A role for β-dystroglycan in the organization and structure of the nucleus in myoblasts

Ivette A. Martínez-Vieyra, Alejandra Vásquez-Limeta, Ricardo González-Ramírez, Sara L. Morales-Lázaro, Mónica Mondragón, Ricardo Mondragón, Arturo Ortega, Steve J. Winder, Bulmaro Cisneros

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29 Citas (Scopus)

Resumen

We recently characterized a nuclear import pathway for β-dystroglycan; however, its nuclear role remains unknown. In this study, we demonstrate for the first time, the interaction of β-dystroglycan with distinct proteins from different nuclear compartments, including the nuclear envelope (NE) (emerin and lamins A/C and B1), splicing speckles (SC35), Cajal bodies (p80-coilin), and nucleoli (Nopp140). Electron microscopy analysis revealed that β-dystroglycan localized in the inner nuclear membrane, nucleoplasm, and nucleoli. Interestingly, downregulation of β-dystroglycan resulted in both mislocalization and decreased expression of emerin and lamin B1, but not lamin A/C, as well in disorganization of nucleoli, Cajal bodies, and splicing speckles with the concomitant decrease in the levels of Nopp140, and p80-coilin, but not SC35. Quantitative reverse transcription PCR and cycloheximide-mediated protein arrest assays revealed that β-dystroglycan deficiency did not change mRNA expression of NE proteins emerin and lamin B1 bud did alter their stability, accelerating protein turnover. Furthermore, knockdown of β-dystroglycan disrupted NE-mediated processes including nuclear morphology and centrosome-nucleus linkage, which provides evidence that β-dystroglycan association with NE proteins is biologically relevant. Unexpectedly, β-dystroglycan-depleted cells exhibited multiple centrosomes, a characteristic of cancerous cells. Overall, these findings imply that β-dystroglycan is a nuclear scaffolding protein involved in nuclear organization and NE structure and function, and that might be a contributor to the biogenesis of nuclear envelopathies.

Idioma originalInglés
Páginas (desde-hasta)698-711
Número de páginas14
PublicaciónBiochimica et Biophysica Acta - Molecular Cell Research
Volumen1833
N.º3
DOI
EstadoPublicada - mar. 2013
Publicado de forma externa

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