Laminin-111 protein therapy prevents muscle disease in the
            <i>mdx</i>
            mouse model for Duchenne muscular dystrophy

Rooney, Jachinta E.; Gurpur, Praveen B.; Burkin, Dean J.

doi:10.1073/pnas.0811599106

Cited by 114 publications

(114 citation statements)

References 27 publications

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“…Studies have indicated that the 71 integrin might act to modulate the organization and deposition of the muscle extracellular matrix (Colognato et al, 1999;Rooney et al, 2009a). To investigate the mechanism by which enhanced 7 integrin expression improved the myopathic phenotype in the absence of the laminin-211-laminin-221 ligand, we examined changes in levels of other ;itga7+ animals have 7-fold and 2.9-fold more galectin-3 protein compared with that in both wildtype and dy W-/-animals, respectively (***P<0.001).…”

Section: Discussionmentioning

confidence: 99%

“…Cryosections from 4-week-old TA and diaphragm muscle were stained using hematoxylin and eosin, as previously described (Rooney et al, 2009a), and were used to determine the percentage of myofibers that contained CLN using a Zeiss Axioskop 2 Plus fluorescence microscope. A minimum of 1000 fibers per animal (five animals per group) were counted and the percentage of myofibers with CLN calculated.…”

Section: Hematoxylin and Eosin Stainingmentioning

confidence: 99%

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Transgenic overexpression of the α7 integrin reduces muscle pathology and improves viability in the dyW mouse model of merosin-deficient congenital muscular dystrophy type 1A

Doe

Wuebbles

Allred

et al. 2011

Journal of Cell Science

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SummaryMerosin-deficient congenital muscular dystrophy 1A (MDC1A) is a devastating neuromuscular disease that results in children being confined to a wheelchair, requiring ventilator assistance to breathe and premature death. MDC1A is caused by mutations in the LAMA2 gene, which results in the partial or complete loss of laminin-211 and laminin-221, the major laminin isoforms found in the basal lamina of skeletal muscle. MDC1A patients exhibit reduced 71 integrin; however, it is unclear how the secondary loss of 71 integrin contributes to MDC1A disease progression. To investigate whether restoring 7 integrin expression can alleviate the myopathic phenotype observed in MDC1A, we produced transgenic mice that overexpressed the 7 integrin in the skeletal muscle of the dy W-/-mouse model of MDC1A. Enhanced expression of the 7 integrin restored sarcolemmal localization of the 71 integrin to laminin-2-deficient myofibers, changed the composition of the muscle extracellular matrix, reduced muscle pathology, maintained muscle strength and function and improved the life expectancy of dy W-/-mice. Taken together, these results indicate that enhanced expression of 7 integrin prevents muscle disease progression through augmentation and/or stabilization of the existing extracellular matrix in laminin-2-deficient mice, and strategies that increase 7 integrin in muscle might provide an innovative approach for the treatment of MDC1A.

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Section: Discussionmentioning

confidence: 99%

Section: Hematoxylin and Eosin Stainingmentioning

confidence: 99%

Transgenic overexpression of the α7 integrin reduces muscle pathology and improves viability in the dyW mouse model of merosin-deficient congenital muscular dystrophy type 1A

Doe

Wuebbles

Allred

et al. 2011

Journal of Cell Science

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“…27 . The most advanced approach is via delivery of Laminin-111 protein, although the efficacy remains low and the need to produce a large amount of bioactive protein is challenging 27 .…”

Section: E)mentioning

confidence: 99%

“…27 . The most advanced approach is via delivery of Laminin-111 protein, although the efficacy remains low and the need to produce a large amount of bioactive protein is challenging 27 . In addition, the utilization of CRISPR/dCas9 system to upregulate Lama1 in mdx mice has been achieved locally via electroporation, which is not easily translatable into clinical settings 28 .…”

Section: E)mentioning

confidence: 99%

A mutation-independent approach via transcriptional upregulation of a disease modifier gene rescues muscular dystrophy in vivo

