Localized Treatment with a Novel FDA-Approved Proteasome Inhibitor Blocks the Degradation of Dystrophin and Dystrophin-Associated Proteins in mdx Mice

Bonuccelli, Gloria; Sotgia, Federica; Capozza, Franco; Gazzerro, Elisabetta; Minetti, Carlo; Lisanti, Michael P.

doi:10.4161/cc.6.10.4182

Cited by 67 publications

(72 citation statements)

References 32 publications

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“…Immunohistochemical (Figure 6i) and WB (Figure 6j) analysis confirmed that β-sarcoglycan expression was markedly reduced at the sarcolemma of skeletal muscle fibers from untreated mdx mice, and it was upregulated in muscles of ONX-0914 treated mice. Similar to previously observations by Bonuccelli,6,23 we suggested that dystrophin re-expression allowed the rescue of DGC complex at the sarcolemma. ONX-0914 treatment reduces dystrophic muscle inflammation in 6-weeks-old mice As the fibroadipogenic degeneration of muscular fibers could be promoted by interaction of inflammatory cells with resident muscle cells, 25,26 we analyzed inflammatory infiltrates in ONX-0914 treated skeletal dystrophic muscles.…”

Section: I-proteosome Inhibition Ameliorates Muscular Dystrophic Featsupporting

confidence: 79%

“…Moreover, WB analysis confirmed the expression of a 120 kDa molecular weight dystrophin protein (Figure 6f), accordingly to previous works. 6,23,24 Interestingly, the ONX-0914 treated mdx showed a reduction of the serum creatine phospho-kinases (CPK) released from damaged myofibers, suggesting muscle preservation in treated animals. Serum CPK levels dramatically decreased throughout the treatment, reaching the physiological level observed in wildtype C57Bl mice (Figure 6g).…”

Section: I-proteosome Inhibition Ameliorates Muscular Dystrophic Featmentioning

confidence: 99%

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Therapeutic Potential of Immunoproteasome Inhibition in Duchenne Muscular Dystrophy

et al. 2016

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Duchenne muscular dystrophy is an inherited fatal genetic disease characterized by mutations in dystrophin gene, causing membrane fragility leading to myofiber necrosis and inflammatory cell recruitment in dystrophic muscles. The resulting environment enriched in proinflammatory cytokines, like IFN-γ and TNF-α, determines the transformation of myofiber constitutive proteasome into the immunoproteasome, a multisubunit complex involved in the activation of cell-mediate immunity. This event has a fundamental role in producing peptides for antigen presentation by MHC class I, for the immune response and also for cytokine production and T-cell differentiation. Here, we characterized for the first time the presence of T-lymphocytes activated against revertant dystrophin epitopes, in the animal model of Duchenne muscular dystrophy, the mdx mice. Moreover, we specifically blocked i-proteasome subunit LMP7, which was up-regulated in dystrophic skeletal muscles, and we demonstrated the rescue of the dystrophin expression and the amelioration of the dystrophic phenotype. The i-proteasome blocking lowered myofiber MHC class I expression and self-antigen presentation to T cells, thus reducing the specific antidystrophin T cell response, the muscular cell infiltrate, and proinflammatory cytokine production, together with muscle force recovery. We suggest that i-proteasome inhibition should be considered as new promising therapeutic approach for Duchenne muscular dystrophy pathology.

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Section: I-proteosome Inhibition Ameliorates Muscular Dystrophic Featsupporting

confidence: 79%

Section: I-proteosome Inhibition Ameliorates Muscular Dystrophic Featmentioning

confidence: 99%

Therapeutic Potential of Immunoproteasome Inhibition in Duchenne Muscular Dystrophy

et al. 2016

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“…Each of the tested proteasome inhibitors restored mutant dystrophin to WT levels at concentrations less than 10 μM. Several previous studies have tested proteasome inhibition to treat the nonsense mutation mdx mouse model of dystrophinopathy (44)(45)(46)(47) but have reported contradictory results. Although proteasome inhibition by MG132 in the mdx mouse restored the amino-terminal fragment of dystrophin translated up to the premature stop codon (44), prolonged treatment with MG132 resulted in no improvement of muscle function (46).…”

Section: Discussionmentioning

confidence: 99%

Disease-proportional proteasomal degradation of missense dystrophins

Talsness

Belanto

Ervasti

2015

Proc. Natl. Acad. Sci. U.S.A.

