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Publication : Human laminin-111 and laminin-211 protein therapy prevents muscle disease progression in an immunodeficient mouse model of LAMA2-CMD.

First Author  Barraza-Flores P Year  2020
Journal  Skelet Muscle Volume  10
Issue  1 Pages  18
PubMed ID  32498713 Mgi Jnum  J:308130
Mgi Id  MGI:6728499 Doi  10.1186/s13395-020-00235-4
Citation  Barraza-Flores P, et al. (2020) Human laminin-111 and laminin-211 protein therapy prevents muscle disease progression in an immunodeficient mouse model of LAMA2-CMD. Skelet Muscle 10(1):18
abstractText  BACKGROUND: Laminin-alpha2-related congenital muscular dystrophy (LAMA2-CMD) is a devastating genetic disease caused by mutations in the LAMA2 gene. These mutations result in progressive muscle wasting and inflammation leading to delayed milestones, and reduced lifespan in affected patients. There is currently no cure or treatment for LAMA2-CMD. Preclinical studies have demonstrated that mouse laminin-111 can serve as an effective protein replacement therapy in a mouse model of LAMA2-CMD. METHODS: In this study, we generated a novel immunocompromised dy(W) mouse model of LAMA2-CMD to study the role the immune system plays in muscle disease progression. We used this immune-deficient dy(W) mouse model to test the therapeutic benefits of recombinant human laminin-111 and laminin-211 protein therapy on laminin-alpha2-deficient muscle disease progression. RESULTS: We show that immunodeficient laminin-alpha2 null mice demonstrate subtle differences in muscle regeneration compared to immunocompetent animals during early disease stages but overall exhibit a comparable muscle disease progression. We found human laminin-111 and laminin-211 could serve as effective protein replacement strategies with mice showing improvements in muscle pathology and function. We observed that human laminin-111 and laminin-211 exhibit differences on satellite and myoblast cell populations and differentially affect muscle repair. CONCLUSIONS: This study describes the generation of a novel immunodeficient mouse model that allows investigation of the role the immune system plays in LAMA2-CMD. This model can be used to assess the therapeutic potential of heterologous therapies that would elicit an immune response. Using this model, we show that recombinant human laminin-111 can serve as effective protein replacement therapy for the treatment of LAMA2-CMD.
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