed to expand clinical and genetic information about this disease, including its worldwide distribution. A multicenter historical cohort study was performed at 13 centers in Brazil in which data from index cases and their affected relatives from consecutive families with LGMD2G/R7 were reviewed from July 2017 to August 2023. Additionally, a systematic literature review was conducted to identify case reports and series of the disease worldwide. Forty‐one LGMD2G/R7 cases were described in the Brazilian cohort, being all subjects homozygous for the c.157C>T/(p.Gln53*) variant in TCAP. Survival curves showed that the median disease duration before individuals required walking aids was 21 years. Notably, women exhibited a slower disease progression, requiring walking aids 13 years later than men. LGMD2G/R7 was frequently reported not only in Brazil but also in China and Bulgaria, with 119 cases identified globally, with possible founder effects in the Brazilian, Eastern European, and Asian populations. These findings are pivotal in raising awareness of LGMD2G/R7, understanding its progression, and identifying potential modifiers. This can significantly contribute to the development of future natural history studies and clinical trials for this disease. [ABSTRACT FROM AUTHOR]

Published

2024

2. Muscle ultrastructure and histopathological findings in a Brazilian single-centre series of genetically classified telethoninopathy patients

Author

Ana Cotta, Elmano Carvalho, Antonio Lopes da-Cunha-Júnior, Eni Braga da Silveira, Bruno Arrivabene Cordeiro, Maria Isabel Lima, Monica Machado Navarro, Frederico Godinho, Jaquelin Valicek, Miriam Melo Menezes, Simone Vilela Nunes-Neves, Antonio Pedro Vargas, Rafael Xavier da-Silva-Neto, Cynthia Costa-e-Silva, Reinaldo Issao Takata, Alexandre Faleiros Cauhi, Julia Filardi Paim, and Mariz Vainzof

Subjects

Telethoninopathy, Telethonin, TCAP, Limb girdle muscular dystrophy, LGMD, LGMDR7, Surgery, RD1-811, Pathology, RB1-214

Abstract

Abstract Background Telethoninopathy or TCAP-gene related Limb Girdle Muscular Dystrophy is a rare genetic disease that was first described in Brazil. There are around 100 families reported worldwide. Due to its rarity, detailed information on muscle biopsy light and electron microscopic features are lacking. Cases presentation Retrospective study of consecutive muscle biopsies performed in patients from a Neuromuscular Outpatient Clinic between 2011 and 2023. Inclusion criteria: telethoninopathy diagnosed by both immunohistochemistry and molecular studies. Seven patients (0.7% or 7/953) were found: five male and two female, admitted from 6 to 54 years old. Detailed light and electron microscopy findings are illustrated. Muscle imaging is presented. A dystrophic pattern on muscle biopsy was found in 57% (4/7) of the patients. Other 43% (3/7) presented myopathic features such as variation in fibre calibre, nuclear internalization, rimmed vacuoles, and oxidative irregularities. Morphometry disclosed type 1 lobulated fibres that were 34%, 52%, and 57% smaller than type 2 fibres, respectively, in three patients, without type 1 fibre predominance. Electron microscopy demonstrated nuclear pseudoinclusions, pyknosis, multifocal loss of the sarcolemma, and 17 nm intrasarcoplasmic filamentous inclusions. All patients presented: (1) complete absence of the immunohistochemical expression of telethonin, and (2) the homozygous c.157C > T, p.(Gln53*) pathogenic variant in exon 2 of the TCAP gene. Conclusion Anti-telethonin immunohistochemistry may be helpful in unsolved cases with nonspecific myopathic abnormalities, specially with small type 1 lobulated fibres. Appropriate diagnosis is important for adequate genetic counselling.

Published

2024

3. Muscle ultrastructure and histopathological findings in a Brazilian single-centre series of genetically classified telethoninopathy patients

Author

Cotta, Ana, Carvalho, Elmano, da-Cunha-Júnior, Antonio Lopes, da Silveira, Eni Braga, Cordeiro, Bruno Arrivabene, Lima, Maria Isabel, Navarro, Monica Machado, Godinho, Frederico, Valicek, Jaquelin, Menezes, Miriam Melo, Nunes-Neves, Simone Vilela, Vargas, Antonio Pedro, da-Silva-Neto, Rafael Xavier, Costa-e-Silva, Cynthia, Takata, Reinaldo Issao, Cauhi, Alexandre Faleiros, Paim, Julia Filardi, and Vainzof, Mariz

Published

2024

4. AAV-based TCAP delivery rescues mitochondria dislocation in limb-girdle muscular dystrophy R7.

Author

Lv X, Liu S, Li X, Lv H, Shao K, Luo S, Zhao D, Yan C, and Lin P

Abstract

Limb-girdle muscular dystrophy R7 is a rare genetic disease caused by homozygous or compound heterozygous variants in the titin-cap (TCAP) gene that results in the absence of the protein telethonin. The primary pathological features of limb-girdle muscular dystrophy R7 are fiber size variation, nuclear centralization, and abnormal mitochondrial distribution. The mechanisms underlying this disease are unclear, and there is currently no specific treatment for limb-girdle muscular dystrophy R7. This study established a Tcap-deficient mouse model to explore the disease mechanism of mitochondria dislocation and potential therapeutic strategies. We use methods such as proteomics, immunofluorescence, histopathological staining, and western blotting to explore the mechanism of mitochondrial dislocation. Moreover, in the quest for a prospective therapeutic intervention for this disorder, the adeno-associated virus serotype 2/9 was employed to deliver the Tcap gene into the muscles of these mice, facilitating preclinical experimentation. After 2 months and 7 months, the muscular phenotype was evaluated and selected mice were humanely euthanized for subsequent molecular and histological analysis. The phenotype of Tcap-/- mice mimicked that observed in individuals diagnosed with limb-girdle muscular dystrophy R7. This study elucidated the mechanism of mitochondrial dislocation in limb-girdle muscular dystrophy R7. Through our in vitro experiments, we discovered that telethonin aids in preserving the integrity of desmin by preventing truncation at the N-terminus. Additionally, telethonin combined with desmin and colocalized at the Z-disc. Research has shown that the Tcap gene plays a crucial role in controlling the desmin cytoskeleton organization. The absence of telethonin leads to a collapsed desmin cytoskeleton. This causes disorganization of the mitochondrial network, leading to mitochondrial dysfunction. In addition, the study investigated the efficacy of adeno-associated virus (AAV)-mediated Tcap replacement in Tcap-/- mice. By intramuscular delivery of AAV, we observed dramatic improvements in muscle phenotype, muscle pathology, CK levels, muscle magnetic resonance imaging, mitochondrial network organization, and mitochondrial function. The results of this study demonstrated that telethonin deficiency led to desmin cytoskeleton collapse that caused mitochondrial dislocation. AAV-mediated replacement therapy could be a promising safe and efficient treatment option for limb-girdle muscular dystrophy R7. The study highlights the potential of AAV-mediated replacement therapy for specific types of limb-girdle muscular dystrophy., (© The Author(s) 2024. Published by Oxford University Press on behalf of the Guarantors of Brain. All rights reserved. For commercial re-use, please contact reprints@oup.com for reprints and translation rights for reprints. All other permissions can be obtained through our RightsLink service via the Permissions link on the article page on our site—for further information please contact journals.permissions@oup.com.)

Published

2024

5. Findings of limb-girdle muscular dystrophy R7 telethonin-related patients from a Chinese neuromuscular center.

Author

Huang, Kun, Li, Qiu-Xiang, Duan, Hui-Qian, Luo, Yue-Bei, Bi, Fang-Fang, and Yang, Huan

Subjects

LIMB-girdle muscular dystrophy, NEUROMUSCULAR diseases, MUSCLE weakness, MUSCULAR atrophy, WESTERN immunoblotting, FAMILIAL spastic paraplegia

Abstract

Limb-girdle muscular dystrophy (LGMD) is a group of clinically and genetically heterogeneous neuromuscular disorders. LGMD-R7, which is caused by telethonin gene (TCAP) mutations, is one of the rarest forms of LGMD, and only a small number of LGMD-R7 cases have been described and mostly include patients from Brazil. A total of two LGMD-R7 patients were enrolled at a Chinese neuromuscular center. Demographic and clinical data were collected. Laboratory investigations and electromyography were performed. Routine and immunohistochemistry staining of muscle specimens was performed, and a next-generation sequencing panel array for genes associated with hereditary neuromuscular disorders was used for analysis. The patients exhibited predominant muscle weakness. Electromyography revealed myopathic changes. The muscle biopsy showed myopathic features, such as increased fiber size variation, muscle fiber atrophy and regeneration, slight hyperplasia of the connective tissue, and disarray of the myofibrillar network. Two patients were confirmed to have mutations in the open reading frame of TCAP by next-generation sequencing. One patient had compound heterozygous mutations, and the other patient harbored a novel homozygous mutation. Western blotting analysis of the skeletal muscle lysate confirmed the absence of telethonin in the patients. We described two LGMD-R7 patients presenting a classical LGMD phenotype and a novel homozygous TCAP mutation. Our research expands the spectrum of LGMD-R7 due to TCAP mutations based on patients from a Chinese neuromuscular center. [ABSTRACT FROM AUTHOR]

Published

2022

6. Phosphorylation at Serines 157 and 161 Is Necessary for Preserving Cardiac Expression Level and Functions of Sarcomeric Z-Disc Protein Telethonin

Author

Hannah R. Lewis, Seda Eminaga, Mathias Gautel, and Metin Avkiran

Subjects

telethonin, TCAP, cardiac hypertrophy, phosphorylation, proteasome, Physiology, QP1-981

Abstract

Aims: In cardiac myocytes, the sarcomeric Z-disc protein telethonin is constitutively bis-phosphorylated at C-terminal residues S157 and S161; however, the functional significance of this phosphorylation is not known. We sought to assess the significance of telethonin phosphorylation in vivo, using a novel knock-in (KI) mouse model generated to express non-phosphorylatable telethonin (TcapS157/161A).Methods and Results:TcapS157/161A and wild-type (WT) littermates were characterized by echocardiography at baseline and after sustained β-adrenergic stimulation via isoprenaline infusion. Heart tissues were collected for gravimetric, biochemical, and histological analyses. At baseline, TcapS157/161A mice did not show any variances in cardiac structure or function compared with WT littermates and mutant telethonin remained localized to the Z-disc. Ablation of telethonin phosphorylation sites resulted in a gene-dosage dependent decrease in the cardiac telethonin protein expression level in mice carrying the S157/161A alleles, without any alteration in telethonin mRNA levels. The proteasome inhibitor MG132 significantly increased the expression level of S157/161A telethonin protein in myocytes from TcapS157/161A mice, but not telethonin protein in myocytes from WT mice, indicating a role for the ubiquitin–proteasome system in the regulation of telethonin protein expression level. TcapS157/161A mice challenged with sustained β-adrenergic stimulation via isoprenaline infusion developed cardiac hypertrophy accompanied by mild systolic dysfunction. Furthermore, the telethonin protein expression level was significantly increased in WT mice following isoprenaline stimulation but this response was blunted in TcapS157/161A mice.Conclusion: Overall, these data reveal that telethonin protein turnover in vivo is regulated in a novel phosphorylation-dependent manner and suggest that C-terminal phosphorylation may protect telethonin against proteasomal degradation and preserve cardiac function during hemodynamic stress. Given that human telethonin C-terminal mutations have been associated with cardiac and skeletal myopathies, further research on their potential impact on phosphorylation-dependent regulation of telethonin protein expression could provide valuable mechanistic insight into those myopathies.

Published

2021

7. Phosphorylation at Serines 157 and 161 Is Necessary for Preserving Cardiac Expression Level and Functions of Sarcomeric Z-Disc Protein Telethonin.