Kemaladewi

Lindsay

et al. 2018

Preprint

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Introductory paragraphIdentification of protective and/or pathogenic genetic modifiers provides important insight into the heterogeneity of disease presentations in individuals affected by neuromuscular disorders (NMDs), despite having well-defined pathogenic variants. Targeting modifier genes to improve disease phenotypes could be especially beneficial in cases where the causative genes are large, structurally complex and the mutations are heterogeneous. Here, we report a mutation-independent strategy to upregulate expression of a compensatory disease-modifying gene in Congenital Muscular Dystrophy type 1A (MDC1A) using a CRISPR/dCas9-based transcriptional activation system. MDC1A is caused by nonfunctional Laminin α2, which compromises muscle fibers stability and axon myelination in peripheral nerves 1. Transgenic overexpression of Lama1, encoding a structurally similar protein Laminin α1, ameliorates muscle wasting and paralysis in the MDC1A mouse models, demonstrating its role as a protective disease modifier 2. Yet, upregulation of Lama1 as a postnatal gene therapy is hampered by its large size, which exceeds the current genome packaging capacity of clinically relevant delivery vehicles such as adeno-associated viral vectors (AAVs). In this study, we sought to upregulate Lama1 using CRISPR/dCas9-based transcriptional activation system, comprised of catalytically inactive S. aureus Cas9 (dCas9) fused to VP64 transactivation domains and sgRNAs targeting the Lama1 promoter. We first demonstrated robust upregulation of Lama1 in myoblasts, and following AAV9-mediated intramuscular delivery, in skeletal muscles of dy2j/dy2j mouse model of MDC1A.We therefore assessed whether systemic upregulation of Lama1 would yield therapeutic benefits in dy2j/dy2j mice. When the intervention was started early in pre-symptomatic dy2j/dy2j mice, Lama1 upregulation prevented muscle fibrosis and hindlimb paralysis. An important question for future therapeutic approaches for a variety of disorders concerns the therapeutic window and phenotypic reversibility. This is particularly true for muscular dystrophies as it has long been hypothesized that fibrotic changes in skeletal muscle represent an irreversible disease state that would impair any therapeutic intervention at advanced stages of the disease. Here, we demonstrate that dystrophic features and disease progression were significantly improved and partially reversed when the treatment was initiated in symptomatic 3-week old dy2j/dy2j mice with already-apparent hind limb paralysis and significant muscle fibrosis.Collectively, our data demonstrate the feasibility and therapeutic benefit of CRISPR/dCas9-mediated modulation of a disease modifier gene, which opens up an entirely new and mutation-independent treatment approach for all MDC1A patients. Moreover, this treatment strategy provides evidence that muscle fibrosis can be reversible, thus extending the therapeutic window for this disorder. Our data provide a proof-of-concept strategy that can be applied to a variety of disease modifier genes and a powerful therapeutic approach for various inherited and acquired diseases.

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“…14 LM-111 supplementation has demonstrated remarkable regenerative capacity in several models of muscular disease [15][16][17] and injury, 18 primarily by enhancing satellite cell activity. In mice with congenital muscular dystrophy due to missing LM α 2 chains, overall health and survival can be improved by administration of LM α1 chains, 19,20 In vitro, LM-111 promotes muscle stem cell proliferation and differentiation to a greater extent than other ECM components such as collagen type I and fibronectin.…”

Section: Skeletal Muscle Regenerationmentioning

confidence: 99%

Laminin Enriched Scaffolds for Tissue Engineering Applications

Garg¹

2017

ATROA

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Laminin (LM) is heterotrimeric large molecular weight glycoprotein that forms a crucial component of the basal lamina (or basement membrane) of most tissues. LMs are integral for cell adhesion, proliferation, survival, migration, and differentiation. Several studies have used a LM-coated 2D substrate for the culture and maintenance of stem cell phenotype in vitro. Recent studies have reported that LM can also be incorporated in 3D scaffolds for tissue engineering applications. This article illustrates the bioactivity and regenerative potential of LM protein in 3D scaffolds for skeletal muscle, nerve, vascular, and intervertebral-disc regeneration.

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Laminin-111 protein therapy prevents muscle disease in the mdx mouse model for Duchenne muscular dystrophy

Cited by 114 publications

References 27 publications

Transgenic overexpression of the α7 integrin reduces muscle pathology and improves viability in the dyW mouse model of merosin-deficient congenital muscular dystrophy type 1A

Transgenic overexpression of the α7 integrin reduces muscle pathology and improves viability in the dyW mouse model of merosin-deficient congenital muscular dystrophy type 1A

A mutation-independent approach via transcriptional upregulation of a disease modifier gene rescues muscular dystrophy in vivo

Laminin Enriched Scaffolds for Tissue Engineering Applications

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