Warning: Undefined array key "mm" in /www/wwwroot/www.ai-bt.com/si.php on line 10 Deprecated: trim(): Passing null to parameter #1 ($string) of type string is deprecated in /www/wwwroot/www.ai-bt.com/si.php on line 10 Expression of dog microdystrophin in mouse and dog muscles by gene therapy.

Literature DB >> 20179674

Expression of dog microdystrophin in mouse and dog muscles by gene therapy.

Christophe Pichavant¹, Pierre Chapdelaine, Daniel G Cerri, Jean-Christophe Dominique, Simon P Quenneville, Daniel Skuk, Joe N Kornegay, João Cs Bizario, Xiao Xiao, Jacques P Tremblay.

Abstract

Duchenne muscular dystrophy (DMD) is characterized by the absence of dystrophin. Several previous studies demonstrated the feasibility of delivering microdystrophin complementary DNA (cDNA) into mouse and normal nonhuman primate muscles by ex vivo gene therapy. However, these animal models do not reproduce completely the human DMD phenotype, while the dystrophic dog model does. To progress toward the use of the best animal model of DMD, a dog microdystrophin was transduced into human and dystrophic dog muscle precursor cells (MPCs) with a lentivirus before their transplantation into mouse muscles. One month following MPC transplantation, myofibers expressing the dog microdystrophin were observed. We also used another approach to introduce this transgene into myofibers, i.e., the electrotransfer of a plasmid coding for the dog microdystrophin. The plasmid was injected into mouse and dog muscles, and brief electric pulses were applied in the region of injection. Two weeks later, the transgene was detected in both animals. Therefore, ex vivo gene therapy and electrotransfer are two possible methods to introduce a truncated version of dystrophin into myofibers of animal models and eventually into myofibers of DMD patients.

Entities: Disease Gene Species

Mesh：

Substances：
Dystrophin

Year: 2010 PMID： 20179674 PMCID： PMC2890099 DOI： 10.1038/mt.2010.23

Source DB: PubMed Journal: Mol Ther ISSN： 1525-0016 Impact factor: 11.454

41 in total

1. Mutation segregation and rapid carrier detection of X-linked muscular dystrophy in dogs.

Authors: R J Bartlett; N J Winand; S L Secore; J T Singer; S Fletcher; S Wilton; D J Bogan; J R Metcalf-Bogan; W T Bartlett; J M Howell; B J Cooper; J N Kornegay
Journal: Am J Vet Res Date: 1996-05 Impact factor: 1.156

2. The muscle creatine kinase gene is regulated by multiple upstream elements, including a muscle-specific enhancer.

Authors: J B Jaynes; J E Johnson; J N Buskin; C L Gartside; S D Hauschka
Journal: Mol Cell Biol Date: 1988-01 Impact factor: 4.272

3. Membrane organization of the dystrophin-glycoprotein complex.

Authors: J M Ervasti; K P Campbell
Journal: Cell Date: 1991-09-20 Impact factor: 41.582

4. Antibody formation after myoblast transplantation in Duchenne-dystrophic patients, donor HLA compatible.

Authors: R Roy; J P Tremblay; J Huard; C Richards; F Malouin; J P Bouchard
Journal: Transplant Proc Date: 1993-02 Impact factor: 1.066

5. Association of dystrophin and an integral membrane glycoprotein.

Authors: K P Campbell; S D Kahl
Journal: Nature Date: 1989-03-16 Impact factor: 49.962

Review 6. Progress in therapeutic antisense applications for neuromuscular disorders.

Authors: Annemieke Aartsma-Rus; Gert-Jan B van Ommen
Journal: Eur J Hum Genet Date: 2009-10-07 Impact factor: 4.246

7. X-irradiation improves mdx mouse muscle as a model of myofiber loss in DMD.

Authors: S Wakeford; D J Watt; T A Partridge
Journal: Muscle Nerve Date: 1991-01 Impact factor: 3.217

8. Very efficient myoblast allotransplantation in mice under FK506 immunosuppression.

Authors: I Kinoshita; J T Vilquin; B Guérette; I Asselin; R Roy; J P Tremblay
Journal: Muscle Nerve Date: 1994-12 Impact factor: 3.217

9. Normal myogenic cells from newborn mice restore normal histology to degenerating muscles of the mdx mouse.

Authors: J E Morgan; E P Hoffman; T A Partridge
Journal: J Cell Biol Date: 1990-12 Impact factor: 10.539

10. Successful histocompatible myoblast transplantation in dystrophin-deficient mdx mouse despite the production of antibodies against dystrophin.