Author

Lewis, Hannah R., Eminaga, Seda, Gautel, Mathias, and Avkiran, Metin

Subjects

C-terminal residues, LABORATORY mice, PROTEIN expression, CARDIAC hypertrophy, PHOSPHORYLATION, N-terminal residues

Abstract

Aims: In cardiac myocytes, the sarcomeric Z-disc protein telethonin is constitutively bis-phosphorylated at C-terminal residues S157 and S161; however, the functional significance of this phosphorylation is not known. We sought to assess the significance of telethonin phosphorylation in vivo , using a novel knock-in (KI) mouse model generated to express non-phosphorylatable telethonin (Tcap S157/161A). Methods and Results: Tcap S157/161A and wild-type (WT) littermates were characterized by echocardiography at baseline and after sustained β-adrenergic stimulation via isoprenaline infusion. Heart tissues were collected for gravimetric, biochemical, and histological analyses. At baseline, Tcap S157/161A mice did not show any variances in cardiac structure or function compared with WT littermates and mutant telethonin remained localized to the Z-disc. Ablation of telethonin phosphorylation sites resulted in a gene-dosage dependent decrease in the cardiac telethonin protein expression level in mice carrying the S157/161A alleles, without any alteration in telethonin mRNA levels. The proteasome inhibitor MG132 significantly increased the expression level of S157/161A telethonin protein in myocytes from Tcap S157/161A mice, but not telethonin protein in myocytes from WT mice, indicating a role for the ubiquitin–proteasome system in the regulation of telethonin protein expression level. Tcap S157/161A mice challenged with sustained β-adrenergic stimulation via isoprenaline infusion developed cardiac hypertrophy accompanied by mild systolic dysfunction. Furthermore, the telethonin protein expression level was significantly increased in WT mice following isoprenaline stimulation but this response was blunted in Tcap S157/161A mice. Conclusion: Overall, these data reveal that telethonin protein turnover in vivo is regulated in a novel phosphorylation-dependent manner and suggest that C-terminal phosphorylation may protect telethonin against proteasomal degradation and preserve cardiac function during hemodynamic stress. Given that human telethonin C-terminal mutations have been associated with cardiac and skeletal myopathies, further research on their potential impact on phosphorylation-dependent regulation of telethonin protein expression could provide valuable mechanistic insight into those myopathies. [ABSTRACT FROM AUTHOR]

Published

2021

8. Functional analysis of a gene‑edited mouse model to gain insights into the disease mechanisms of a titin missense variant.

Author

He Jiang, Hooper, Charlotte, Kelly, Matthew, Steeples, Violetta, Simon, Jillian N., Beglov, Julia, Azad, Amar J., Leinhos, Lisa, Bennett, Pauline, Ehler, Elisabeth, Kalisch‑Smith, Jacinta I., Sparrow, Duncan B., Fischer, Roman, Heilig, Raphael, Isackson, Henrik, Ehsan, Mehroz, Patone, Giannino, Huebner, Norbert, Davies, Benjamin, and Watkins, Hugh

Published

2021

9. Nesprin-2 is a novel scaffold protein for telethonin and FHL-2 in the cardiomyocyte sarcomere.

Author

Li C, Warren DT, Zhou C, De Silva S, Wilson DGS, Garcia-Maya M, Wheeler MA, Meinke P, Sawyer G, Ehler E, Wehnert M, Rao L, Zhang Q, and Shanahan CM

Subjects

Animals, Humans, Mice, Rats, Cytoskeletal Proteins metabolism, Cytoskeletal Proteins genetics, Intracellular Signaling Peptides and Proteins metabolism, Intracellular Signaling Peptides and Proteins genetics, LIM-Homeodomain Proteins, Microfilament Proteins metabolism, Microfilament Proteins genetics, Protein Binding, Transcription Factors, Connectin metabolism, Connectin genetics, LIM Domain Proteins metabolism, LIM Domain Proteins genetics, Muscle Proteins metabolism, Muscle Proteins genetics, Myocytes, Cardiac metabolism, Nerve Tissue Proteins metabolism, Nerve Tissue Proteins genetics, Nuclear Proteins metabolism, Nuclear Proteins genetics, Sarcomeres metabolism

Abstract

Nesprins comprise a family of multi-isomeric scaffolding proteins, forming the linker of nucleoskeleton-and-cytoskeleton complex with lamin A/C, emerin and SUN1/2 at the nuclear envelope. Mutations in nesprin-1/-2 are associated with Emery-Dreifuss muscular dystrophy (EDMD) with conduction defects and dilated cardiomyopathy (DCM). We have previously observed sarcomeric staining of nesprin-1/-2 in cardiac and skeletal muscle, but nesprin function in this compartment remains unknown. In this study, we show that specific nesprin-2 isoforms are highly expressed in cardiac muscle and localize to the Z-disc and I band of the sarcomere. Expression of GFP-tagged nesprin-2 giant spectrin repeats 52 to 53, localized to the sarcomere of neonatal rat cardiomyocytes. Yeast two-hybrid screening of a cardiac muscle cDNA library identified telethonin and four-and-half LIM domain (FHL)-2 as potential nesprin-2 binding partners. GST pull-down and immunoprecipitation confirmed the individual interactions between nesprin-2/telethonin and nesprin-2/FHL-2, and showed that nesprin-2 and telethonin binding was dependent on telethonin phosphorylation status. Importantly, the interactions between these binding partners were impaired by mutations in nesprin-2, telethonin, and FHL-2 identified in EDMD with DCM and hypertrophic cardiomyopathy patients. These data suggest that nesprin-2 is a novel sarcomeric scaffold protein that may potentially participate in the maintenance and/or regulation of sarcomeric organization and function., Competing Interests: Conflict of interest The authors declare that they have no conflicts of interest with the contents of this article., (Crown Copyright © 2024. Published by Elsevier Inc. All rights reserved.)

Published

2024

10. Telethonin variants found in Brugada syndrome, J‐wave pattern ECG, and ARVC reduce peak Nav1.5 currents in HEK‐293 cells.

Author

Turker, Isik, Makiyama, Takeru, Ueyama, Takeshi, Shimizu, Akihiko, Yamakawa, Masaru, Chen, Peng‐Sheng, Vatta, Matteo, Horie, Minoru, and Ai, Tomohiko

Subjects

*MUSCLE protein metabolism, *ARRHYTHMIA, *CARDIAC arrest, *CELL lines, *CYTOLOGY, *ELECTROCARDIOGRAPHY, *ELECTROPHYSIOLOGY, *EPITHELIAL cells, *CASE studies, *GENETIC mutation, *SODIUM, *BRUGADA syndrome, *DESCRIPTIVE statistics, *MEMBRANE transport proteins, *ARRHYTHMOGENIC right ventricular dysplasia

Abstract

Background: Telethonin (TCAP) is a Z‐disk protein that maintains cytoskeletal integrity and various signaling pathways in cardiomyocytes. TCAP is shown to modulate α‐subunit of the human cardiac sodium channel (hNav1.5) by direct interactions. Several TCAP variants are found in cardiomyopathies. We sought to investigate whether TCAP variants are associated with arrhythmia syndromes. Methods: Mutational analyses for TCAP were performed in 303 Japanese patients with Brugada syndrome, arrhythmogenic right ventricular cardiomyopathy, and J‐wave pattern ECG. Using patch‐clamp techniques, electrophysiological characteristics of hNav1.5 were studied in HEK‐293 cells stably expressing hNav1.5 and transiently transfected with wild‐type (WT) or variant TCAP. Results: We identified two TCAP variants, c.145G>A:p.E49K and c.458G>A:p.R153H, in four individuals. p.E49K was found in two patients with ARVC or BrS. p.R153H was found in two patients with BrS or J‐wave pattern ECG. No patient had variant hNav1.5. Patch‐clamp experiments demonstrated that peak sodium currents were significantly reduced in cells expressing p.R153H and p.E49K compared with WT‐TCAP (66%, p.R153H; 72%, p.E49K). Voltage dependency of peak IV curve was rightward‐shifted by 5 mV in cells expressing p.E49K compared with WT‐TCAP. Voltage dependency of activation was not leftward‐shifted by p.R153H, while voltage dependency of steady‐state inactivation was leftward‐shifted by p.E49K. Conclusions: We found two TCAP variants in the patients with BrS, J‐wave pattern ECG, and ARVC that can cause loss‐of‐function of the hNav1.5 in heterologous expression systems. Our observation suggests that these variants might impair INa and be associated with the patients' electrophysiological phenotypes. Further studies linking our experimental data to clinical phenotypes are warranted. [ABSTRACT FROM AUTHOR]

Published

2020

11. A new case of limb girdle muscular dystrophy 2G in a Greek patient, founder effect and review of the literature.

Author

Brusa, Roberta, Magri, Francesca, Papadimitriou, Dimitra, Govoni, Alessandra, Del Bo, Roberto, Ciscato, Patrizia, Savarese, Marco, Cinnante, Claudia, Walter, Maggie C., Abicht, Angela, Bulst, Stefanie, Corti, Stefania, Moggio, Maurizio, Bresolin, Nereo, Nigro, Vincenzo, and Comi, Giacomo Pietro

Subjects

*MUSCULAR dystrophy, *MUSCLE diseases, *SINGLE nucleotide polymorphisms, *WESTERN immunoblotting, *PROTEINS

Abstract

Limb girdle muscular dystrophy (LGMD) type 2G is a rare form of muscle disease, described only in a few patients worldwide, caused by mutations in TCAP gene, encoding the protein telethonin. It is characterised by proximal limb muscle weakness associated with distal involvement of lower limbs, starting in the first or second decade of life. We describe the case of a 37-year-old woman of Greek origin, affected by disto-proximal lower limb weakness. No cardiac or respiratory involvement was detected. Muscle biopsy showed myopathic changes with type I fibre hypotrophy, cytoplasmic vacuoles, lipid overload, multiple central nuclei and fibre splittings; ultrastructural examination showed metabolic abnormalities. Next generation sequencing analysis detected a homozygous frameshift mutation in the TCAP gene (c.90_91del), previously described in one Turkish family. Immunostaining and Western blot analysis showed complete absence of telethonin. Interestingly, Single Nucleotide Polymorphism analysis of the 10 Mb genomic region containing the TCAP gene showed a shared homozygous haplotype of both the Greek and the Turkish patients, thus suggesting a possible founder effect of TCAP gene c.90_91del mutation in this part of the Mediterranean area. [ABSTRACT FROM AUTHOR]

Published

2018

12. Functional analysis of a gene-edited mouse model to gain insights into the disease mechanisms of a titin missense variant

Author

Jiang, He, Hooper, Charlotte, Kelly, Matthew, Steeples, Violetta, Simon, Jillian N., Beglov, Julia, Azad, Amar J., Leinhos, Lisa, Bennett, Pauline, Ehler, Elisabeth, Kalisch-Smith, Jacinta I., Sparrow, Duncan B., Fischer, Roman, Heilig, Raphael, Isackson, Henrik, Ehsan, Mehroz, Patone, Giannino, Huebner, Norbert, Davies, Benjamin, Watkins, Hugh, and Gehmlich, Katja

Published

2021

13. Mechanosignaling pathways alter muscle structure and function by post-translational modification of existing sarcomeric proteins to optimize energy usage

Author

Christopher Solís and Brenda Russell

Subjects

Sarcomeres, 0301 basic medicine, Physiology, Protein degradation, Telethonin, Biochemistry, Sarcomere, Article, 03 medical and health sciences, Myosin head, 0302 clinical medicine, Troponin complex, Humans, Actinin, Connectin, Actin, CapZ Actin Capping Protein, biology, Chemistry, CapZ, Cell Biology, Actins, Cell biology, 030104 developmental biology, biology.protein, Titin, Protein Processing, Post-Translational, 030217 neurology & neurosurgery

Abstract

A transduced mechanical signal arriving at its destination in muscle alters sarcomeric structure and function. A major question addressed is how muscle mass and tension generation are optimized to match actual performance demands so that little energy is wasted. Three cases for improved energy efficiency are examined: the troponin complex for tuning force production, control of the myosin heads in a resting state, and the Z-disc proteins for sarcomere assembly. On arrival, the regulation of protein complexes is often controlled by post-translational modification (PTM), of which the most common are phosphorylation by kinases, deacetylation by histone deacetylases and ubiquitination by E3 ligases. Another branch of signals acts not through peptide covalent bonding but via ligand interactions (e.g. Ca(2+) and phosphoinositide binding). The myosin head and the regulation of its binding to actin by the troponin complex is the best and earliest example of signal destinations that modify myofibrillar contractility. PTMs in the troponin complex regulate both the efficiency of the contractile function to match physiologic demand for work, and muscle mass via protein degradation. The regulation of sarcomere assembly by integration of incoming signaling pathways causing the same PTMs or ligand binding are discussed in response to mechanical loading and unloading by the Z-disc proteins CapZ, α-actinin, telethonin, titin N-termini, and others. Many human mutations that lead to cardiomyopathy and heart disease occur in the proteins discussed above, which often occur at their PTM or ligand binding sites.

