Fibroblast phenotype in male carriers of FMR1 premutation alleles

doi:10.1093/hmg/ddp497

Human Molecular Genetics Advance Access first published online on October 28, 2009
This version [Corrected Proof] published online on November 11, 2009
Human Molecular Genetics, doi:10.1093/hmg/ddp497

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Fibroblast phenotype in male carriers of FMR1 premutation alleles

Dolores Garcia-Arocena¹, Jane E. Yang¹, Judith R. Brouwer³, Flora Tassone¹^,4, Christine Iwahashi¹, Elizabeth M. Berry-Kravis⁷, Christopher G. Goetz⁸, Allison M. Sumis⁹, Lili Zhou⁹, Danh V. Nguyen², Luis Campos², Erin Howell¹, Anna Ludwig¹, Claudia Greco⁵, Rob Willemsen³, Randi J. Hagerman⁴^,6 and Paul J. Hagerman¹^,4^,*

¹ Department of Biochemistry and Molecular Medicine and ² Division of Biostatistics, Department of Public Health Sciences, School of Medicine, University of California, Davis, CA, USA, ³ CBG-Department of Clinical Genetics, Erasmus MC, Rotterdam, The Netherlands, ⁴ M.I.N.D. Institute, ⁵ Department of Pathology and ⁶ Department of Pediatrics, University of California, Davis, Health System, Sacramento, CA, USA, ⁷ Departments of Pediatrics, Neurological Sciences, and Biochemistry, ⁸ Departments of Neurological Sciences and Pharmacology and ⁹ Department of Pediatrics, Rush University Medical Center, Chicago, IL, USA

^* To whom correspondence should be addressed at: Department of Biochemistry and Molecular Medicine, University of California, Davis, School of Medicine, One Shields Avenue, Davis, CA 95616, USA. Tel: +1 5307547266; Fax: +1 5307547269; Email: pjhagerman{at}ucdavis.edu

Received June 16, 2009; Accepted October 26, 2009

Fragile X-associated tremor/ataxia syndrome (FXTAS) is an adult-onsetneurodegenerative disorder among carriers of premutation expansions(55–200 CGG repeats) of the fragile X mental retardation1 (FMR1) gene. The clinical features of FXTAS, as well as variousforms of clinical involvement in carriers without FXTAS, arethought to arise through a direct toxic gain of function ofhigh levels of FMR1 mRNA containing the expanded CGG repeat.Here we report a cellular endophenotype involving increasedstress response (HSP27, HSP70 and CRYAB) and altered lamin A/Cexpression/organization in cultured skin fibroblasts from 11male carriers of premutation alleles of the FMR1 gene, includingsix patients with FXTAS and five premutation carriers with noclinical evidence of FXTAS, compared with six controls. A similarabnormal cellular phenotype was found in CNS tissue from 10patients with FXTAS. Finally, there is an analogous abnormalcellular distribution of lamin A/C isoforms in knock-in micebearing the expanded CGG repeat in the murine Fmr1 gene. Thesealterations are evident even in mouse embryonic fibroblasts,raising the possibility that, in humans, the expanded-repeatmRNA triggers pathogenic mechanisms early in development, thusproviding a molecular basis for the neurodevelopmental abnormalitiesobserved in some children and clinical symptoms in some adultswho are carriers of premutation FMR1 alleles. Cellular dysregulationin fibroblasts represents a novel and highly advantageous modelfor investigating disease pathogenesis in premutation carriersand for quantifying and monitoring disease progression. Fibroblaststudies may also prove useful in screening and testing the efficacyof therapeutic interventions.

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