Abstract

Fragile X syndrome is a frequent cause of mental retardation that is inherited as an X-linked dominant with reduced penetrance. The mutational change in nearly all affected patients is the unstable expansion of a CGC trinucleotide repeat in the 5' untranslated region of the FMRI gene. This repeat is normally polymorphic in length and content, exhibiting a mode of 30 cryptic repeats in the normal population, but the triplet is found in excess of approximately 230 repeats in affected patients, often approaching 1,000 copies. Male, and most female, carriers have a FMRI premutation with an intermediate number of repeats, between about 60 and 200 triplets. In most penetrant males with full mutation alleles containing >230 repeats, the FMRI gene is abnormally methylated and late replicating. In such a state, the lengthy CGG repeat is believed to constitute the chromosomal fragile site. As a consequence, the FMRI gene is transcriptionally repressed in full mutation patients and the absence of the encoded protein, FMRP, a selective RNA-binding protein, is responsible for the clinical phenotype. Much of the understanding of this previously quite puzzling disorder emerged in the past 4 years, in part due to research supported under this award. Proposed below is a research program to continue our studies, initiated over a decade ago, to more fully understand this syndrome. We plan three broad specific aims. We will characterize the FMRI repeat in order to more fully understand molecular influences over its stability and evolution. We will continue our characterization of the FMR protein, absent in fragile X syndrome, with the hope that understanding its normal function will give insight into the pathophysiology of fragile X syndrome and human cognition. Finally, we will continue development of clinically useful diagnostic tools for this syndrome, in particular development of ELISA methods to rapidly and accurately quantitate FMRP. We will measure FMRP in women with the full fragile X mutation, who exhibit incomplete penetrance and extremely broad expressivity. Thus, the goal of this proposal is to capitalize upon the successful positional cloning of the FMRI gene and now use it as a molecular reagent to explore the mechanisms and consequences of the remarkable trinucleotide repeat expansion at the fragile X site.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Method to Extend Research in Time (MERIT) Award (R37)
Project #
5R37HD020521-12
Application #
2392363
Study Section
Special Emphasis Panel (ZRG2-GNM (Q2))
Project Start
1996-04-29
Project End
2001-03-31
Budget Start
1997-04-01
Budget End
1998-03-31
Support Year
12
Fiscal Year
1997
Total Cost
Indirect Cost

  Institution

Name
Emory University
Department
Biochemistry
Type
Schools of Medicine
DUNS #
042250712
City
Atlanta
State
GA
Country
United States
Zip Code
30322

  Publications

Alpatov, Roman; Lesch, Bluma J; Nakamoto-Kinoshita, Mika et al. (2014) A chromatin-dependent role of the fragile X mental retardation protein FMRP in the DNA damage response. Cell 157:869-81
Zhu, Gengzhen; Li, Yujing; Zhu, Fei et al. (2014) Coordination of engineered factors with TET1/2 promotes early-stage epigenetic modification during somatic cell reprogramming. Stem Cell Reports 2:253-61
Nelson, David L; Orr, Harry T; Warren, Stephen T (2013) The unstable repeats--three evolving faces of neurological disease. Neuron 77:825-43
Wang, Tao; Bray, Steven M; Warren, Stephen T (2012) New perspectives on the biology of fragile X syndrome. Curr Opin Genet Dev 22:256-63
Santoro, Michael R; Bray, Steven M; Warren, Stephen T (2012) Molecular mechanisms of fragile X syndrome: a twenty-year perspective. Annu Rev Pathol 7:219-45
Henderson, Christina; Wijetunge, Lasani; Kinoshita, Mika Nakamoto et al. (2012) Reversal of disease-related pathologies in the fragile X mouse model by selective activation of GABAB receptors with arbaclofen. Sci Transl Med 4:152ra128
Muddashetty, Ravi S; Nalavadi, Vijayalaxmi C; Gross, Christina et al. (2011) Reversible inhibition of PSD-95 mRNA translation by miR-125a, FMRP phosphorylation, and mGluR signaling. Mol Cell 42:673-88
Gross, Christina; Nakamoto, Mika; Yao, Xiaodi et al. (2010) Excess phosphoinositide 3-kinase subunit synthesis and activity as a novel therapeutic target in fragile X syndrome. J Neurosci 30:10624-38
Collins, Stephen C; Bray, Steven M; Suhl, Joshua A et al. (2010) Identification of novel FMR1 variants by massively parallel sequencing in developmentally delayed males. Am J Med Genet A 152A:2512-20
Collins, Stephen C; Coffee, Brad; Benke, Paul J et al. (2010) Array-based FMR1 sequencing and deletion analysis in patients with a fragile X syndrome-like phenotype. PLoS One 5:e9476

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