Published

2021

14. Expression and purification of a difficult sarcomeric protein: Telethonin.

Author

Tan, Huanbo, Su, Wencheng, Wang, Pengju, Zhang, Wenyu, Sattler, Michael, and Zou, Peijian

Subjects

*SARCOMERES, *IMMUNOGLOBULIN G, *PROTEASE inhibitors, *NUCLEAR magnetic resonance spectroscopy, *GENE expression

Abstract

Telethonin anchors the N-terminal region of titin in the Z-disk of the sarcomere by binding to two immunoglobulin-like (Ig) domains (Z1 and Z2) of titin (Z1Z2). Thereby telethonin plays an important role in myofibril assembly and in muscle development and functional regulation. The expression and purification of recombinant telethonin is very challenging. In previous studies, recombinant telethonin expressed from E. coli was refolded in the presence of Z1Z2. Here, we report various strategies to establish a reliable and efficient protocol for the preparation of telethonin and titin Z1Z2 protein. First, a co-expression strategy was designed to obtain soluble Z1Z2/telethonin complexes. The concentration of antibiotics and the type of expression vector were found to be important for achieving high yields of purified complex. Second, the five cysteine residues of telethonin were mutated to serine to avoid severe problems with cysteine oxidation. Third, a short version of telethonin (telethonin 1-90 ) was designed to avoid the proteolytic degradation observed for longer constructs of the protein. The short telethonin formed a highly stable complex with Z1Z2 with no degradation being observed for 30 days at 4 °C. Fourth, an improved refolding protocol was developed to achieve high yields of Z1Z2/telethonin complex. Finally, based on the crystal structure in which Z1Z2 and telethonin 1-90 assemble into a 2:1 complex, a single chain fusion protein was designed, comprising two Z1Z2 modules that are connected by flexible linkers N- and C-terminally of the telethonin 1-90 . Expression of this fusion protein, named ZTZ, affords high yields of soluble expressed and purified protein. [ABSTRACT FROM AUTHOR]

Published

2017

15. TELETHONIN AS AN EARLY IMMUNOHISTOCHEMICAL MARKER IN LIGATION-INDUCED ISCHEMIC MYOCARDIAL INJURY.

Author

Liang, He-Shiuan, Hsu, Tzu-Cheng, Lu, Pong-Jeu, and Wang, Fun-In

Subjects

IMMUNOSTAINING, NECROSIS, ANIMAL diseases, CORONARY artery abnormalities, METALLOPROTEINASE regulation, DISEASE risk factors

Published

2017

16. Tandem Mass Tag-Based Serum Proteome Profiling for Biomarker Discovery in Young Duchenne Muscular Dystrophy Boys

Author

Tchilabalo Dilezitoko Alayi, Alison M. Samsel, Shefa M. Tawalbeh, Marissa L Barbieri, Holly R Smith, Michael Olarewaju Ogundele, and Yetrib Hathout

Subjects

medicine.medical_specialty, biology, business.industry, General Chemical Engineering, Duchenne muscular dystrophy, General Chemistry, Telethonin, Tandem mass tag, medicine.disease, Blood proteins, Article, Chemistry, Endocrinology, Pantetheinase, Internal medicine, medicine, biology.protein, Vitronectin, Biomarker discovery, Receptor, business, QD1-999

Abstract

Blood-accessible molecular biomarkers are becoming highly attractive tools to assess disease progression and response to therapies in Duchenne muscular dystrophy (DMD) especially in very young patients for whom other outcome measures remain subjective and challenging. In this study, we have standardized a highly specific and reproducible multiplexing mass spectrometry method using the tandem mass tag (TMT) strategy in combination with depletion of abundant proteins from serum and high-pH reversed-phase peptide fractionation. Differential proteome profiling of 4 year-old DMD boys (n = 9) and age-matched healthy controls (n = 9) identified 38 elevated and 50 decreased serum proteins (adjusted P < 0.05, FDR

Published

2020

17. Telethonin variants found in Brugada syndrome, J‐wave pattern ECG, and ARVC reduce peak Na v 1.5 currents in HEK‐293 cells

Author

Minoru Horie, Masaru Yamakawa, Takeshi Ueyama, Peng Sheng Chen, Takeru Makiyama, Isik Turker, Matteo Vatta, Tomohiko Ai, and Akihiko Shimizu

Subjects

medicine.medical_specialty, 030204 cardiovascular system & hematology, Telethonin, sudden cardiac death, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, ARVC, Medicine, 030212 general & internal medicine, telethonin, J wave, Brugada syndrome, business.industry, Brugada, Sodium channel, HEK 293 cells, General Medicine, Transfection, medicine.disease, Phenotype, Electrophysiology, Endocrinology, J-wave syndromes, Cardiology and Cardiovascular Medicine, business, arrhythmias

Abstract

Background:Telethonin (TCAP) is a Z-disk protein that maintains cytoskeletal integrity and various signaling pathways in cardiomyocytes. TCAP is shown to modulate α-subunit of the human cardiac sodium channel (hNav 1.5) by direct interactions. Several TCAP variants are found in cardiomyopathies. We sought to investigate whether TCAP variants are associated with arrhythmia syndromes., Methods:Mutational analyses for TCAP were performed in 303 Japanese patients with Brugada syndrome, arrhythmogenic right ventricular cardiomyopathy, and J-wave pattern ECG. Using patch-clamp techniques, electrophysiological characteristics of hNav 1.5 were studied in HEK-293 cells stably expressing hNav 1.5 and transiently transfected with wild-type (WT) or variant TCAP., Results:We identified two TCAP variants, c.145G>A:p.E49K and c.458G>A:p.R153H, in four individuals. p.E49K was found in two patients with ARVC or BrS. p.R153H was found in two patients with BrS or J-wave pattern ECG. No patient had variant hNav 1.5. Patch-clamp experiments demonstrated that peak sodium currents were significantly reduced in cells expressing p.R153H and p.E49K compared with WT-TCAP (66%, p.R153H; 72%, p.E49K). Voltage dependency of peak IV curve was rightward-shifted by 5 mV in cells expressing p.E49K compared with WT-TCAP. Voltage dependency of activation was not leftward-shifted by p.R153H, while voltage dependency of steady-state inactivation was leftward-shifted by p.E49K., Conclusions:We found two TCAP variants in the patients with BrS, J-wave pattern ECG, and ARVC that can cause loss-of-function of the hNav 1.5 in heterologous expression systems. Our observation suggests that these variants might impair INa and be associated with the patients' electrophysiological phenotypes. Further studies linking our experimental data to clinical phenotypes are warranted.

Published

2020

18. Identification of a novel titin-cap/telethonin mutation in a Portuguese family with hypertrophic cardiomyopathy

Author

Cemil Özcelik, Nuno Cardim, Andreas Perrot, and Alexandra Toste

Subjects

lcsh:Diseases of the circulatory (Cardiovascular) system, Population, Telethonin, Biology, Sudden cardiac death, 03 medical and health sciences, 0302 clinical medicine, Teletonina, medicine, Humans, Miocardiopatia hipertrófica, Connectin, cardiovascular diseases, 030212 general & internal medicine, Family history, education, General Environmental Science, Genetics, education.field_of_study, Portugal, Hypertrophic cardiomyopathy, Titin-cap, Cardiomyopathy, Hypertrophic, medicine.disease, Variante provavelmente patogénica, 030228 respiratory system, Cardiovascular and Metabolic Diseases, lcsh:RC666-701, Mutation (genetic algorithm), Mutation, cardiovascular system, General Earth and Planetary Sciences, MYH7, Mutação do gene TCAP, Cardiology and Cardiovascular Medicine, Heart failure with preserved ejection fraction, Carrier Proteins

Abstract

Introduction and objectives: Hypertrophic cardiomyopathy (HCM) is a genetically and phenotypically heterogeneous disease; there is still a large proportion of patients with no identified disease-causing mutation. Although the majority of mutations are found in the MYH7 and MYBPC3 genes, mutations in Z-disk-associated proteins have also been linked to HCM. Methods: We assessed a small family with HCM based on family history, physical examination, 12-lead ECG, echocardiogram and magnetic resonance imaging. After exclusion of mutations in eleven HCM disease genes, we performed direct sequencing of the TCAP gene encoding the Z-disk protein titin-cap (also known as telethonin). Results: We present a novel TCAP mutation in a small family affected by HCM. The identified p.C57W mutation showed a very low population frequency, as well as high conservation across species. All of the bioinformatic prediction tools used considered this mutation to be damaging/deleterious. Family members were screened for this new mutation and a co-segregation pattern was detected. Both affected members of this family presented with late-onset HCM, moderate asymmetric left ventricular hypertrophy, atrial fibrillation and heart failure with preserved ejection fraction and low risk of sudden cardiac death. Conclusions: We present evidence supporting the classification of the TCAP p.C57W mutation, encoding the Z-disk protein titin-cap/telethonin as a new likely pathogenic variant of hypertrophic cardiomyopathy, with a specific phenotype in the family under analysis. Resumo: Introdução e objetivos: A miocardiopatia hipertrófica (HCM) é uma doença genética e fenotipicamente heterogénea, existindo ainda uma grande proporção de doentes sem uma mutação patogénica identificada. Embora a maioria das mutações seja encontrada nos genes MYH7 e MYBPC3, mutações em proteínas associadas ao disco Z também foram associadas à HCM. Métodos: Avaliámos uma pequena família com HCM com base na história familiar e exame objetivo, eletrocardiograma de 12 derivações, ecocardiograma e ressonância magnética. Após exclusão de mutações em 11 genes causadores de HCM, realizámos a sequenciação direta do gene TCAP que codifica a proteína titin-cap do disco-Z (também conhecida como teletonina). Resultados: Relatamos aqui uma nova mutação do gene TCAP numa pequena família com HCM. A mutação identificada, p.C57W, mostrou uma frequência populacional muito baixa, bem como alta conservação entre as espécies. Todas as ferramentas de previsão de bioinformática usadas previram que essa mutação seria funcionalmente prejudicial. A presença desta nova mutação foi avaliada nos outros membros da família, tendo-se detetado um padrão de cossegregação. Ambos os membros da família afetados apresentaram HCM de início tardio, com hipertrofia ventricular esquerda assimétrica moderada, fibrilhação auricular e insuficiência cardíaca com fracão de ejeção preservada, com baixo risco de morte súbita cardíaca. Conclusão: Apresentamos evidência que suporta a classificação da mutação TCAP p.C57W, que codifica a proteína titin-cap do disco-Z (teletonina), como uma nova variante provavelmente patogénica da HCM, com um perfil fenotípico específico na família analisada.

Published

2020

19. Clinical and genetic characterization of limb girdle muscular dystrophy R7 telethonin-related patients from three unrelated Chinese families

Author

Min-Ting Lin, Hai-Zhu Chen, Nai-Qing Cai, Zhixian Ye, Ning Wang, Feng Lin, Guo-Rong Xu, Lili Wang, Liangliang Qiu, and Ming Jin

Subjects

Adult, Male, musculoskeletal diseases, 0301 basic medicine, China, Pathology, medicine.medical_specialty, Proximal muscle weakness, Telethonin, Muscle disorder, 03 medical and health sciences, 0302 clinical medicine, medicine, Humans, Connectin, Progressive proximal muscle weakness, Age of Onset, Muscular dystrophy, Muscle, Skeletal, Genetics (clinical), Pelvic girdle, business.industry, Middle Aged, medicine.disease, Magnetic Resonance Imaging, Muscle atrophy, Pedigree, 030104 developmental biology, Muscular Dystrophies, Limb-Girdle, Neurology, Pediatrics, Perinatology and Child Health, Female, Neurology (clinical), medicine.symptom, business, 030217 neurology & neurosurgery, Limb-girdle muscular dystrophy

Abstract

Limb girdle muscular dystrophy LGMD R7 telethonin-related is a rare autosomal recessive muscle disorder characterized by proximal muscle weakness of pelvic and shoulder girdles. Mutation in TCAP is responsible for LGMD R7, and the disease has a wide geographic distribution in diverse populations, but genotype-phenotype relationships remain unclear. We collected 5 LGMD R7 patients from three unrelated Chinese families. The average onset age was 16 ± 1.41; the initial symptoms included progressive proximal muscle weakness in limbs, difficulty in fast running, and asymmetric muscle atrophy in calves. Muscle MR imaging showed varying severity of fatty infiltration in the pelvic girdle, thigh, and calf muscles, and the severity of muscle infiltration was related to the length of the disease course. Muscle histopathology revealed aberrantly sized muscle fibers, internal nuclei, split fibers, rimmed vacuoles, monocyte invasion, and necrotic fibers. Sequencing identified one novel and one previously reported TCAP mutation. Our study extends the known distribution of this rare muscular dystrophy and presents the first detailed clinical and genetic characterizations of LGMD R7 cases from the Chinese population. Our work expands the mutation spectrum known for LGMD R7 and emphasizes the need for clinicians to consider TCAP mutations when evaluating patients with symptoms of limb girdle muscular dystrophy.

