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Severe Muscular Dystrophy in Mice That Lack Dystrophin and Alpha7 Integrin.

Authors:
  • Rooney Jachinta E
  • Welser Jennifer V
  • Dechert Melissa A
  • Flintoff-Dye Nichole L
  • Kaufman Stephen J
  • Burkin Dean J

From: Department of Pharmacology, University of Nevada, Reno, 89557, USA. dburkin@med.unr.edu

Journal of cell science

  • Publish Date: Jun 2006
  • ISSN: 0021-9533
  • Volume: 119
  • Issue: Pt 11
  • Pages: 2185-95
  • Medium: Print
  • Language: English
  • Citation (JAMA): Rooney Jachinta E, Welser Jennifer V, Dechert Melissa A, et al. Severe Muscular Dystrophy in Mice That Lack Dystrophin and Alpha7 Integrin.. J. Cell. Sci. Jun 2006;119:2185-95

Abstract

The dystrophin glycoprotein complex links laminin in the extracellular matrix to the cell cytoskeleton. Loss of dystrophin causes Duchenne muscular dystrophy, the most common human X-chromosome-linked genetic disease. The alpha7beta1 integrin is a second transmembrane laminin receptor expressed in skeletal muscle. Mutations in the alpha7 integrin gene cause congenital myopathy in humans and mice. The alpha7beta1 integrin is increased in the skeletal muscle of Duchenne muscular dystrophy patients and mdx mice. This observation has led to the suggestion that dystrophin and alpha7beta1 integrin have complementary functional and structural roles. To test this hypothesis, we generated mice lacking both dystrophin and alpha7 integrin (mdx/alpha7(-/-)). The mdx/alpha7(-/-) mice developed early-onset muscular dystrophy and died at 2-4 weeks of age. Muscle fibers from mdx/alpha7(-/-) mice exhibited extensive loss of membrane integrity, increased centrally located nuclei and inflammatory cell infiltrate, greater necrosis and increased muscle degeneration compared to mdx or alpha7-integrin null animals. In addition, loss of dystrophin and/or alpha7 integrin resulted in altered expression of laminin-alpha2 chain. These results point to complementary roles for dystrophin and alpha7beta1 integrin in maintaining the functional integrity of skeletal muscle.

Mesh Headings (Keywords): Animals, Antigens, CD, Dystrophin, Integrin alpha Chains, Laminin, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Muscle, Skeletal, Muscular Dystrophy, Duchenne, Regeneration, Severity of Illness Index, Survival Rate

Check for Full Text / PubMed Unique Identifier (PMID): 16684813

This abstract is part of PubMed, a service of the U.S. National Library of Medicine. PubMed includes more than 17 million citations from MEDLINE and other life science journals for biomedical articles. See Copyright and Disclaimers.

Linked medical terms appearing on this page are added by Healia to help readers find more information and are not part of the original PubMed document.

The data herein was last updated on July 8th, 2008 and may not reflect the most current and accurate data available from NLM.

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