Age-related retinal degeneration (arrd2) in a novel mouse model due to a nonsense mutation in the Mdm1 gene

doi:10.1093/hmg/ddn295

Human Molecular Genetics Advance Access first published online on September 18, 2008
This version published online on September 23, 2008
Human Molecular Genetics, doi:10.1093/hmg/ddn295

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Age-related retinal degeneration (arrd2) in a novel mouse model due to a nonsense mutation in the Mdm1 gene

Bo Chang¹^,, Md Nawajes A. Mandal²^,, Venkata R. M. Chavali², Norman L. Hawes¹, Naheed W. Khan², Ronald E. Hurd¹, Richard S. Smith¹, Muriel L. Davisson¹, Laura Kopplin³, Barbara E. K. Klein⁴, Ronald Klein⁴, Sudha K. Iyengar³, John R. Heckenlively² and Radha Ayyagari²^,*

¹ The Jackson Laboratory, Bar Harbor, Maine 04609 ² W.K. Kellogg Eye Center, The University of Michigan, 1000 Wall Street, Ann Arbor, MI 48105 ³ Department of Epidemiology and Biostatistics, Case Western Reserve University, Cleveland, OH 44106 ⁴ University of Wisconsin-Madison, Dept. Ophthalmology and Visual Sciences, Madison, WI 53705

^* Corresponding author: Radha Ayyagari ( Email: rayyagari{at}ucsd.edu). Present Address: Jacobs Retina Center, Rm 206, Shiley Eye Center, University of California San Diego, 9415 Campus Point Drive, La Jolla, CA, 92093-0946., Phone: 858-534-0929, Fax: 858-534-8293

Received July 2, 2008; Revised August 25, 2008; Accepted September 9, 2008

We observed that a naturally occurring mouse strain developedage-related retinal degeneration (arrd2). These mice had normalfundi, ERGs and retinal histology at 6 months of age; vesselattenuation, RPE atrophy, and pigmentary abnormalities at 14months, which progressed to complete loss of photoreceptorsand extinguished ERG by 22 months. Genetic analysis revealedthat the retinal degeneration in arrd2 segregates in an autosomalrecessive manner and the disease gene localizes to mouse Chromosome10. A positional candidate cloning approach detected a nonsensemutation in the mouse double minute-1 gene (Mdm1), which resultsin the truncation of the putative protein from 718 amino acidsto 398. We have identified a novel transcript of the Mdm1 gene,which is the predominant transcript in the retina. The Mdm1transcript is localized to the nuclear layers of neural retina.Expression of Mdm1 in the retina increases steadily from post-natalday 30 to one year, and a high level of Mdm1 is subsequentlymaintained. The Mdm1 transcript was found to be significantlydepleted in the retina of arrd2 mice and the transcript wasobserved to degrade by nonsense-mediated decay. These resultsindicate that depletion of the Mdm1 transcript may underliethe mechanism leading to late-onset progressive retinal degenerationin arrd2 mice. Analysis of a cohort of patients with age-relatedmacular degeneration (AMD) wherein the susceptibility locusmaps to chromosome 12q, a region bearing the human orthologto MDM1, did not reveal association between human MDM1 and AMD.

The title has been corrected.

These authors contributed equally to this work

Sequences submitted to the GenBank: GI: 1064299, and GI: 1064301

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