Published

2020

20. Disordered yet functional atrial t-tubules on recovery from heart failure

Author

David A. Eisner, Christian Pinali, Emma J. Radcliffe, Charles M. Pearman, Katharine M. Dibb, Charlotte E.R. Smith, Andrew W. Trafford, Amy E. Watkins, Margaux A. Horn, Jessica D. Clarke, Jessica L. Caldwell, Elizabeth F. Bode, Mark Eisner, Aiste Adomaviciene, and Callum J. Quinn

Subjects

Serial block-face scanning electron microscopy, medicine.medical_specialty, medicine.diagnostic_test, Chemistry, Myotubularin, Telethonin, medicine.disease, Tubule, Western blot, Internal medicine, Heart failure, medicine, Ultrastructure, Cardiology, Myocyte

Abstract

Transverse (t)-tubules drive the rapid and synchronous Ca2+ rise in cardiac myocytes. The virtual complete loss of atrial t-tubules in heart failure (HF) decreases Ca2+ release. It is unknown if or how atrial t-tubules can be restored and if restored t-tubules are functional.Sheep were tachypaced to induce HF and recovered when pacing was stopped. Serial block face Scanning Electron Microscopy and confocal imaging were used to understand t-tubule ultrastructure and function. Candidate proteins involved in atrial t-tubule recovery were identified by western blot and causality determined using expression studies.Sheep atrial t-tubules reappeared following recovery from HF. Despite being disordered (branched, longer and longitudinally arranged) recovered t-tubules triggered Ca2+ release and were associated with restoration of systolic Ca2+. Telethonin and myotubularin abundance correlated with t-tubule density and altered the density and structure of BIN1-driven tubules in neonatal myocytes. Myotubularin had a greater effect, increasing tubule length and branching, replicating that seen in the recovery atria.Recovery from HF restores atrial t-tubules and systolic Ca2+ and myotubularin facilitates this process. Atrial t-tubule restoration could present a new and viable therapeutic strategy.Brief SummaryThe loss of atrial transverse (t)-tubules and the associated dysfunction in heart failure is reversible and the protein myotubularin plays an important role.

Published

2021

21. Combination of Whole Genome Sequencing, Linkage, and Functional Studies Implicates a Missense Mutation in Titin as a Cause of Autosomal Dominant Cardiomyopathy With Features of Left Ventricular Noncompaction.

Author

Hastings, Robert, de Villiers, Carin P., Hooper, Charlotte, Ormondroyd, Liz, Pagnamenta, Alistair, Lise, Stefano, Salatino, Silvia, Knight, Samantha J. L., Taylor, Jenny C., Thomson, Kate L., Arnold, Linda, Chatziefthimiou, Spyros D., Konarev, Petr V., Wilmanns, Matthias, Ehler, Elisabeth, Ghisleni, Andrea, Gautel, Mathias, Blair, Edward, Watkins, Hugh, and Gehmlich, Katja

Subjects

MISSENSE mutation, TREATMENT of cardiomyopathies, GEL permeation chromatography

Abstract

Background--High throughput next-generation sequencing techniques have made whole genome sequencing accessible in clinical practice; however, the abundance of variation in the human genomes makes the identification of a disease-causing mutation on a background of benign rare variants challenging. Methods and Results--Here we combine whole genome sequencing with linkage analysis in a 3-generation family affected by cardiomyopathy with features of autosomal dominant left ventricular noncompaction cardiomyopathy. A missense mutation in the giant protein titin is the only plausible disease-causing variant that segregates with disease among the 7 surviving affected individuals, with interrogation of the entire genome excluding other potential causes. This A178D missense mutation, affecting a conserved residue in the second immunoglobulin-like domain of titin, was introduced in a bacterially expressed recombinant protein fragment and biophysically characterized in comparison to its wild-type counterpart. Multiple experiments, including size exclusion chromatography, small-angle x ray scattering, and circular dichroism spectroscopy suggest partial unfolding and domain destabilization in the presence of the mutation. Moreover, binding experiments in mammalian cells show that the mutation markedly impairs binding to the titin ligand telethonin. Conclusions--Here we present genetic and functional evidence implicating the novel A178D missense mutation in titin as the cause of a highly penetrant familial cardiomyopathy with features of left ventricular noncompaction. This expands the spectrum of titin's roles in cardiomyopathies. It furthermore highlights that rare titin missense variants, currently often ignored or left uninterpreted, should be considered to be relevant for cardiomyopathies and can be identified by the approach presented here. [ABSTRACT FROM AUTHOR]

Published

2016

22. Phosphorylation at Serines 157 and 161 Is Necessary for Preserving Cardiac Expression Level and Functions of Sarcomeric Z-Disc Protein Telethonin

Author

Metin Avkiran, Seda Eminaga, Mathias Gautel, and Hannah R. Lewis

Subjects

Cardiac function curve, Chemistry, phosphorylation, Physiology, cardiac hypertrophy, Protein turnover, Telethonin, Cell biology, chemistry.chemical_compound, proteasome, Physiology (medical), Isoprenaline, MG132, medicine, Proteasome inhibitor, Phosphorylation, Myocyte, QP1-981, telethonin, TCAP, medicine.drug, Original Research

Abstract

Aims: In cardiac myocytes, the sarcomeric Z-disc protein telethonin is constitutively bis-phosphorylated at C-terminal residues S157 and S161; however, the functional significance of this phosphorylation is not known. We sought to assess the significance of telethonin phosphorylation in vivo, using a novel knock-in (KI) mouse model generated to express non-phosphorylatable telethonin (TcapS157/161A).Methods and Results:TcapS157/161A and wild-type (WT) littermates were characterized by echocardiography at baseline and after sustained β-adrenergic stimulation via isoprenaline infusion. Heart tissues were collected for gravimetric, biochemical, and histological analyses. At baseline, TcapS157/161A mice did not show any variances in cardiac structure or function compared with WT littermates and mutant telethonin remained localized to the Z-disc. Ablation of telethonin phosphorylation sites resulted in a gene-dosage dependent decrease in the cardiac telethonin protein expression level in mice carrying the S157/161A alleles, without any alteration in telethonin mRNA levels. The proteasome inhibitor MG132 significantly increased the expression level of S157/161A telethonin protein in myocytes from TcapS157/161A mice, but not telethonin protein in myocytes from WT mice, indicating a role for the ubiquitin–proteasome system in the regulation of telethonin protein expression level. TcapS157/161A mice challenged with sustained β-adrenergic stimulation via isoprenaline infusion developed cardiac hypertrophy accompanied by mild systolic dysfunction. Furthermore, the telethonin protein expression level was significantly increased in WT mice following isoprenaline stimulation but this response was blunted in TcapS157/161A mice.Conclusion: Overall, these data reveal that telethonin protein turnover in vivo is regulated in a novel phosphorylation-dependent manner and suggest that C-terminal phosphorylation may protect telethonin against proteasomal degradation and preserve cardiac function during hemodynamic stress. Given that human telethonin C-terminal mutations have been associated with cardiac and skeletal myopathies, further research on their potential impact on phosphorylation-dependent regulation of telethonin protein expression could provide valuable mechanistic insight into those myopathies.

Published

2021

23. Conserved expression of truncated telethonin in a patient with limb-girdle muscular dystrophy 2G.

Author

Barresi, Rita, Morris, Charlotte, Hudson, Judith, Curtis, Elizabeth, Pickthall, Clare, Bushby, Kate, Davies, Nicholas P., and Straub, Volker

Subjects

*LIMB-girdle muscular dystrophy, *GENE expression, *GENETIC mutation, *PHENOTYPES, *IMMUNOHISTOCHEMISTRY, *WESTERN immunoblotting

Abstract

Limb-girdle muscular dystrophy 2G is caused by mutations in the TCAP gene that encodes for telethonin. Here we describe a 49 year-old male patient of Indian descent presenting a classical LGMD phenotype. He had normal motor milestones but became noticeably slower in his early teens and was wheelchair bound by age 44. The muscle biopsy showed myopathic features and absence of labeling with an antibody to the C-terminal portion of telethonin. Sequence analysis of the TCAP gene revealed a novel homozygous mutation in exon 2, predicted to generate a truncated protein of 81 amino acids. Interestingly, an antibody for the full-length protein showed labeling on sections and a single band of ~10 kDa on Western blot. The truncated protein co-localized with filamin C at the Z-line. Our findings indicate that mutant telethonin can be incorporated into the sarcomere and that other LGMD2G patients with retention of telethonin expression may exist. [ABSTRACT FROM AUTHOR]

Published

2015

24. The role of Z-disc proteins in myopathy and cardiomyopathy

Author

Katja Gehmlich, Kirsty Wadmore, and Amar J. Azad

Subjects

0301 basic medicine, myotilin, Muscle Proteins, Review, Telethonin, Biology, Filamin, Models, Biological, Z-disc alternatively spliced PDZ-motif (ZASP), Sarcomere, Catalysis, lcsh:Chemistry, Inorganic Chemistry, 03 medical and health sciences, 0302 clinical medicine, Muscular Diseases, medicine, Animals, Humans, Myotilin, Myocyte, Physical and Theoretical Chemistry, Myopathy, lcsh:QH301-705.5, telethonin, Molecular Biology, Spectroscopy, Actin, Organic Chemistry, Skeletal muscle, General Medicine, missense variant, truncating variant, Computer Science Applications, Cell biology, myopalladin, α-actinin 2, 030104 developmental biology, medicine.anatomical_structure, lcsh:Biology (General), lcsh:QD1-999, Mutation, medicine.symptom, Cardiomyopathies, cardiomyopathy, 030217 neurology & neurosurgery, filamin C, myopathy

Abstract

The Z-disc acts as a protein-rich structure to tether thin filament in the contractile units, the sarcomeres, of striated muscle cells. Proteins found in the Z-disc are integral for maintaining the architecture of the sarcomere. They also enable it to function as a (bio-mechanical) signalling hub. Numerous proteins interact in the Z-disc to facilitate force transduction and intracellular signalling in both cardiac and skeletal muscle. This review will focus on six key Z-disc proteins: α-actinin 2, filamin C, myopalladin, myotilin, telethonin and Z-disc alternatively spliced PDZ-motif (ZASP), which have all been linked to myopathies and cardiomyopathies. We will summarise pathogenic variants identified in the six genes coding for these proteins and look at their involvement in myopathy and cardiomyopathy. Listing the Minor Allele Frequency (MAF) of these variants in the Genome Aggregation Database (GnomAD) version 3.1 will help to critically re-evaluate pathogenicity based on variant frequency in normal population cohorts.

