Abstract

Facioscapulohumeral muscular dystrophy (FSHD) is an autosomal dominant muscle disorder that is characterized by the progressive weakness and wasting of the muscles from face, upper-arm and shoulder girdle to lower limb. While there is consensus that FSHD is a disorder of transcription and gene regulation, the molecular pathways leading to muscular dystrophy and other unique clinical features of the disease are far from clear. Our preliminary study of whole genome profiles of 125 muscle biopsies representing 12 neuromuscular disorders showed that paired-like homeodomain transcription factor 1 (PITX1) gene was specifically up-regulated in FSHD patients. The significant PITX1 over-expression we observed in FSHD can not be due to inflammation, degeneration/ regeneration, or other """"""""dystrophic"""""""" changes in muscle, as no other muscle disease (including juvenile dermatomyositis, Duchenne dystrophy, and others) showed up- regulation. Based on our extensive preliminary data both in vitro and in vivo, we present a model where over-expression of PITX1 in adult muscle invokes key muscle atrophy pathways, and, further, that PITX1 is regulated by DUX4 expression. The goal of this current proposal is to further develop our pathophysiological model to show direct relationships between 4q35 deletions, DUX4, and PITX1. The proposed research relies heavily on temporal series, conducted both in vivo and in vitro. Gene/gene interactions will also be determined.
In aim 1, we propose to determine if Pitxl is a direct target of DUX4. We will determine whether a putative DUX4 binding site in the promoter region of Pitxl is functional, and whether it is specifically and directly regulated by DUX4. Additional DUX4 targets will be identified by temporal profiling. Interaction between DUX4 and potential target genes will be determined.
In aim 2, we propose to generate and characterize a conditional muscle-specific Pitxl transgenic mouse model. The phenotype will be evaluated for changes in various clinical, functional, biochemical, molecular, and histological parameters. The phenotype of myoblasts, including appearance, proliferation, differentiation and susceptibility to oxidative stress, will also be evaluated. In addition, we will determine whether the disease phenotype is reversible.
In aim 3, we will define molecular transcriptional pathways downstream of Pitxl expression using the Pitxl transgenic mouse. Temporal expression profiling will be performed to construct the pathways regulated by Pitxl. Interactions between Pitxl and potential regulatory targets of Pitxl will be further studied. Our preliminary data showed that disease-specific up-regulation of DUX4 and Pitxl and downstream changes of genes involved in muscle wasting might be involved in the pathophysiology of FSHD. The proposed research will identify key players in the pathological cascades of FSHD and define the interactions among them, which could potentially be used for developing treatments of the disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
Research Project (R01)
Project #
3R01AR052027-04S1
Application #
8073308
Study Section
Skeletal Muscle and Exercise Physiology Study Section (SMEP)
Program Officer
Nuckolls, Glen H
Project Start
2010-05-20
Project End
2010-09-30
Budget Start
2010-05-20
Budget End
2010-09-30
Support Year
4
Fiscal Year
2010
Total Cost
$70,520
Indirect Cost

  Institution

Name
Children's Research Institute
Department
Type
DUNS #
143983562
City
Washington
State
DC
Country
United States
Zip Code
20010

  Publications

Chen, Yi-Wen; Gregory, Chris; Ye, Fan et al. (2017) Molecular signatures of differential responses to exercise trainings during rehabilitation. Biomed Genet Genom 2:
Munters, Li Alemo; Loell, Ingela; Ossipova, Elena et al. (2016) Endurance Exercise Improves Molecular Pathways of Aerobic Metabolism in Patients With Myositis. Arthritis Rheumatol 68:1738-50
Sharma, Vishakha; Pandey, Sachchida Nand; Khawaja, Hunain et al. (2016) PARP1 Differentially Interacts with Promoter region of DUX4 Gene in FSHD Myoblasts. J Genet Syndr Gene Ther 7:
Baligand, Celine; Chen, Yi-Wen; Ye, Fan et al. (2015) Transcriptional Pathways Associated with Skeletal Muscle Changes after Spinal Cord Injury and Treadmill Locomotor Training. Biomed Res Int 2015:387090
Guadagnin, Eleonora; Narola, Jigna; Bönnemann, Carsten G et al. (2015) Tyrosine 705 Phosphorylation of STAT3 Is Associated with Phenotype Severity in TGF?1 Transgenic Mice. Biomed Res Int 2015:843743
Burniston, Jatin G; Kenyani, Jenna; Gray, Donna et al. (2014) Conditional independence mapping of DIGE data reveals PDIA3 protein species as key nodes associated with muscle aerobic capacity. J Proteomics 106:230-45
Pandey, Sachchida Nand; Lee, Yi-Chien; Yokota, Toshifumi et al. (2014) Morpholino treatment improves muscle function and pathology of Pitx1 transgenic mice. Mol Ther 22:390-396
Narola, Jigna; Pandey, Sachchida Nand; Glick, Adam et al. (2013) Conditional expression of TGF-?1 in skeletal muscles causes endomysial fibrosis and myofibers atrophy. PLoS One 8:e79356
Sharma, Vishakha; Harafuji, Naoe; Belayew, Alexandra et al. (2013) DUX4 differentially regulates transcriptomes of human rhabdomyosarcoma and mouse C2C12 cells. PLoS One 8:e64691
Burniston, Jatin G; Meek, Thomas H; Pandey, Sachchida Nand et al. (2013) Gene expression profiling of gastrocnemius of ""minimuscle"" mice. Physiol Genomics 45:228-36

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