Authors: J T Vilquin; E Wagner; I Kinoshita; R Roy; J P Tremblay
Journal: J Cell Biol Date: 1995-11 Impact factor: 10.539

10 in total

Review 1. The function of dog models in developing gene therapy strategies for human health.

Authors: Keri L Nowend; Alison N Starr-Moss; Keith E Murphy
Journal: Mamm Genome Date: 2011-07-06 Impact factor: 2.957

2. Intra-amniotic rAAV-mediated microdystrophin gene transfer improves canine X-linked muscular dystrophy and may induce immune tolerance.

Authors: Hiromi Hayashita-Kinoh; Naoko Yugeta; Hironori Okada; Yuko Nitahara-Kasahara; Tomoko Chiyo; Takashi Okada; Shin'ichi Takeda
Journal: Mol Ther Date: 2015-01-14 Impact factor: 11.454

Review 3. Current status of pharmaceutical and genetic therapeutic approaches to treat DMD.

Authors: Christophe Pichavant; Annemieke Aartsma-Rus; Paula R Clemens; Kay E Davies; George Dickson; Shin'ichi Takeda; Steve D Wilton; Jon A Wolff; Christine I Wooddell; Xiao Xiao; Jacques P Tremblay
Journal: Mol Ther Date: 2011-04-05 Impact factor: 11.454

Expression of dog microdystrophin in mouse and dog muscles by gene therapy.

1. Mutation segregation and rapid carrier detection of X-linked muscular dystrophy in dogs.

2. The muscle creatine kinase gene is regulated by multiple upstream elements, including a muscle-specific enhancer.

3. Membrane organization of the dystrophin-glycoprotein complex.

4. Antibody formation after myoblast transplantation in Duchenne-dystrophic patients, donor HLA compatible.

5. Association of dystrophin and an integral membrane glycoprotein.

Review 6. Progress in therapeutic antisense applications for neuromuscular disorders.

7. X-irradiation improves mdx mouse muscle as a model of myofiber loss in DMD.

8. Very efficient myoblast allotransplantation in mice under FK506 immunosuppression.

9. Normal myogenic cells from newborn mice restore normal histology to degenerating muscles of the mdx mouse.

10. Successful histocompatible myoblast transplantation in dystrophin-deficient mdx mouse despite the production of antibodies against dystrophin.

Review 1. The function of dog models in developing gene therapy strategies for human health.

2. Intra-amniotic rAAV-mediated microdystrophin gene transfer improves canine X-linked muscular dystrophy and may induce immune tolerance.

Review 3. Current status of pharmaceutical and genetic therapeutic approaches to treat DMD.

Review 4. Duchenne muscular dystrophy gene therapy in the canine model.

5. Safety and feasibility of high-pressure transvenous limb perfusion with 0.9% saline in human muscular dystrophy.

Review 6. Nanotherapy for Duchenne muscular dystrophy.

7. Intramuscular Transplantation of Muscle Precursor Cells over-expressing MMP-9 improves Transplantation Success.

Review 8. Canine and Feline Models of Human Genetic Diseases and Their Contributions to Advancing Clinical Therapies .

9. Targeted Gene Addition of Microdystrophin in Mice Skeletal Muscle via Human Myoblast Transplantation.

Review 10. Combined Therapies for Duchenne Muscular Dystrophy to Optimize Treatment Efficacy.

Review 6. Progress in therapeutic antisense applications for neuromuscular disorders.

Review 1. The function of dog models in developing gene therapy strategies for human health.

Review 3. Current status of pharmaceutical and genetic therapeutic approaches to treat DMD.

Review 4. Duchenne muscular dystrophy gene therapy in the canine model.

Review 6. Nanotherapy for Duchenne muscular dystrophy.

Review 8. Canine and Feline Models of Human Genetic Diseases and Their Contributions to Advancing Clinical Therapies .

Review 10. Combined Therapies for Duchenne Muscular Dystrophy to Optimize Treatment Efficacy.

Review 8. Canine and Feline Models of Human Genetic Diseases and Their Contributions to Advancing Clinical Therapies .