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The 427-kDa protein dystrophin is expressed in striated muscle where it physically links the interior of muscle fibers to the extracellular matrix. A range of mutations in the DMD gene encoding dystrophin lead to a severe muscular dystrophy known as Duchenne (DMD) or a typically milder form known as Becker (BMD). Patients with nonsense mutations in dystrophin are specifically targeted by stop codon read-through drugs, whereas out-of-frame deletions and insertions are targeted by exon-skipping therapies. Both treatment strategies are currently in clinical trials. Dystrophin missense mutations, however, cause a wide range of phenotypic severity in patients. The molecular and cellular consequences of such mutations are not well understood, and there are no therapies specifically targeting this genotype. Here, we have modeled two representative missense mutations, L54R and L172H, causing DMD and BMD, respectively, in full-length dystrophin. In vitro, the mutation associated with the mild phenotype (L172H) caused a minor decrease in tertiary stability, whereas the L54R mutation associated with a severe phenotype had a more dramatic effect. When stably expressed in mammalian muscle cells, the mutations caused steadystate decreases in dystrophin protein levels inversely proportional to the tertiary stability and directly caused by proteasomal degradation. Both proteasome inhibitors and heat shock activators were able to increase mutant dystrophin to WT levels, establishing the new cell lines as a platform to screen for potential therapeutics personalized to patients with destabilized dystrophin.Duchenne muscular dystrophy | missense mutation | protein folding | proteasome inhibitor | heat shock activator

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“…mg/m 2 no segundo ciclo e, no terceiro para 1,60 mg/m 2 . Esse ajuste de dose se justifica pela inibição da atividade do proteassoma pelo bortezomibe ser dose-dependente e de atuação reversível sobre o sitio quimiotripsina-símile, com melhores resultados sobre a fibra muscular quando utilizado na dose máxima (BONUCCELLI et al, 2003;BONUCCELLI et al, 2007).…”

Section: Delineamento Experimentalunclassified

“…No entanto, para diagnostico da deficiência especifica de distrofina no músculo, ambas as técnicas são consideradas efetivas (VAINZOF et al, 1991 Nos estudos de Bonuccelli et al (2003), Assereto et al (2006) e Bonuccelli (2007 melhores resultados quanto restauração da distrofina e proteínas associadas nas fibras musculares tratadas com inibidores de proteassoma ocorreu de forma dose-dependente, ou seja, melhores alterações na integridade da fibra muscular quando administradas maiores doses do inibidor. Em nosso estudo, apesar de termos aumentado a dose a cada ciclo de administração, essa comparação não foi possível, uma vez que realizamos duas biópsias musculares, uma antes do tratamento e após o mesmo (T1).…”

Section: Microscopia Eletrônica De Transmissão (Met)unclassified

Uso de Bortezomibe (PS-341) em cães da raça Golden Retriever afetados pela Distrofia Muscular Progressiva (GRMD) - Avaliação da viabilidade da terapia e reestruturação da Distrofina Muscular

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Localized Treatment with a Novel FDA-Approved Proteasome Inhibitor Blocks the Degradation of Dystrophin and Dystrophin-Associated Proteins in mdx Mice

Cited by 67 publications

References 32 publications

Therapeutic Potential of Immunoproteasome Inhibition in Duchenne Muscular Dystrophy

Therapeutic Potential of Immunoproteasome Inhibition in Duchenne Muscular Dystrophy

Disease-proportional proteasomal degradation of missense dystrophins

Uso de Bortezomibe (PS-341) em cães da raça Golden Retriever afetados pela Distrofia Muscular Progressiva (GRMD) - Avaliação da viabilidade da terapia e reestruturação da Distrofina Muscular

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