Published

2021

25. Sarcomere Shortening of Pluripotent Stem Cell-Derived Cardiomyocytes using Fluorescent-Tagged Sarcomere Proteins

Author

Keiichiro Koiwai, Hiroaki Suzuki, Nawin Chanthra, Tomoki Murakami, Razan Elfadil Ahmed, Tatsuya Anzai, Hideki Uosaki, and Yutaka Hanazono

Subjects

Pluripotent Stem Cells, Sarcomeres, General Chemical Engineering, Cellular differentiation, Biology, Telethonin, Time-Lapse Imaging, Sarcomere, General Biochemistry, Genetics and Molecular Biology, Mice, Live cell imaging, Animals, Humans, Myocyte, Myocytes, Cardiac, Induced pluripotent stem cell, Cells, Cultured, Embryoid Bodies, Fluorescent Dyes, Staining and Labeling, General Immunology and Microbiology, General Neuroscience, Cell Differentiation, Mouse Embryonic Stem Cells, Dependovirus, MYOM2, Embryonic stem cell, Cell biology

Abstract

Pluripotent stem cell-derived cardiomyocytes (PSC-CMs) can be produced from both embryonic and induced pluripotent stem (ES/iPS) cells. These cells provide promising sources for cardiac disease modeling. For cardiomyopathies, sarcomere shortening is one of the standard physiological assessments that are used with adult cardiomyocytes to examine their disease phenotypes. However, the available methods are not appropriate to assess the contractility of PSC-CMs, as these cells have underdeveloped sarcomeres that are invisible under phase-contrast microscopy. To address this issue and to perform sarcomere shortening with PSC-CMs, fluorescent-tagged sarcomere proteins and fluorescent live-imaging were used. Thin Z-lines and an M-line reside at both ends and the center of a sarcomere, respectively. Z-line proteins - α-Actinin (ACTN2), Telethonin (TCAP), and actin-associated LIM protein (PDLIM3) - and one M-line protein - Myomesin-2 (Myom2) - were tagged with fluorescent proteins. These tagged proteins can be expressed from endogenous alleles as knock-ins or from adeno-associated viruses (AAVs). Here, we introduce the methods to differentiate mouse and human pluripotent stem cells to cardiomyocytes, to produce AAVs, and to perform and analyze live-imaging. We also describe the methods for producing polydimethylsiloxane (PDMS) stamps for a patterned culture of PSC-CMs, which facilitates the analysis of sarcomere shortening with fluorescent-tagged proteins. To assess sarcomere shortening, time-lapse images of the beating cells were recorded at a high framerate (50-100 frames per second) under electrical stimulation (0.5-1 Hz). To analyze sarcomere length over the course of cell contraction, the recorded time-lapse images were subjected to SarcOptiM, a plug-in for ImageJ/Fiji. Our strategy provides a simple platform for investigating cardiac disease phenotypes in PSC-CMs.

Published

2021

26. Functional analysis of a gene-edited mouse to gain insights into the disease mechanisms of a titin missense variant

Author

Julia Beglov, Henrik Isackson, Elisabeth Ehler, Jacinta I. Kalisch-Smith, Violetta Steeples, Duncan B. Sparrow, Katja Gehmlich, Pauline M. Bennett, Norbert Huebner, Charlotte Hooper, Raphael Heilig, Giannino Patone, Benjamin Davies, Hugh Watkins, Amar J. Azad, He Jiang, Mehroz Ehsan, Lisa Leinhos, Jillian N. Simon, Roman Fischer, and Matthew Kelly

Subjects

Proteome, Physiology, Cardiomyopathy, 030204 cardiovascular system & hematology, Ventricular Function, Left, 0302 clinical medicine, Missense mutation, Cardiac and Cardiovascular Systems, Connectin, Gene Editing, 0303 health sciences, Kardiologi, biology, Homozygote, Age Factors, Titin missense variant, Original Contribution, Phenotype, Cell biology, Titin, Cardiomyopathies, Cardiology and Cardiovascular Medicine, Heterozygote, Proteasome Endopeptidase Complex, Telethonin, Mutation, Missense, Mouse model, 03 medical and health sciences, Downregulation and upregulation, Physiology (medical), Heat shock protein, medicine, Animals, Genetic Predisposition to Disease, Proteo-toxic response, 030304 developmental biology, LIM domain, Proteasome, medicine.disease, Mice, Mutant Strains, Mice, Inbred C57BL, Cardiovascular and Metabolic Diseases, Proteolysis, biology.protein, Transcriptome, Protein Kinases

Abstract

Titin truncating variants are a well-established cause of cardiomyopathy; however, the role of titin missense variants is less well understood. Here we describe the generation of a mouse model to investigate the underlying disease mechanism of a previously reported titin A178D missense variant identified in a family with non-compaction and dilated cardiomyopathy. Heterozygous and homozygous mice carrying the titin A178D missense variant were characterised in vivo by echocardiography. Heterozygous mice had no detectable phenotype at any time point investigated (up to 1 year). By contrast, homozygous mice developed dilated cardiomyopathy from 3 months. Chronic adrenergic stimulation aggravated the phenotype. Targeted transcript profiling revealed induction of the foetal gene programme and hypertrophic signalling pathways in homozygous mice, and these were confirmed at the protein level. Unsupervised proteomics identified downregulation of telethonin and four-and-a-half LIM domain 2, as well as the upregulation of heat shock proteins and myeloid leukaemia factor 1. Loss of telethonin from the cardiac Z-disc was accompanied by proteasomal degradation; however, unfolded telethonin accumulated in the cytoplasm, leading to a proteo-toxic response in the mice.We show that the titin A178D missense variant is pathogenic in homozygous mice, resulting in cardiomyopathy. We also provide evidence of the disease mechanism: because the titin A178D variant abolishes binding of telethonin, this leads to its abnormal cytoplasmic accumulation. Subsequent degradation of telethonin by the proteasome results in proteasomal overload, and activation of a proteo-toxic response. The latter appears to be a driving factor for the cardiomyopathy observed in the mouse model. Supplementary Information The online version contains supplementary material available at 10.1007/s00395-021-00853-z.

Published

2021

27. A pilot study of muscle plasma protein changes after exercise.

Author

Dahlqvist, Julia R., Voss, Line G., Lauridsen, Thomas, Krag, Thomas O., and Vissing, John

Abstract

ABSTRACT Introduction: Creatine kinase (CK) and myoglobin (Mb) do not possess all good qualities as biomarkers of skeletal muscle damage. We investigated the utility of troponin I (TnI) and telethonin (Tcap) as markers and examined their temporal profiles after skeletal muscle damage. Methods: Plasma profiles were measured before and after exercise in 3 groups: subjects affected by either Becker muscular dystrophy or McArdle disease, and healthy subjects. Results: Mb and TnI appeared early in the blood, and the increase of TnI was only observed in patients with muscle disease. The CK increase was more delayed in plasma. Tcap was not detectable at any time. Conclusions: Our results suggest that TnI is a marker of more severe damage signifying sarcomeric damage, and it could therefore be an important supplement to CK and Mb in clinical practice. Tcap is not useful as a marker for skeletal muscle damage. Muscle Nerve 49: 261-266, 2014 [ABSTRACT FROM AUTHOR]

Published

2014

28. Limb Girdle Muscular Dystrophies

Author

Matthew Wicklund and Jacob Bockhorst

Subjects

Adult, Male, Pathology, medicine.medical_specialty, Limb girdle, Telethonin, Dysferlin, 03 medical and health sciences, 0302 clinical medicine, medicine, Humans, 030212 general & internal medicine, Muscle, Skeletal, Muscle biopsy, Fukutin-related protein, medicine.diagnostic_test, biology, business.industry, Skeletal muscle, Middle Aged, medicine.disease, Sarcoglycan, medicine.anatomical_structure, Muscular Dystrophies, Limb-Girdle, biology.protein, Disease Progression, Female, Neurology (clinical), business, 030217 neurology & neurosurgery, Limb-girdle muscular dystrophy

Abstract

The limb girdle muscular dystrophies (LGMDs) are genetic muscle diseases with primary skeletal muscle involvement in persons with the ability to walk independently at some point in the disease course. They usually have increased creatine kinase levels along with patterns of fatty and fibrous deposition on muscle imaging and/or dystrophic features on muscle biopsy. Distinctive clinical features provide valuable diagnostic clues to the diagnosis and sometimes treatment of these disorders. The advent of gene and cell-based therapies; gene replacement, editing, and modulation; along with stem cell and small molecule therapies may significantly ameliorate clinical severity in the LGMDs.

Published

2020

29. Identification of a novel titin-cap/telethonin mutation in a Portuguese family with hypertrophic cardiomyopathy

Author

Toste, Alexandra, Perrot, Andreas, Özcelik, Cemil, Cardim, Nuno, and NOVA Medical School|Faculdade de Ciências Médicas (NMS|FCM)

Subjects

Telethonin, TCAP mutation, Likely pathogenic variant, Titin-cap, Cardiology and Cardiovascular Medicine, Hypertrophic cardiomyopathy

Abstract

Introduction and objectives: Hypertrophic cardiomyopathy (HCM) is a genetically and phenotypically heterogeneous disease; there is still a large proportion of patients with no identified disease-causing mutation. Although the majority of mutations are found in the MYH7 and MYBPC3 genes, mutations in Z-disk-associated proteins have also been linked to HCM. Methods: We assessed a small family with HCM based on family history, physical examination, 12-lead ECG, echocardiogram and magnetic resonance imaging. After exclusion of mutations in eleven HCM disease genes, we performed direct sequencing of the TCAP gene encoding the Z-disk protein titin-cap (also known as telethonin). Results: We present a novel TCAP mutation in a small family affected by HCM. The identified p.C57W mutation showed a very low population frequency, as well as high conservation across species. All of the bioinformatic prediction tools used considered this mutation to be damaging/deleterious. Family members were screened for this new mutation and a co-segregation pattern was detected. Both affected members of this family presented with late-onset HCM, moderate asymmetric left ventricular hypertrophy, atrial fibrillation and heart failure with preserved ejection fraction and low risk of sudden cardiac death. Conclusions: We present evidence supporting the classification of the TCAP p.C57W mutation, encoding the Z-disk protein titin-cap/telethonin as a new likely pathogenic variant of hypertrophic cardiomyopathy, with a specific phenotype in the family under analysis. publishersversion published

Published

2020

30. A new case of limb girdle muscular dystrophy 2G in a Greek patient, founder effect and review of the literature

Author

Patrizia Ciscato, Roberto Del Bo, Roberta Brusa, Angela Abicht, Francesca Magri, Stefania Corti, Vincenzo Nigro, Marco Savarese, Nereo Bresolin, Alessandra Govoni, Dimitra Papadimitriou, Giacomo P. Comi, Maurizio Moggio, Claudia Cinnante, Maggie C. Walter, Stefanie Bulst, Brusa, Roberta, Magri, Francesca, Papadimitriou, Dimitra, Govoni, Alessandra, Del Bo, Roberto, Ciscato, Patrizia, Savarese, Marco, Cinnante, Claudia, Walter, Maggie C., Abicht, Angela, Bulst, Stefanie, Corti, Stefania, Moggio, Maurizio, Bresolin, Nereo, Nigro, Vincenzo, and Comi, Giacomo Pietro

Subjects

Adult, 0301 basic medicine, Pathology, medicine.medical_specialty, Telethonin, Biology, medicine.disease_cause, Polymorphism, Single Nucleotide, Frameshift mutation, 03 medical and health sciences, 0302 clinical medicine, Limb girdle muscular dystrophy 2G, medicine, Humans, Connectin, Muscle, Skeletal, Genetics (clinical), Mutation, Muscle biopsy, Greece, medicine.diagnostic_test, Haplotype, Skeletal muscle, TCAP gene, medicine.disease, Founder Effect, 3. Good health, 030104 developmental biology, medicine.anatomical_structure, Muscular Dystrophies, Limb-Girdle, Neurology, Pediatrics, Perinatology and Child Health, Female, Neurology (clinical), 030217 neurology & neurosurgery, Limb-girdle muscular dystrophy, Founder effect

Abstract

Limb girdle muscular dystrophy (LGMD) type 2G is a rare form of muscle disease, described only in a few patients worldwide, caused by mutations in TCAP gene, encoding the protein telethonin. It is characterised by proximal limb muscle weakness associated with distal involvement of lower limbs, starting in the first or second decade of life. We describe the case of a 37-year-old woman of Greek origin, affected by disto-proximal lower limb weakness. No cardiac or respiratory involvement was detected. Muscle biopsy showed myopathic changes with type I fibre hypotrophy, cytoplasmic vacuoles, lipid overload, multiple central nuclei and fibre splittings; ultrastructural examination showed metabolic abnormalities. Next generation sequencing analysis detected a homozygous frameshift mutation in the TCAP gene (c.90_91del), previously described in one Turkish family. Immunostaining and Western blot analysis showed complete absence of telethonin. Interestingly, Single Nucleotide Polymorphism analysis of the 10 Mb genomic region containing the TCAP gene showed a shared homozygous haplotype of both the Greek and the Turkish patients, thus suggesting a possible founder effect of TCAP gene c.90_91del mutation in this part of the Mediterranean area.

