Clathrin Adaptor GGA1 Modulates Myogenesis of C2C12 Myoblasts

Overview

Journal PLoS One

Specialties General Medicine
Science

Date 2018 Nov 16

PMID 30440034

Citations 5

Authors

Mari Isobe

Sachiko Lee

Satoshi Waguri

Satoshi Kametaka

Affiliations

Soon will be listed here.

Abstract

During myogenesis, myogenic stem cells undergo several sequential events, including cell division, migration, and cell-cell fusion, leading to the formation of multinuclear myotubes, which are the precursors of myofibers. To understand the molecular mechanisms underlying these complex processes, an RNA interference-based gene depletion approach was used. Golgi associated, gamma adaptin ear containing, ARF binding protein 1 (GGA1), a Golgi-resident monomeric clathrin adaptor, was found to be required for the process of myotube formation in C2C12 cells, a cultured murine myoblast cell line. Gga1 mRNA expression was upregulated during myogenesis, and Gga1 depletion prevented the formation of large multi-nucleated myotubes. Moreover, inhibition of lysosomal proteases in Gga1 knockdown myoblasts increased the amount of insulin receptor, suggesting that GGA1 is involved in the cell surface expression and sorting of the insulin receptor. These results suggested that GGA1 plays a significant role in the formation and maturation of myotubes by targeting the insulin receptor to the cell surface to establish functionally mature myofibers.

Citing Articles

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The ESCRT-0 subcomplex component Hrs/Hgs is a master regulator of myogenesis via modulation of signaling and degradation pathways.

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Activation of IGF-1 pathway and suppression of atrophy related genes are involved in Epimedium extract (icariin) promoted C2C12 myotube hypertrophy.

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Inactivation of the three GGA genes in HeLa cells partially compromises lysosomal enzyme sorting.

Doray B, Liu L, Lee W, Jennings B, Kornfeld S FEBS Open Bio. 2020; 11(2):367-374.

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Correction: Clathrin adaptor GGA1 modulates myogenesis of C2C12 myoblasts.

Isobe M, Lee S, Waguri S, Kametaka S PLoS One. 2018; 13(12):e0209441.

PMID: 30543706 PMC: 6292604. DOI: 10.1371/journal.pone.0209441.

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