Literature DB >> 24325401

Distinct regions of triadin are required for targeting and retention at the junctional domain of the sarcoplasmic reticulum.

Daniela Rossi, Cristina Bencini1, Marina Maritati1, Francesca Benini1, Stefania Lorenzini1, Enrico Pierantozzi1, Angela Maria Scarcella1, Cecilia Paolini, Feliciano Protasi, Vincenzo Sorrentino.   

Abstract

Ca2+ release, which is necessary for muscle contraction, occurs at the j-SR (junctional domain of the sarcoplasmic reticulum). It requires the assembly of a large multiprotein complex containing the RyR (ryanodine receptor) and additional proteins, including triadin and calsequestrin. The signals which drive these proteins to the j-SR and how they assemble to form this multiprotein complex are poorly understood. To address aspects of these questions we studied the localization, dynamic properties and molecular interactions of triadin. We identified three regions, named TR1 (targeting region 1), TR2 and TR3, that contribute to the localization of triadin at the j-SR. FRAP experiments showed that triadin is stably associated with the j-SR and that this association is mediated by TR3. Protein pull-down experiments indicated that TR3 contains binding sites for calsequestrin-1 and that triadin clustering can be enhanced by binding to calsequestrin-1. These findings were confirmed by FRET experiments. Interestingly, the stable association of triadin to the j-SR was significantly decreased in myotubes from calsequestrin-1 knockout mice. Taken together, these results identify three regions in triadin that mediate targeting to the j-SR and reveal a role for calsequestrin-1 in promoting the stable association of triadin to the multiprotein complex associated with RyR.

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Year:  2014        PMID: 24325401     DOI: 10.1042/BJ20130719

Source DB:  PubMed          Journal:  Biochem J        ISSN: 0264-6021            Impact factor:   3.857


  18 in total

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5.  Three residues in the luminal domain of triadin impact on Trisk 95 activation of skeletal muscle ryanodine receptors.

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Review 6.  Physiology and pathophysiology of excitation-contraction coupling: the functional role of ryanodine receptor.

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7.  Molecular determinants of homo- and heteromeric interactions of Junctophilin-1 at triads in adult skeletal muscle fibers.

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Review 10.  Calsequestrin, a key protein in striated muscle health and disease.

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