Mutation-independent Proteomic Signatures of Pathological Progression in Murine Models of Duchenne Muscular Dystrophy

Tle., van Westering; Johansson, Henrik J.; Hanson, Britt; Coenen-Stass, Anna M.L.; Lomonosova, Yulia; Tanihata, Jun; Matsuki, Norio; Yokota, Toshifumi; Takeda, Shin’ichi; Lehtiö, Janne; Wood, Matthew J.; Andaloussi, Samir El; Aoki, Yosuke; Roberts, Thomas C.

doi:10.1074/mcp.ra120.002345

Cited by 27 publications

(24 citation statements)

References 109 publications

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“…Importantly, the mdx mouse exhibits only a small decrease in lifespan, and impairment of muscle function is relatively mild. Disease in the mdx mouse is similar to that observed in other dystrophin-null models 45 . In contrast, the dKO mouse (a double knock-out of dystrophin and its paralog utrophin) exhibits much more severe pathology, including kyphosis, respiratory difficulties, and premature death (animals typically die ~8-10 weeks of age) [46][47][48][49] .…”

Section: Introductionsupporting

confidence: 74%

Non-uniform dystrophin re-expression after CRISPR-mediated exon excision in the dystrophin/utrophin double-knockout mouse model of DMD

Hanson

Stenler

Ahlskog

et al. 2022

Preprint

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Duchenne muscular dystrophy (DMD) is the most prevalent inherited myopathy affecting children, caused by genetic loss of the gene encoding the dystrophin protein. There are currently four FDA-approved drugs for DMD that aim to restore expression of dystrophin by exon skipping using splice switching oligonucleotides. While these therapies require lifelong repeat administration, recent advancements in gene editing technologies have raised the possibility of achieving 'permanent exon skipping', and thereby curing the disease with a single treatment. Here we have investigated the use of the Staphylococcus aureus CRISPR/Cas9 system and a double-cut strategy, delivered using a pair of AAV9 vectors, for dystrophin restoration in the severely-affected dystrophin/utrophin double knock-out (dKO) mouse. Single guide RNAs were designed to induce double-strand DNA breaks on either side of Dmd exon 23, such that the intervening exon 23 sequence is excised when the flanking intronic regions are joined via the non-homologous end joining repair pathway. Exon 23 deletion was confirmed at the DNA level by PCR and Sanger sequencing, and at the RNA level by RT-qPCR. Restoration of dystrophin protein expression was demonstrated by western blot and immunofluorescence staining in mice treated via either intraperitoneal or intravenous routes of delivery. Dystrophin restoration was most effective in the diaphragm, where a maximum of 5.7% of wild-type dystrophin expression was observed. CRISPR treatment was insufficient to extend lifespan in the dKO mouse, and dystrophin was expressed in a within-fiber patchy manner in skeletal muscle tissues. Further analysis revealed a plethora of non-productive DNA repair events, including AAV genome integration at the CRISPR cut sites. This study highlights potential challenges for the successful development of CRISPR therapies in the context of DMD.

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Section: Introductionsupporting

confidence: 74%

Non-uniform dystrophin re-expression after CRISPR-mediated exon excision in the dystrophin/utrophin double-knockout mouse model of DMD

Hanson

Stenler

Ahlskog

et al. 2022

Preprint

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“…The heat map illustrates the distribution pattern of changes between normal and dystrophic specimens. In contrast to other sub-types of dystrophin-deficient skeletal muscles [ 31 , 39 , 42 , 84 , 85 , 86 , 87 ], Dp427-lacking EOMs seem to exhibit relatively minor proteome-wide changes.…”

Section: Resultsmentioning

confidence: 85%

Mass Spectrometric Profiling of Extraocular Muscle and Proteomic Adaptations in the mdx-4cv Model of Duchenne Muscular Dystrophy

