Literature DB >> 24668811

Z-disc-associated, alternatively spliced, PDZ motif-containing protein (ZASP) mutations in the actin-binding domain cause disruption of skeletal muscle actin filaments in myofibrillar myopathy.

Xiaoyan Lin1, Janelle Ruiz, Ilda Bajraktari, Rachel Ohman, Soojay Banerjee, Katherine Gribble, Joshua D Kaufman, Paul T Wingfield, Robert C Griggs, Kenneth H Fischbeck, Ami Mankodi.   

Abstract

The core of skeletal muscle Z-discs consists of actin filaments from adjacent sarcomeres that are cross-linked by α-actinin homodimers. Z-disc-associated, alternatively spliced, PDZ motif-containing protein (ZASP)/Cypher interacts with α-actinin, myotilin, and other Z-disc proteins via the PDZ domain. However, these interactions are not sufficient to maintain the Z-disc structure. We show that ZASP directly interacts with skeletal actin filaments. The actin-binding domain is between the modular PDZ and LIM domains. This ZASP region is alternatively spliced so that each isoform has unique actin-binding domains. All ZASP isoforms contain the exon 6-encoded ZASP-like motif that is mutated in zaspopathy, a myofibrillar myopathy (MFM), whereas the exon 8-11 junction-encoded peptide is exclusive to the postnatal long ZASP isoform (ZASP-LΔex10). MFM is characterized by disruption of skeletal muscle Z-discs and accumulation of myofibrillar degradation products. Wild-type and mutant ZASP interact with α-actin, α-actinin, and myotilin. Expression of mutant, but not wild-type, ZASP leads to Z-disc disruption and F-actin accumulation in mouse skeletal muscle, as in MFM. Mutations in the actin-binding domain of ZASP-LΔex10, but not other isoforms, cause disruption of the actin cytoskeleton in muscle cells. These isoform-specific mutation effects highlight the essential role of the ZASP-LΔex10 isoform in F-actin organization. Our results show that MFM-associated ZASP mutations in the actin-binding domain have deleterious effects on the core structure of the Z-discs in skeletal muscle.

Entities:  

Keywords:  Actin; Actinin; Muscular Dystrophy; Myofibrillar Myopathy; Myotilin; Protein Complex; Protein-Protein Interaction; Skeletal Muscle; Z-disc; ZASP

Mesh:

Substances:

Year:  2014        PMID: 24668811      PMCID: PMC4036366          DOI: 10.1074/jbc.M114.550418

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  41 in total

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Journal:  Mol Biol Cell       Date:  2016-06-15       Impact factor: 4.138

6.  Evaluation of the Genetic Basis of Familial Aggregation of Pacemaker Implantation by a Large Next Generation Sequencing Panel.

Authors:  Patrícia B S Celestino-Soper; Anisiia Doytchinova; Hillel A Steiner; Andrea Uradu; Ty C Lynnes; William J Groh; John M Miller; Hai Lin; Hongyu Gao; Zhiping Wang; Yunlong Liu; Peng-Sheng Chen; Matteo Vatta
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7.  Zasp52, a Core Z-disc Protein in Drosophila Indirect Flight Muscles, Interacts with α-Actinin via an Extended PDZ Domain.

Authors:  Kuo An Liao; Nicanor González-Morales; Frieder Schöck
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8.  Coexistence of congenital left ventricular aneurysm and prominent left ventricular trabeculation in a patient with LDB3 mutation: a case report.

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9.  Characterizing the actin-binding ability of Zasp52 and its contribution to myofibril assembly.

Authors:  Kuo An Liao; Nicanor González-Morales; Frieder Schöck
Journal:  PLoS One       Date:  2020-07-02       Impact factor: 3.240

10.  Proteomic profiling of skeletal and cardiac muscle in cancer cachexia: alterations in sarcomeric and mitochondrial protein expression.

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Journal:  Oncotarget       Date:  2018-04-24
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