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Development of rabbit monoclonal antibodies for detection of alpha-dystroglycan in normal and dystrophic tissue

  • Marisa J. Fortunato
  • , Charlotte E. Ball
  • , Katrin Hollinger
  • , Niraj B. Patel
  • , Jill N. Modi
  • , Vedika Rajasekaran
  • , Dan J. Nonneman
  • , Jason W. Ross
  • , Eileen J. Kennedy
  • , Joshua T. Selsby
  • , Aaron M. Beedle

Research output: Contribution to journalArticlepeer-review

13 Scopus citations

Abstract

Alpha-dystroglycan requires a rare O-mannose glycan modification to form its binding epitope for extracellular matrix proteins such as laminin. This functional glycan is disrupted in a cohort of muscular dystrophies, the secondary dystroglycanopathies, and is abnormal in some metastatic cancers. The most commonly used reagent for detection of alpha-dystroglycan is mouse monoclonal antibody IIH6, but it requires the functional O-mannose structure for recognition. Therefore, the ability to detect alpha-dystroglycan protein in disease states where it lacks the full O-mannose glycan has been limited. To overcome this hurdle, rabbit monoclonal antibodies against the alpha-dystroglycan C-terminus were generated. The new antibodies, named 5-2, 29-5, and 45-3, detect alpha-dystroglycan from mouse, rat and pig skeletal muscle by Western blot and immunofluorescence. In a mouse model of fukutin-deficient dystroglycanopathy, all antibodies detected low molecular weight alpha-dystroglycan in disease samples demonstrating a loss of functional glycosylation. Alternately, in a porcine model of Becker muscular dystrophy, relative abundance of alpha-dystroglycan was decreased, consistent with a reduction in expression of the dystrophin-glycoprotein complex in affected muscle. Therefore, these new rabbit monoclonal antibodies are suitable reagents for alpha-dystroglycan core protein detection and will enhance dystroglycan-related studies.

Original languageEnglish
Article numbere97567
JournalPLoS ONE
Volume9
Issue number5
DOIs
StatePublished - May 13 2014

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