Published

2018

31. Reduced dietary intake of micronutrients with antioxidant properties negatively impacts muscle health in aged mice

Author

van Dijk, Miriam, Dijk, Francina J., Hartog, Anita, van Norren, Klaske, Verlaan, Sjors, van Helvoort, Ardy, Jaspers, Richard T., Luiking, Yvette, RS: NUTRIM - R3 - Respiratory & Age-related Health, Bedrijfsbureau NTM, Internal medicine, Physiology, and AMS - Ageing and Morbidity

Subjects

Adult, Male, lcsh:Diseases of the musculoskeletal system, UBIQUITIN-CONJUGATING ENZYME, TELETHONIN, Antioxidants, lcsh:QM1-695, Mice, Young Adult, Animals, Humans, E2 ENZYMES, Micronutrients, Function, Muscle, Skeletal, SDG 2 - Zero Hunger, GENE-EXPRESSION, Nutrition, DEPENDENT PROTEOLYSIS, Muscle quality, E3 LIGASE MURF1, PROTEIN LIGASES, RAT SOLEUS MUSCLE, Original Articles, lcsh:Human anatomy, Diet, Mice, Inbred C57BL, RING-FINGER, SKELETAL-MUSCLE, Original Article, Strength, lcsh:RC925-935

Abstract

Background: Inadequate intake of micronutrients with antioxidant properties is common among older adults and has been associated with higher risk of frailty, adverse functional outcome, and impaired muscle health. However, a causal relationship is less well known. The aim was to determine in old mice the impact of reduced dietary intake of vitamins A/E/B6/B12/folate, selenium, and zinc on muscle mass, oxidative capacity, strength, and physical activity (PA) over time. Methods: Twenty-one-month-old male mice were fed either AIN-93-M (control) or a diet low in micronutrients with antioxidant properties (=LOWOX-B: 50% of mouse recommended daily intake of vitamins A, E, B6, and B12, folate, selenium, and zinc) for 4 months. Muscle mass, grip strength, physical activity (PA), and general oxidative status were assessed. Moreover, muscle fatigue was measured of m. extensor digitorum longus (EDL) during an ex vivo moderate exercise protocol. Effects on oxidative capacity [succinate dehydrogenase (SDH) activity], muscle fibre type, number, and fibre cross-sectional area (fCSA) were assessed on m. plantaris (PL) using histochemistry. Results: After 2 months on the diet, bodyweight of LOWOX-B mice was lower compared with control (P

Published

2018

32. Reduced dietary intake of micronutrients with antioxidant properties negatively impacts muscle health in aged mice

Subjects

Muscle quality, DEPENDENT PROTEOLYSIS, E3 LIGASE MURF1, PROTEIN LIGASES, RAT SOLEUS MUSCLE, UBIQUITIN-CONJUGATING ENZYME, TELETHONIN, Antioxidants, RING-FINGER, SKELETAL-MUSCLE, E2 ENZYMES, Strength, Function, Nutrition, GENE-EXPRESSION

Abstract

Background Inadequate intake of micronutrients with antioxidant properties is common among older adults and has been associated with higher risk of frailty, adverse functional outcome, and impaired muscle health. However, a causal relationship is less well known. The aim was to determine in old mice the impact of reduced dietary intake of vitamins A/E/B6/B12/folate, selenium, and zinc on muscle mass, oxidative capacity, strength, and physical activity (PA) over time.Methods Twenty-one-month-old male mice were fed either AIN-93-M (control) or a diet low in micronutrients with antioxidant properties (= LOWOX-B: 50% of mouse recommended daily intake of vitamins A, E, B6, and B12, folate, selenium, and zinc) for 4 months. Muscle mass, grip strength, physical activity (PA), and general oxidative status were assessed. Moreover, muscle fatigue was measured of m. extensor digitorum longus (EDL) during an ex vivo moderate exercise protocol. Effects on oxidative capacity [succinate dehydrogenase (SDH) activity], muscle fibre type, number, and fibre cross-sectional area (fCSA) were assessed on m. plantaris (PL) using histochemistry.Results After 2 months on the diet, bodyweight of LOWOX-B mice was lower compared with control (P Conclusions Reduced dietary intake of vitamins A, E, B6, and B12, folate, selenium, and zinc resulted in a lower oxidative capacity and has major impact on muscle health as shown by decreased force production and PA, without effects on muscle mass. The reduced fCSA in combination with similar SDH activity per fibre might explain the reduced oxidative capacity resulting in the increased fatigue after exercise in LOWOX-B mice.

Published

2018

33. Muscle Phenotypic Variability in Limb Girdle Muscular Dystrophy 2 G.

Author

Paim, Julia, Cotta, Ana, Vargas, Antonio, Navarro, Monica, Valicek, Jaquelin, Carvalho, Elmano, da-Cunha-Junior, Antonio, Plentz, Estevão, Braz, Shelida, Takata, Reinaldo, Almeida, Camila, and Vainzof, Mariz

Abstract

Limb girdle muscular dystrophy type 2 G (LGMD2G) is caused by mutations in the telethonin gene. Only few families were described presenting this disease, and they are mainly Brazilians. Here, we identified one additional case carrying the same common c.157C > T mutation in the telethonin gene but with an atypical histopathological muscle pattern. In a female patient with a long duration of symptoms (46 years), muscle biopsy showed, in addition to telethonin deficiency, the presence of nemaline rods, type 1 fiber predominance, nuclear internalization, lobulated fibers, and mitochondrial paracrystalline inclusions. Her first clinical signs were identified at 8 years old, which include tiptoe walking, left lower limb deformity, and frequent falls. Ambulation loss occurred at 41 years old, and now, at 54 years old, she presented pelvic girdle atrophy, winging scapula, foot deformity with incapacity to perform ankle dorsiflexion, and absent tendon reflexes. The presence of nemaline bodies could be a secondary phenomenon, possibly associated with focal Z-line abnormalities of a long-standing disease. However, these new histopathological findings, characteristic of congenital myopathies, expand muscle phenotypic variability of telethoninopathy. [ABSTRACT FROM AUTHOR]

Published

2013

34. A ZASP missense mutation, S196L, leads to cytoskeletal and electrical abnormalities in a mouse model of cardiomyopathy.

Author

Zhaohui Li, Ai, Tomohiko, Samani, Kaveh, Yutao Xi, Huei-Ping Tzeng, Mingxing Xie, Shah Wu, Shuping Ge, Taylor, Michael D., Jian-Wen Dong, Jie Cheng, Ackerman, Michael J., Kimura, Akinori, Sinagra, Gianfranco, Brunelli, Luca, Faulkner, Georgine, Vatta, Matteo, Li, Zhaohui, Xi, Yutao, and Tzeng, Huei-Ping

Subjects

CYTOSKELETAL proteins, CYTOARCHITECTONICS, ELECTROPHYSIOLOGY, HEART cells, GENETIC mutation, CELL metabolism, ANIMAL experimentation, BIOLOGICAL models, CARRIER proteins, CELLS, COMPARATIVE studies, CYTOPLASM, DNA, ELECTRON microscopy, GENES, HEART conduction system, HEART function tests, IMMUNOHISTOCHEMISTRY, MAGNETIC resonance imaging, RESEARCH methodology, MEDICAL cooperation, MICE, MUSCLE proteins, POLYMERASE chain reaction, PROTEINS, RESEARCH, RESEARCH funding, EVALUATION research, DILATED cardiomyopathy

Abstract

Background: Dilated cardiomyopathy (DCM) is a primary disease of the heart muscle associated with sudden cardiac death secondary to ventricular tachyarrhythmias and asystole. However, the molecular pathways linking DCM to arrhythmias and sudden cardiac death are unknown. We previously identified a S196L mutation in exon 4 of LBD3-encoded ZASP in a family with DCM and sudden cardiac death. These findings led us to hypothesize that this mutation may precipitate both cytoskeletal and conduction abnormalities in vivo. Therefore, we investigated the role of the ZASP4 mutation S196L in cardiac cytoarchitecture and ion channel biology.Methods and Results: We generated and analyzed transgenic mice with cardiac-restricted expression of the S196L mutation. We also performed cellular electrophysiological analysis on isolated S196L cardiomyocytes and protein-protein interaction studies. Ten month-old S196L mice developed hemodynamic dysfunction consistent with DCM, whereas 3-month-old S196L mice presented with cardiac conduction defects and atrioventricular block. Electrophysiological analysis on isolated S196L cardiomyocytes demonstrated that the L-type Ca(2+) currents and Na(+) currents were altered. The pull-down assay demonstrated that ZASP4 complexes with both calcium (Ca(v)1.2) and sodium (Na(v)1.5) channels.Conclusions: Our findings provide new insight into the mechanisms by which mutations of a structural/cytoskeletal protein, such as ZASP, lead to cardiac functional and electric abnormalities. This work represents a novel framework to understand the development of conduction defects and arrhythmias in subjects with cardiomyopathies, including DCM. [ABSTRACT FROM AUTHOR]

Published

2010

35. Limb–Girdle and Congenital Muscular Dystrophies: Current Diagnostics, Management, and Emerging Technologies.

Author

Tesi Rocha, Carolina and Hoffman, Eric

Abstract

The muscular dystrophies show muscle degeneration and regeneration (necrotizing myopathy) on muscle biopsy, typically associated with elevated serum creatine kinase, and muscle weakness. In 1986, the first causative gene was identified for the most prevalent and best-characterized form of muscular dystrophy, Duchenne muscular dystrophy. Over the past 25 years, the number of other genes determined to cause different subtypes has grown rapidly. This review gives a synopsis of the 45 genetically defined types of muscular dystrophies and describes the clinical, pathologic, and molecular aspects of each disease. DNA diagnosis remains the most sensitive and specific method for differential diagnosis, but molecular diagnostics can be expensive and complex (because of multiple genes at multiple testing facilities) and reimbursement may be challenging to obtain. However, emerging DNA sequencing technologies (eg, single-molecule third-generation sequencing units) promise to dramatically reduce the complexity and costs of DNA diagnostics. Treatment for nearly all forms remains supportive and is aimed at preventing complications. However, several promising approaches have entered clinical trials, providing tangible hope that quality of life will improve for many patients in the near future. [ABSTRACT FROM AUTHOR]

Published

2010

36. Telethonin

Author

Rédei, George P.

