Nuclear pore complexes (NPCs) are multiprotein channels that penetrate the nuclear envelope and connect the nucleus with the cytoplasm. Besides controlling nucleocytoplasmic transport, NPCs are involved in chromatin organization and gene expression regulation. Changes in the composition of these structures have been recently linked to myoblast differentiation, suggesting a role for specialized NPCs in muscle physiology. In adults, muscle regeneration and repair requires the efficient function of satellite cells. Upon injury, these muscle stem cells are induced to proliferate, differentiate into myoblasts and fuse to regenerate muscle fibers. Because satellite cells are essential for muscle repair and regeneration, transplantation of these cells represents a promising therapy for the treatment of damaged muscle, muscular dystrophies and sarcopenia. Therefore, understanding the mechanisms of satellite cell function has become of great interest for regenerative medicine. Previous studies have found that the expression of the nuclear pore complex protein Nup210 is required for myoblast differentiation and survival, indicating an essential role for this protein i skeletal muscle differentiation and regeneration. Additionally, up-regulation of Nup210 levels in myoblasts has been shown to accelerate myogenesis, suggesting that modulation of its activity could be exploited to stimulate muscle regeneration. The overall objectives of this proposal are to establish the molecular mechanisms through which the nucleoporin Nup210 regulates myogenesis and to define its function in muscle formation and maintenance, with the ultimate goal of defining its potential as a therapeutic target for muscle regeneration. By combining in vivo and in vitro genetic approaches with muscle injury studies we expect to establish the role of Nup210 in muscle formation, growth and repair (Aim 1) and define the molecular mechanisms of myogenic regulation by Nup210 (Aim 2). In addition, we will determine if modulating the activity of this nuclear pore complex component can stimulate muscle regeneration and reverse the myogenic defects of dystrophic myoblasts. Defining the function of Nup210 in muscle physiology and understanding its molecular mechanisms of action are critical steps to determine whether this pathway could be used to develop therapies directed to stimulate muscle healing and prevent muscle degeneration. Our contribution here is expected to be a detailed understanding of the role of Nup210 in myogenesis, muscle development and muscle regeneration. These studies will significantly advance our knowledge of how changes in nuclear pore complex composition and function regulate these processes and could uncover new targets on which therapies to improve muscle function or prevent muscle degeneration can be developed.

Public Health Relevance

Muscle maintenance and regeneration requires the proper activation, proliferation and differentiation (myogenesis) of muscle stem cells known as satellite cells. A decrease in the number and myogenic activity of satellite cells contributes to the development of several muscle dystrophies and is associated with the gradual loss of skeletal muscle mass associated with aging (sarcopenia). Our objective is to establish the molecular mechanisms through which the nucleoporin Nup210 regulates myogenesis and define its function in muscle formation and maintenance, with the ultimate goal of uncovering its role in muscle regeneration. Our findings may enable the design of novel therapeutic strategies for the treatment of muscle injury and myopathies.

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
Research Project (R01)
Project #
5R01AR065083-05
Application #
9269458
Study Section
Nuclear and Cytoplasmic Structure/Function and Dynamics Study Section (NCSD)
Program Officer
Boyce, Amanda T
Project Start
2014-10-01
Project End
2019-04-30
Budget Start
2017-05-01
Budget End
2018-04-30
Support Year
5
Fiscal Year
2017
Total Cost
$386,100
Indirect Cost
$188,100
Name
Sanford Burnham Prebys Medical Discovery Institute
Department
Type
Research Institutes
DUNS #
020520466
City
La Jolla
State
CA
Country
United States
Zip Code
92037
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Borlido, Joana; D'Angelo, Maximiliano A (2018) Nup62-mediated nuclear import of p63 in squamous cell carcinoma. EMBO Rep 19:3-4
Borlido, Joana; Sakuma, Stephen; Raices, Marcela et al. (2018) Nuclear pore complex-mediated modulation of TCR signaling is required for naïve CD4+ T cell homeostasis. Nat Immunol 19:594-605
Raices, Marcela; D'Angelo, Maximiliano A (2017) Nuclear pore complexes and regulation of gene expression. Curr Opin Cell Biol 46:26-32
Raices, Marcela; Bukata, Lucas; Sakuma, Stephen et al. (2017) Nuclear Pores Regulate Muscle Development and Maintenance by Assembling a Localized Mef2C Complex. Dev Cell 41:540-554.e7
Sakuma, Stephen; D'Angelo, Maximiliano A (2017) The roles of the nuclear pore complex in cellular dysfunction, aging and disease. Semin Cell Dev Biol 68:72-84
Wong, Richard W; D'Angelo, Maximiliano (2016) Linking Nucleoporins, Mitosis, and Colon Cancer. Cell Chem Biol 23:537-539