Gargan

Dowling

Zweyer

et al. 2021

Life

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Extraocular muscles (EOMs) represent a specialized type of contractile tissue with unique cellular, physiological, and biochemical properties. In Duchenne muscular dystrophy, EOMs stay functionally unaffected in the course of disease progression. Therefore, it was of interest to determine their proteomic profile in dystrophinopathy. The proteomic survey of wild type mice and the dystrophic mdx-4cv model revealed a broad spectrum of sarcomere-associated proteoforms, including components of the thick filament, thin filament, M-band and Z-disk, as well as a variety of muscle-specific markers. Interestingly, the mass spectrometric analysis revealed unusual expression levels of contractile proteins, especially isoforms of myosin heavy chain. As compared to diaphragm muscle, both proteomics and immunoblotting established isoform MyHC14 as a new potential marker in wild type EOMs, in addition to the previously identified isoforms MyHC13 and MyHC15. Comparative proteomics was employed to establish alterations in the protein expression profile between normal EOMs and dystrophin-lacking EOMs. The analysis of mdx-4cv EOMs identified elevated levels of glycolytic enzymes and molecular chaperones, as well as decreases in mitochondrial enzymes. These findings suggest a process of adaptation in dystrophin-deficient EOMs via a bioenergetic shift to more glycolytic metabolism, as well as an efficient cellular stress response in EOMs in dystrophinopathy.

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“…The analysis of proteins and the proteome, their activity, interaction, localization and composition, structure and function are some of the aspects proteomics may resolve. Proteomic experiments are generally used to detect specific signatures of disease progression [ 73 ], to unravel pathogenicity mechanisms and detect biomarkers, or to discover targets or processes for therapeutic intervention [ 74 , 75 ]. In 2004, Jaffe et al coined the concept of proteogenomics, a viewpoint focused on the integration of genomic and proteomic data [ 76 ].…”

Section: Multi-omics Approachesmentioning

confidence: 99%

The Increasing Impact of Translational Research in the Molecular Diagnostics of Neuromuscular Diseases

Yubero

Benito

Pijuan

et al. 2021

IJMS

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The diagnosis of neuromuscular diseases (NMDs) has been progressively evolving from the grouping of clinical symptoms and signs towards the molecular definition. Optimal clinical, biochemical, electrophysiological, electrophysiological, and histopathological characterization is very helpful to achieve molecular diagnosis, which is essential for establishing prognosis, treatment and genetic counselling. Currently, the genetic approach includes both the gene-targeted analysis in specific clinically recognizable diseases, as well as genomic analysis based on next-generation sequencing, analyzing either the clinical exome/genome or the whole exome or genome. However, as of today, there are still many patients in whom the causative genetic variant cannot be definitely established and variants of uncertain significance are often found. In this review, we address these drawbacks by incorporating two additional biological omics approaches into the molecular diagnostic process of NMDs. First, functional genomics by introducing experimental cell and molecular biology to analyze and validate the variant for its biological effect in an in-house translational diagnostic program, and second, incorporating a multi-omics approach including RNA-seq, metabolomics, and proteomics in the molecular diagnosis of neuromuscular disease. Both translational diagnostics programs and omics are being implemented as part of the diagnostic process in academic centers and referral hospitals and, therefore, an increase in the proportion of neuromuscular patients with a molecular diagnosis is expected. This improvement in the process and diagnostic performance of patients will allow solving aspects of their health problems in a precise way and will allow them and their families to take a step forward in their lives.

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Mutation-independent Proteomic Signatures of Pathological Progression in Murine Models of Duchenne Muscular Dystrophy

Cited by 27 publications

References 109 publications

Non-uniform dystrophin re-expression after CRISPR-mediated exon excision in the dystrophin/utrophin double-knockout mouse model of DMD

Non-uniform dystrophin re-expression after CRISPR-mediated exon excision in the dystrophin/utrophin double-knockout mouse model of DMD

Mass Spectrometric Profiling of Extraocular Muscle and Proteomic Adaptations in the mdx-4cv Model of Duchenne Muscular Dystrophy

The Increasing Impact of Translational Research in the Molecular Diagnostics of Neuromuscular Diseases

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