Published

2008

37. Maintenance of muscle mass, fiber size, and contractile function in mice lacking the Z-disc protein myotilin.

Author

Ochala, Julien, Carpén, Olli, and Larsson, Lars

Abstract

Background. Myofibrillar myopathies constitute a rare group of congenital neuromuscular disorders, frequently associated with mutations in Z-disc proteins such as myotilin. Myotilin location and interactions with other Z-disc proteins are clearly defined, but its role in the regulation of muscle structure and function remains unknown. The present study aims at investigating this specific role of myotilin. Methods. Skeletal and cardiac muscles were collected from adult mice with a targeted deletion of myotilin (myo-/-) and wildtype animals (myo+/+). Results and conclusion. Similar skeletal and cardiac muscle weights were observed in myo-/- and myo+/+ mice. At the muscle cell level, the size and force production of single membrane permeabilized fibers were identical between myo-/- and myo+/+ rodents. Thus, myotilin does not have a significant influence on muscle mass, muscle fiber size, or regulation of muscle contraction. Alternatively, compensatory over-expressions of other elements including proteins from the same subfamily, or Z-disc proteins such as telethonin, or intermediate filaments may compensate for the lack of myotilin. [ABSTRACT FROM AUTHOR]

Published

2009

38. Structure and dynamics of the human muscle LIM protein

Author

Schallus, Thomas, Fehér, Krisztina, Ulrich, Anne S., Stier, Gunter, and Muhle-Goll, Claudia

Subjects

*PROTEIN structure, *MOLECULAR dynamics, *PROTEIN-protein interactions, *MYOGENESIS, *OVERHAUSER effect (Nuclear physics), *NUCLEAR magnetic resonance spectroscopy

Abstract

Abstract: The family of cysteine rich proteins (CRP) comprises three closely homologous members that have been reported to interact with α-actinin. Muscular LIM protein (MLP/CRP3), the skeletal muscle variant, was originally discovered as a positive regulator of myogenesis and is suggested to be part of the stretch sensor of the myofibril through its interaction with telethonin (T-Cap). We determined the structure of both LIM domains of human MLP by nuclear magnetic resonance spectroscopy. We confirm by 15N relaxation measurements that both LIM domains act as independent units and that the adjacent linker regions are fully flexible. With the published structures of CRP1 and CRP2, the complete family has now been structurally characterized. [Copyright &y& Elsevier]

Published

2009

39. Transcription-terminating mutation in telethonin causing autosomal recessive muscular dystrophy type 2G in a European patient

Author

Olivé, Montse, Shatunov, Alexey, Gonzalez, Laura, Carmona, Olga, Moreno, Dolores, Quereda, Lidia Gonzalez, Martinez-Matos, J.A., Goldfarb, Lev G., and Ferrer, Isidro

Subjects

*MUSCULAR dystrophy, *GENETIC transcription, *GENETIC mutation, *DISEASES in women, *HYPERTROPHY, *IMMUNOFLUORESCENCE, *PATIENTS, MUSCULAR dystrophy genetics

Abstract

Abstract: A 27-year-old woman of Moldavian origin presented at the age of 15 with progressive proximal limb weakness and painful cramps in her calf muscles. Clinical examination revealed prominent muscle weakness in proximal muscles of the lower extremities and distal anterior compartment of legs, and mild weakness in shoulder girdle muscles. In addition, she had marked calf hypertrophy, muscle atrophy involving the anterior and posterior compartments of the thighs, and the distal anterior compartment of legs, as well as mild scapular winging and hyperlordosis. A muscle biopsy taken from the biceps brachii showed mild dystrophic changes, absent vacuoles, and abundant lobulated fibers. Immunofluorescence and Western blot assays demonstrated complete telethonin deficiency. Molecular analysis revealed a homozygous Trp25X mutation in the telethonin (TCAP) gene resulting in termination of transcription at an early point. Four families from Brazil with telethonin deficiency have previously been reported and classified as LGMD2G, but the actual frequency of this disease is unknown. With this current identification of a case outside the Brazilian population, telethonin mutation-associated LGMD should be considered worldwide. [Copyright &y& Elsevier]

Published

2008

40. Coordinate expression of the 19S regulatory complex and evidence for ubiquitin-dependent telethonin degradation in the unloaded soleus muscle

Author

Heng, A.E., Ventadour, S., Jarzaguet, M., Pouch-Pélissier, M.N., Guezennec, C.Y., Bigard, X., Attaix, D., and Taillandier, D.

Subjects

*UBIQUITIN, *MESSENGER RNA, *MUSCULOSKELETAL system, *CARRIER proteins

Abstract

Abstract: Catabolic stimuli induce a coordinate expression of the 20S proteasome subunits in skeletal muscles. However, contradictory data have been obtained for the 19S regulatory complex (RC) subunits, which could reflect differential regulation at the transcriptional and/or translational level. To address this point we used a well-established model of muscle atrophy (hindlimb suspension) and determined the mRNA levels for 19S subunits belonging to both the base (non-ATPase S1, ATPases S7 and S8) and the lid (S14) of the 19S RC. Concomitant increased mRNA levels were observed for all studied subunits in rat soleus muscles after 9 days of unloading. In addition, analysis of polysome profiles showed a similar proportion of actively translated mRNA (50%) in unloaded and control soleus muscle. Furthermore, the repressed pool of messenger ribonucleoparticles (mRNPs) was low in both control (14%) and unloaded (15%) animals. Our data show that representative 19S subunits (S7 and S8) were efficiently translated, suggesting a coordinate production of 19S RC subunits. The 19S RC is responsible for the binding of polyubiquitin conjugates that are subsequently degraded inside the 20S proteasome core particle. We observed that soleus muscle atrophy was accompanied by an accumulation of ubiquitin conjugates. Purification of ubiquitin conjugates using the S5a 19S subunit followed by deubiquitination identified telethonin as a 26S proteasome substrate. In conclusion, muscle atrophy induces a concomitant expression of 26S proteasome subunits. Substrates to be degraded include a protein required for maintaining the structural integrity of sarcomeres. [Copyright &y& Elsevier]

Published

2008

41. TCAP knockdown by RNA interference inhibits myoblast differentiation in cultured skeletal muscle cells

Author

Markert, Chad D., Ning, Jie, Staley, Jerry T., Heinzke, Laura, Childers, Charles K., Ferreira, J. Andries, Brown, Marybeth, Stoker, Aaron, Okamura, Carol, and Childers, Martin K.

Subjects

*DYSTROPHY, *NEUROMUSCULAR diseases, *MUSCLE diseases, *NEUROLOGICAL disorders, *NEUROMUSCULAR system

Abstract

Abstract: Null mutation of titin-cap (TCAP) causes limb-girdle muscular dystrophy type 2G (LGMD2G). LGMD2G patients develop muscle atrophy, and lose the ability to walk by their third decade. Previous findings suggest that TCAP regulates myostatin, a key regulator of muscle growth. We tested the hypothesis that TCAP knockdown with RNA interference will lead to differential expression of genes involved in muscle proliferation and differentiation, impairing muscle cell growth. mRNA from cultured cells treated with TCAP siRNA duplex constructs was analyzed using Northern blots and real-time RT-PCR. siRNA treatment decreased TCAP mRNA expression in differentiating muscle cells. Significant (p <0.05) decreases in mRNA were observed for myogenic regulatory factors. siRNA treatment also prevented development of the normal phenotype of muscle cells. Our findings suggest that TCAP knockdown with RNA interference alters normal muscle cell differentiation. [Copyright &y& Elsevier]

Published

2008

42. Tracking changes in Z-band organization during myofibrillogenesis with FRET imaging.

Author

Stout, Andrea L., Wang, Jushuo, Sanger, Jean M., and Sanger, Joseph W.

Abstract

There are a large number of proteins associated with Z-bands in myofibrils, but the precise arrangements of most of these proteins in Z-bands are largely unknown. Even less is known about how these arrangements change during myofibrillogenesis. We have begun to address this issue using Sensitized Emission Fluorescence Resonance Energy Transfer (SE-FRET) microscopy. Cultured skeletal muscle cells from quail embryos were transfected to express fusions of alpha-actinin, FATZ, myotilin, or telethonin with cyan and yellow fluorescent proteins in various pair wise combinations. FATZ and myotilin were selected because previous biochemical studies have suggested that they bind to alpha-actinin, the major protein of the Z-band. Telethonin was selected for its reported ability to bind FATZ. Statistical analysis of data from FRET imaging studies yield results that are in agreement with published biochemical data suggesting that FATZ and myotilin bind to alpha-actinin near its C-terminus as well as to each other and that a region near the amino-terminus of FATZ is responsible for its interaction with telethonin. In addition, our analysis has revealed changes in the arrangement of alpha-actinin and FATZ that take place during the transition as the z-bodies of premyofibrils fuse to form the Z-bands of mature myofibrils. There was no evidence for a change in the arrangement of myotilin as z-bodies transformed into Z-bands. Myotilin is one Z-band protein that does not exhibit decreased dynamics as z-bodies fuse to form Z-bands. These FRET results from living cells support a stepwise model for the assembly of myofibrils. Cell Motil. Cytoskeleton 2008. © 2008 Wiley-Liss, Inc. [ABSTRACT FROM AUTHOR]

Published

2008

43. A muscle-specific MuRF1-E2 network requires stabilization of MuRF1-E2 complexes by telethonin, a newly identified substrate

Author

Stéphanie Cabantous, Didier Attaix, Daniel Taillandier, Lydie Combaret, Agnès Claustre, Catherine Bouchenot, Antoine Hauvette, Cécile Polge, Daniel Béchet, Julien Aniort, and Christiane Deval

Subjects

0301 basic medicine, chemistry.chemical_classification, biology, business.industry, HEK 293 cells, Skeletal muscle, Ubiquitin-conjugating enzyme, Telethonin, Ubiquitin ligase, Cell biology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Enzyme, medicine.anatomical_structure, chemistry, Ubiquitin, 030220 oncology & carcinogenesis, Physiology (medical), Myosin, biology.protein, Medicine, Orthopedics and Sports Medicine, business

Abstract

Muscle wasting is observed in the course of many diseases and also during physiological conditions (disuse, aging). Skeletal muscle mass is largely controlled by the ubiquitin-proteasome system and thus by the ubiquitinating enzymes (E2s and E3s) that target substrates for subsequent degradation. MuRF1 is the only E3 ubiquitin ligase known to target contractile proteins (α-actin, myosins) during catabolic situations. MuRF1 is therefore a putative target for preventing muscle wasting. However, MuRF1 depends on E2 ubiquitin conjugating enzymes for ubiquitin chain formation on the substrates. We focused on 14 E2 enzymes that are either expressed in skeletal muscle or up-regulated during atrophying conditions. In this work, we demonstrated that only highly sensitive and complementary interactomic approaches (Surface Plasmon Resonance, Yeast three-Hybrid and split-GFP) allowed the identification of MuRF1 E2 partners. Five E2 enzymes physically interacted with MuRF1, namely E2E1, E2G1, E2J1, E2J2 and E2L3. Moreover, we demonstrated that MuRF1-E2E1 and MuRF1-E2J1 interactions are facilitated by telethonin, a newly identified MuRF1 substrate. We next showed that the 5 identified E2s functionally interacted with MuRF1 since, in contrast to the non-interacting E2D2, their co-expression in HEK293T cells with MuRF1 led to increased telethonin degradation. Finally, we showed that telethonin governed the affinity between MuRF1 and E2E1 or E2J1.We report here the first MuRF1-E2s network, which may prove valuable for deciphering the precise mechanisms involved in the atrophying muscle program and for proposing new therapeutical approaches.

Published

2017

44. TELETHONIN AS AN EARLY IMMUNOHISTOCHEMICAL MARKER IN LIGATION-INDUCED ISCHEMIC MYOCARDIAL INJURY

Author

Pong-Jeu Lu, Tzu-Cheng Hsu, He-Shiuan Liang, and Fun-In Wang

Subjects

0301 basic medicine, medicine.medical_specialty, Necrosis, business.industry, 030204 cardiovascular system & hematology, Telethonin, Anterior Descending Coronary Artery, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Internal medicine, Cardiology, medicine, Immunohistochemistry, Circumflex, medicine.symptom, Ligation, business

Abstract

In this study, acute myocardial injuries or necrosis were experimentally induced in calves and pigs by ligation of either the left anterior descending coronary artery or left circumflex branch for 30[Formula: see text]min without reperfusion. Various antibodies directed to structural and functional proteins of the sarcomere, as well as activated proteinases, were employed in immunohistochemistry to compare for their potentials to detect early myocardial injury. For comparison, the histological criteria (designated as “Method A”) of cardiomyocyte necrosis such as nuclear pyknosis, sarcoplasmic fragmentation, flocculation, and/or the presence of a contraction band, and inflammatory infiltration were also scored. Additional criteria (designated “Method B”) of changes in late reversible stage of cell injury such as irregular nuclear shape or hyperchromasia, sarcomplasmic hypereosinophilia with either swelling or atrophy in diameter, and perinuclear vacuolation likely of swollen organelles, were also scored. In this setting, telethonin (T-cap), cardiac troponin I (cTnI), the current gold standard, and Method B, were superior to others in detecting ligation-induced ischemic injury. Other markers were either less specific, or less sensitive, or inconclusive for the current application. In conclusion, telethonin may serve as an early immunohistochemical marker in ligation-induced ischemic myocardial injury due to a combination of biomechanical stress, hypoxia, and possibly additional factor as matrix metalloproteinase activation.

