Spectrin-like repeats from dystrophin and {alpha}-actinin-2 are not functionally interchangeable

doi:10.1093/hmg/11.16.1807

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Human Molecular Genetics, 2002, Vol. 11, No. 16 1807-1815
© 2002 Oxford University Press

Spectrin-like repeats from dystrophin and ${alpha}$ -actinin-2 are not functionally interchangeable

Scott Q. Harper¹^,2, Robert W. Crawford¹, Christiana DelloRusso¹ and Jeffrey S. Chamberlain¹^,2^,*

¹Department of Neurology, University of Washington School of Medicine, HSB Room K243, Box 357720, Seattle, WA 98195-7720, USA and ²Program in Cellular and Molecular Biology, University of Michigan Medical School, Ann Arbor, MI 48109, USA

Received March 3, 2002; Revised May 8, 2002; Accepted May 18, 2002

Mutations in the dystrophin gene result in Duchenne musculardystrophy (DMD). Dystrophin is a multidomain protein that functionsto stabilize the sarcolemmal membrane during muscle contraction.The central rod domain has been proposed to act as a shock absorber,as a force transducer or as a spacer separating important N-and C-terminal domains that interact with actin and the dystrophin–glycoproteincomplex (DGC). Structure/function studies demonstrated thatdeletion of large portions of the rod domain can result in theproduction of smaller, yet highly functional, dystrophin proteins.In a dramatic example, a ‘micro-dystrophin’ transgenecontaining only four dystrophin spectrin-like repeats resultedin complete correction of most of the symptoms associated withdystrophy in the mdx mouse model for DMD. Dystrophin sharesconsiderable homology with the multidomain, actin-crosslinkingprotein ${alpha}$ -actinin. To explore the hypothesis that the dystrophinrod domain acts as a spacer region, a chimeric micro-dystrophintransgene containing the four-repeat rod domain of ${alpha}$ -actinin-2was expressed in mdx mice. This chimeric transgene was incapableof correcting the morphological pathology of the mdx mouse,but still functioned to assemble the DGC at the membrane andprovided some protection from contraction-induced injury. Thesedata demonstrated that different spectrin-like repeats are notequivalent, and reinforced the suggestion that the dystrophinrod domain is not merely a spacer but likely contributes animportant mechanical role to overall dystrophin function.

^* To whom correspondence should be addressed. Tel: +1 2062215363;Fax: +1 2066168272; Email: jsc5{at}u.washington.edu

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Human Molecular Genetics

Spectrin-like repeats from dystrophin and -actinin-2 are not functionally interchangeable

Spectrin-like repeats from dystrophin and ${alpha}$ -actinin-2 are not functionally interchangeable