Epigenetic Modifications of the FMR1 Gene

  • Elisabetta Tabolacci
  • Giovanni Neri
Protocol
First Online:
Part of the Methods in Molecular Biology book series (MIMB, volume 1010)

Abstract

The fragile X syndrome (FXS), the most common cause of heritable intellectual disability, is caused by expansion of a CGG repeat located at the 5′ UTR of the FMR1 gene and subsequent epigenetic modifications of its promoter. Epigenetic modifications include both methylation of the cytosines of the CpG island in the promoter region and of the expanded CGG triplet, and posttranslational histone changes. The combination of these changes, one structural (expansion) and one epigenetic (methylation and histone modifications), results in transcriptional silencing, even though the coding region of the FMR1 gene remains intact. Here we describe the molecular methods used to study both DNA methylation and histone epigenetic modifications, namely, bisulfite sequencing and quantification of immunoprecipitated DNA after Chromatin Immunoprecipitation (ChIP).

Key words

FMR1 gene Fragile X syndrome FXS DNA methylation Histone changes Bisulfite sequencing Chromatin immunoprecipitation Epigenetic modifications CGG expansion FMRP 
This is a preview of subscription content, log in to check access.

Notes

Acknowledgments

The authors’ work cited in the references was supported by Telethon Onlus and by the FRAXA Foundation.

References

  1. 1.
    Hagerman PJ (2008) The Fragile X prevalence paradox. J Med Genet 45:498–499PubMedCrossRefGoogle Scholar
  2. 2.
    Smeets HJ, Smits AP, Verheij CE et al (1995) Normal phenotype in two brothers with a full FMR1 mutation. Hum Mol Genet 4:2103–2108PubMedCrossRefGoogle Scholar
  3. 3.
    Pietrobono R, Tabolacci E, Zalfa F et al (2005) Molecular dissection of the events leading to inactivation of the FMR1 gene. Hum Mol Genet 14:267–277PubMedCrossRefGoogle Scholar
  4. 4.
    Tabolacci E, Moscato U, Zalfa F et al (2008) Epigenetic analysis reveals a euchromatic configuration in the FMR1 unmethylated full mutations. Eur J Hum Genet 16:1487–1498PubMedCrossRefGoogle Scholar
  5. 5.
    Naumann A, Hochstein N, Weber S et al (2009) A distinct DNA- methylation boundary in the 5′- upstream sequence of the FMR1 promoter binds nuclear proteins and is lost in fragile X syndrome. Am J Hum Genet 85:606–616PubMedCrossRefGoogle Scholar
  6. 6.
    Coffee B, Zhang F, Warren ST et al (1999) Acetylated histones are associated with FMR1 in normal but not fragile X-syndrome cells. Nat Genet 22:98–101PubMedCrossRefGoogle Scholar
  7. 7.
    Coffee B, Zhang F, Ceman S et al (2002) Histone modifications depict an aberrantly heterochromatinized FMR1 gene in fragile X syndrome. Am J Hum Genet 71:923–932PubMedCrossRefGoogle Scholar
  8. 8.
    Tabolacci E, Pietrobono R, Moscato U et al (2005) Differential epigenetic modifications in the FMR1 gene of the fragile X syndrome after reactivating pharmacological treatments. Eur J Hum Genet 13:641–648PubMedCrossRefGoogle Scholar
  9. 9.
    Chiurazzi P, Pomponi MG, Willemsen R et al (1998) In vitro reactivation of the FMR1 gene involved in fragile X syndrome. Hum Mol Genet 7:109–113PubMedCrossRefGoogle Scholar
  10. 10.
    Chiurazzi P, Pomponi MG, Pietrobono R et al (1999) Synergistic effect of histone hyperacetylation and DNA demethylation in the reactivation of the FMR1 gene. Hum Mol Genet 8:2317–2323PubMedCrossRefGoogle Scholar

Copyright information

© Springer New York 2013

Authors and Affiliations

  • Elisabetta Tabolacci
    • 1
  • Giovanni Neri
    • 1
  1. 1.Facoltà di Medicina e Chirurgia “A. Gemelli”, Istituto di Genetica MedicaUniversità Cattolica del Sacro CuoreRomeItaly

Personalised recommendations