Published

2017

45. Evidence for a dimeric assembly of two titin/telethonin complexes induced by the telethonin C-terminus

Author

Pinotsis, Nikos, Petoukhov, Maxim, Lange, Stephan, Svergun, Dmitri, Zou, Peijian, Gautel, Mathias, and Wilmanns, Matthias

Subjects

*MUSCLE proteins, *PROTEIN-protein interactions, *X-ray scattering, *DICHROISM

Abstract

Abstract: The Z-disk region defines the lateral boundary of the sarcomere and requires a high level of mechanical strength to provide a stable framework for large filamentous muscle proteins. The level of complexity at this area is reflected by a large number of protein–protein interactions. Recently, we unraveled how the N-terminus of the longest filament component, the giant muscle protein titin, is assembled into an antiparallel (2:1) sandwich complex by the N-terminal titin-binding segment of the Z-disk ligand telethonin/T-cap [Zou, P., Pinotsis, N., Lange, S., Song, Y.H., Popov, A., Mavridis, I., Mayans, O.M., Gautel, M., Wilmanns, M., 2006. Palindromic assembly of the giant muscle protein titin in the sarcomeric Z-disk. Nature 439, 229–233]. In this contribution, we present structural data of a related complex of the titin N-terminus with full-length telethonin. The C-terminus of telethonin remains invisible, suggesting that it does not fold into a defined structure even in the presence of titin. In contrast to the structure with truncated telethonin, a dimer of two titin/telethonin complexes is formed within the crystal environment, potentially indicating the formation of higher oligomers. We further investigated the structure and dynamics of this assembly by small-angle X-ray scattering, circular dichroism, and in vivo complementation data. The data consistently indicate the involvement of the C-terminal part of telethonin into the assembly of two titin/telethonin complexes. [Copyright &y& Elsevier]

Published

2006

46. Genotype–phenotype relationships involving hypertrophic cardiomyopathy-associated mutations in titin, muscle LIM protein, and telethonin

Author

Bos, J. Martijn, Poley, Rainer N., Ny, Melissa, Tester, David J., Xu, Xiaolei, Vatta, Matteo, Towbin, Jeffrey A., Gersh, Bernard J., Ommen, Steve R., and Ackerman, Michael J.

Subjects

*CARDIOMYOPATHIES, *HYPERTROPHIC cardiomyopathy, *NUCLEIC acids, *CYTOPLASMIC filaments

Abstract

Abstract: Background: TTN-encoded titin, CSRP3-encoded muscle LIM protein, and TCAP-encoded telethonin are Z-disc proteins essential for the structural organization of the cardiac sarcomere and the cardiomyocyte’s stretch sensor. All three genes have been established as cardiomyopathy-associated genes for both dilated cardiomyopathy (DCM) and hypertrophic cardiomyopathy (HCM). Here, we sought to characterize the frequency, spectrum, and phenotype associated with HCM-associated mutations in these three genes in a large cohort of unrelated patients evaluated at a single tertiary outpatient center. Methods: DNA was obtained from 389 patients with HCM (215 male, left ventricular wall thickness of 21.6±6mm) and analyzed for mutations involving all translated exons of CSRP3 and TCAP and targeted HCM-associated exons (2, 3, 4, and 14) of TTN using polymerase chain reaction (PCR), denaturing high performance liquid chromatography (DHPLC), and direct DNA sequencing. Clinical data were extracted from patient records and maintained independent of the genotype. Results: Overall, 16 patients (4.1%) harbored a Z-disc mutation: 12 had a MLP mutation and 4 patients a TCAP mutation. No TTN mutations were detected. Seven patients were also found to have a concomitant myofilament mutation. Seven patients with a MLP-mutation were found to harbor the DCM-associated, functionally characterized W4R mutation. W4R-MLP was also noted in a single white control subject. Patients with MLP/TCAP-associated HCM clinically mimicked myofilament-HCM. Conclusions: Approximately 4.1% of unrelated patients had HCM-associated MLP or TCAP mutations. MLP/TCAP-HCM phenotypically mirrors myofilament-HCM and is more severe than the subset of patients who still remain without a disease-causing mutation. The precise role of W4R-MLP in the pathogenesis of either DCM or HCM warrants further investigation. [Copyright &y& Elsevier]

Published

2006

47. Telethonin protein expression in neuromuscular disorders

Author

Vainzof, Mariz, Moreira, Eloisa S., Suzuki, Oscar T., Faulkner, Georgine, Valle, Georgio, Beggs, Alan H., Carpen, Olli, Ribeiro, Alberto F., Zanoteli, Edmar, Gurgel-Gianneti, Juliana, Tsanaclis, Ana Maria, Silva, Helga C.A., Passos-Bueno, Maria Rita, and Zatz, Mayana

Subjects

*NEUROMUSCULAR diseases, *PROTEINS, *IMMUNOFLUORESCENCE

Abstract

Telethonin is a 19-kDa sarcomeric protein, localized to the Z-disc of skeletal and cardiac muscles. Mutations in the telethonin gene cause limb–girdle muscular dystrophy type 2G (LGMD2G).We investigated the sarcomeric integrity of muscle fibers in LGMD2G patients, through double immunofluorescence analysis for telethonin with three sarcomeric proteins: titin, α-actinin-2, and myotilin and observed the typical cross striation pattern, suggesting that the Z-line of the sarcomere is apparently preserved, despite the absence of telethonin. Ultrastructural analysis confirmed the integrity of the sarcomeric architecture. The possible interaction of telethonin with other proteins responsible for several forms of neuromuscular disorders was also analyzed. Telethonin was clearly present in the rods in nemaline myopathy (NM) muscle fibers, confirming its localization to the Z-line of the sarcomere. Muscle from patients with absent telethonin showed normal expression for the proteins dystrophin, sarcoglycans, dysferlin, and calpain-3. Additionally, telethonin showed normal localization in muscle biopsies from patients with LGMD2A, LGMD2B, sarcoglycanopathies, and Duchenne muscular dystrophy (DMD). Therefore, the primary deficiency of calpain-3, dysferlin, sarcoglycans, and dystrophin do not seem to alter telethonin expression. [Copyright &y& Elsevier]

Published

2002

48. Novel mutation in TCAP manifesting with asymmetric calves and early-onset joint retractions

Author

Ana Fernández-Marmiesse, Carlos Pablo de Fuenmayor-Fernández de la Hoz, Montse Olivé, Cristina Domínguez-González, and Aurelio Hernández-Laín

Subjects

Adult, Male, 0301 basic medicine, medicine.medical_specialty, Weakness, Nonsense mutation, Mutation, Missense, Telethonin, Diagnosis, Differential, 03 medical and health sciences, 0302 clinical medicine, Tibialis anterior muscle, medicine, Humans, Connectin, Muscular dystrophy, Muscle, Skeletal, Genetics (clinical), Muscle contracture, Leg, Muscle biopsy, medicine.diagnostic_test, business.industry, Homozygote, Anatomy, medicine.disease, Surgery, Phenotype, 030104 developmental biology, Muscular Dystrophies, Limb-Girdle, Neurology, Pediatrics, Perinatology and Child Health, Neurology (clinical), medicine.symptom, Differential diagnosis, business, 030217 neurology & neurosurgery

Abstract

A 29-year-old man, born from consanguineous parents, started with toe walking and frequent falls during his second year of life. He developed weakness in lower limbs during the first decade that subsequently extended to upper limbs. On examination, the patient had weakness in proximal muscles of all four limbs and in the tibialis anterior muscle. In addition, he had bilateral Achilles and patellar contractures, bilateral scapular winging, asymmetric calves and a positive Beevor sign, an upward movement of the umbilicus on contraction of rectus femoris due to weakness in the lower part. The muscle biopsy showed dystrophic changes and lobulated fibers. Genetic analysis through a next-generation sequencing panel of genes related to neuromuscular disorders revealed a novel homozygous nonsense mutation (p.Tyr85*) in the TCAP gene. Subsequent western blot assay showed a complete telethonin deficiency. Our observation expands the phenotypic spectrum of TCAP mutations and indicates that telethonin deficiency should be considered in the differential diagnosis of patients presenting with asymmetric calves and early joint retractions.

Published

2016

49. Myofibril Assembly in Cultured Mouse Neonatal Cardiomyocytes

Author

Jushuo Wang, Yingli Fan, Jean M. Sanger, Joseph W. Sanger, Jennifer White, and Dipak K. Dube

Subjects

0301 basic medicine, Myofibril assembly, animal structures, Histology, macromolecular substances, Telethonin, Sarcomere, 03 medical and health sciences, Mice, 0302 clinical medicine, Myofibrils, Myosin, medicine, Animals, Myocytes, Cardiac, Ecology, Evolution, Behavior and Systematics, Actin, Cells, Cultured, Myomesin, biology, Chemistry, Skeletal muscle, Cell Differentiation, musculoskeletal system, Actins, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Animals, Newborn, embryonic structures, biology.protein, Anatomy, Myofibril, tissues, 030217 neurology & neurosurgery, Biotechnology

Abstract

The formation of myofibrils was analyzed in neonatal mouse cardiomyocytes grown in culture and stained with fluorescent antibodies directed against myofibrillar proteins. The cardiomyocyte cultures also were exposed to siRNA probes to test the role of nonmuscle myosin IIB expression in the formation of myofibrils. In culture, new myofibrils formed in the spreading cell margins surrounding contractile myofibrils previously assembled in utero. Observations indicated that assembly of mature myofibrils occurred in three-stages, as previously reported in cultured mouse skeletal muscle. Premyofibrils, characterized by minisarcomeres with nonmuscle myosin IIB and muscle-specific alpha-actinin bound to actin filaments, formed in the first stage; followed by nascent myofibrils, the second stage when muscle myosin II and titin were first detected. In the mature myofibril stage muscle myosin II filaments aligned in periodic A-Bands; late assembling proteins, including myomesin and telethonin, were integrated in the sarcomeres, and nonmuscle IIB was absent from the sarcomeres. Treatment of the cultured neonatal cardiomyocytes with gene-specific siRNAs for nonmuscle myosin IIB, led to a marked decrease in the formation of premyofibrils, and subsequently of mature myofibrils. Anat Rec, 301:2067-2079, 2018. © 2018 Wiley Periodicals, Inc.

Published

2018

50. The role of the SCN5A-encoded channelopathy in irritable bowel syndrome and other gastrointestinal disorders

Author

Joanna W. Kruimel, Paul G.A. Volders, Ad A.M. Masclee, Tom E Verstraelen, R. M. A. ter Bekke, RS: NUTRIM - R2 - Gut-liver homeostasis, RS: CARIM - R2 - Cardiac function and failure, Cardiologie, and Interne Geneeskunde

Subjects

EXPRESSION, medicine.medical_specialty, INTERSTITIAL-CELLS, Physiology, Gastrointestinal Diseases, IONIC CONDUCTANCES, Population, Motility, LONG-QT SYNDROME, TELETHONIN, Gastroenterology, NAV1.5 Voltage-Gated Sodium Channel, symbols.namesake, Channelopathy, Internal medicine, voltage-gated sodium channel, medicine, Humans, genetics, cardiovascular diseases, education, MUTATION, Irritable bowel syndrome, SODIUM CURRENT, SCN5A, G alpha subunit, Brugada syndrome, irritable bowel syndrome, education.field_of_study, Endocrine and Autonomic Systems, business.industry, Sodium channel, medicine.disease, RANOLAZINE, GI motility, Interstitial cell of Cajal, cardiovascular system, symbols, HEART, Channelopathies, business

Abstract

Background Gastrointestinal functional and motility disorders, like irritable bowel syndrome (IBS), have a high prevalence in the Western population and cause significant morbidity and loss of quality of life leading to considerable costs for health care. A decade ago, it has been demonstrated that interstitial cells of Cajal and intestinal smooth muscle cells, cells important for gastrointestinal motility, express the sodium channel alpha subunit Nav1.5. In the heart, aberrant variants in this sodium channel, encoded by SCN5A, are linked to inherited arrhythmia syndromes, like the long-QT syndrome type 3 and Brugada syndrome. Mounting data show a possible contribution of SCN5A mutants to gastrointestinal functional and motility disorders. Two percent of IBS patients harbor SCN5A mutations with electrophysiological evidence of loss- and gain-of-function. In addition, gastrointestinal symptoms are more prevalent in cardiac SCN5A-mutation positive patients. Purpose This review firstly describes the Nav1.5 channel and its physiological role in ventricular cardiomyocytes and gastrointestinal cells, then we focus on the involvement of mutant Nav1.5 in gastrointestinal functional and motility disorders. Future research might uncover novel mutation-specific treatment strategies for SCN5A-encoded gastrointestinal channelopathies.

Published

2015