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Literature DB >> 14507673

Proteasome inhibitor (MG-132) treatment of mdx mice rescues the expression and membrane localization of dystrophin and dystrophin-associated proteins.

Gloria Bonuccelli¹, Federica Sotgia, William Schubert, David S Park, Philippe G Frank, Scott E Woodman, Luigi Insabato, Michael Cammer, Carlo Minetti, Michael P Lisanti.

Abstract

Dystrophin, the protein product of the Duchenne muscular dystrophy (DMD) gene, is absent in the skeletal muscle of DMD patients and mdx mice. At the plasma membrane of skeletal muscle fibers, dystrophin associates with a multimeric protein complex, termed the dystrophin-glycoprotein complex (DGC). Protein members of this complex are normally absent or greatly reduced in dystrophin-deficient skeletal muscle fibers, and are thought to undergo degradation through an unknown pathway. As such, we reasoned that inhibition of the proteasomal degradation pathway might rescue the expression and subcellular localization of dystrophin-associated proteins. To test this hypothesis, we treated mdx mice with the well-characterized proteasomal inhibitor MG-132. First, we locally injected MG-132 into the gastrocnemius muscle, and observed the outcome after 24 hours. Next, we performed systemic treatment using an osmotic pump that allowed us to deliver different concentrations of the proteasomal inhibitor, over an 8-day period. By immunofluorescence and Western blot analysis, we show that administration of the proteasomal inhibitor MG-132 effectively rescues the expression levels and plasma membrane localization of dystrophin, beta-dystroglycan, alpha-dystroglycan, and alpha-sarcoglycan in skeletal muscle fibers from mdx mice. Furthermore, we show that systemic treatment with the proteasomal inhibitor 1) reduces muscle membrane damage, as revealed by vital staining (with Evans blue dye) of the diaphragm and gastrocnemius muscle isolated from treated mdx mice, and 2) ameliorates the histopathological signs of muscular dystrophy, as judged by hematoxylin and eosin staining of muscle biopsies taken from treated mdx mice. Thus, the current study opens new and important avenues in our understanding of the pathogenesis of DMD. Most importantly, these new findings may have clinical implications for the pharmacological treatment of patients with DMD.

Entities: Chemical

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Year: 2003 PMID： 14507673 PMCID： PMC1868305 DOI： 10.1016/S0002-9440(10)63523-7

Source DB: PubMed Journal: Am J Pathol ISSN： 0002-9440 Impact factor: 4.307

44 in total

1. Dystrophin expression in the mdx mouse restored by stem cell transplantation.

Authors: E Gussoni; Y Soneoka; C D Strickland; E A Buzney; M K Khan; A F Flint; L M Kunkel; R C Mulligan
Journal: Nature Date: 1999-09-23 Impact factor: 49.962

Review 2. Caveolins, liquid-ordered domains, and signal transduction.

Authors: E J Smart; G A Graf; M A McNiven; W C Sessa; J A Engelman; P E Scherer; T Okamoto; M P Lisanti
Journal: Mol Cell Biol Date: 1999-11 Impact factor: 4.272

3. Delay of muscle degeneration and necrosis in mdx mice by calpain inhibition.

Authors: M A Badalamente; A Stracher
Journal: Muscle Nerve Date: 2000-01 Impact factor: 3.217

4. Inhibitors of the proteasome reduce the accelerated proteolysis in atrophying rat skeletal muscles.

Authors: N E Tawa; R Odessey; A L Goldberg
Journal: J Clin Invest Date: 1997-07-01 Impact factor: 14.808

5. Increased caveolin-3 levels in mdx mouse muscles.

Authors: P L Vaghy; J Fang; W Wu; L P Vaghy
Journal: FEBS Lett Date: 1998-07-10 Impact factor: 4.124

6. Caveolin-3 is not an integral component of the dystrophin glycoprotein complex.

Authors: R H Crosbie; H Yamada; D P Venzke; M P Lisanti; K P Campbell
Journal: FEBS Lett Date: 1998-05-08 Impact factor: 4.124

7. Utrophin-dystrophin-deficient mice as a model for Duchenne muscular dystrophy.

Authors: A E Deconinck; J A Rafael; J A Skinner; S C Brown; A C Potter; L Metzinger; D J Watt; J G Dickson; J M Tinsley; K E Davies
Journal: Cell Date: 1997-08-22 Impact factor: 41.582

8. Mutations in the caveolin-3 gene cause autosomal dominant limb-girdle muscular dystrophy.

Authors: C Minetti; F Sotgia; C Bruno; P Scartezzini; P Broda; M Bado; E Masetti; M Mazzocco; A Egeo; M A Donati; D Volonte; F Galbiati; G Cordone; F D Bricarelli; M P Lisanti; F Zara
Journal: Nat Genet Date: 1998-04 Impact factor: 38.330

9. Increased number of caveolae and caveolin-3 overexpression in Duchenne muscular dystrophy.

Authors: S Repetto; M Bado; P Broda; G Lucania; E Masetti; F Sotgia; I Carbone; A Pavan; E Bonilla; G Cordone; M P Lisanti; C Minetti
Journal: Biochem Biophys Res Commun Date: 1999-08-11 Impact factor: 3.575

10. Phenotypic behavior of caveolin-3 mutations that cause autosomal dominant limb girdle muscular dystrophy (LGMD-1C). Retention of LGMD-1C caveolin-3 mutants within the golgi complex.

Authors: F Galbiati; D Volonte; C Minetti; J B Chu; M P Lisanti
Journal: J Biol Chem Date: 1999-09-03 Impact factor: 5.157

55 in total

Proteasome inhibitor (MG-132) treatment of mdx mice rescues the expression and membrane localization of dystrophin and dystrophin-associated proteins.

1. Dystrophin expression in the mdx mouse restored by stem cell transplantation.

Review 2. Caveolins, liquid-ordered domains, and signal transduction.

3. Delay of muscle degeneration and necrosis in mdx mice by calpain inhibition.

4. Inhibitors of the proteasome reduce the accelerated proteolysis in atrophying rat skeletal muscles.

5. Increased caveolin-3 levels in mdx mouse muscles.

6. Caveolin-3 is not an integral component of the dystrophin glycoprotein complex.

7. Utrophin-dystrophin-deficient mice as a model for Duchenne muscular dystrophy.

8. Mutations in the caveolin-3 gene cause autosomal dominant limb-girdle muscular dystrophy.

9. Increased number of caveolae and caveolin-3 overexpression in Duchenne muscular dystrophy.

10. Phenotypic behavior of caveolin-3 mutations that cause autosomal dominant limb girdle muscular dystrophy (LGMD-1C). Retention of LGMD-1C caveolin-3 mutants within the golgi complex.

Review 1. Duchenne muscular dystrophy and dystrophin: pathogenesis and opportunities for treatment.

Review 2. What has the mdx mouse model of Duchenne muscular dystrophy contributed to our understanding of this disease?

3. Altered ubiquitin-proteasome signaling in right ventricular hypertrophy and failure.

Review 4. Immunobiology of Inherited Muscular Dystrophies.

Review 5. The ubiquitin-proteasome system and nonsense-mediated mRNA decay in hypertrophic cardiomyopathy.

6. Alterations of dystrophin-associated glycoproteins in the heart lacking dystrophin or dystrophin and utrophin.

7. Inhibitory effect of ubiquitin-proteasome pathway on proliferation of esophageal carcinoma cells.

8. Immunoproteasome in animal models of Duchenne muscular dystrophy.

Review 9. Recent advances using zebrafish animal models for muscle disease drug discovery.

10. β1-syntrophin modulation by miR-222 in mdx mice.