Abstract

The long-term goal of this project is to elucidate the natural function of FMRP and related gene products, with emphasis on exploring the proposed roles of these proteins as factors contributing to the regulation of gene expression of eukaryotic cells. In particular, we plan to study both expression and function of Scp160p, a candidate homologue of FMRP, in the genetically and biochemically amenable yeast Saccharomyces cerevisiae. In addition, we will use yeast as a model system in which to express and study wild-type and mutant forms of vertebrate FMRP. Current data derived both in vitro and in vivo from studies of mammalian cells indicate that both FMRP and the FMRP-related FXR proteins are ribonucleoproteins that associate with ribosomes and ostensibly mediate the metabolism, transport, stability, and/or translation of specific messages in cells. What remains unknown, however, is the specific impact of FMRP function on these biological pathways, the mechanism by which this impact occurs, and the identities and relationships of gene products subject to FMRP-mediated regulation. We propose to address these questions with regard to both yeast Scp160p and vertebrate FMRP by accomplishing the following specific objectives"""""""" (1) to characterize Scp160p subcellular localization in yeast both biochemically and microscopically and, coupled with deletion and mutagenesis protocols, to initiate structure/function studies of this protein; (2) to study the phenotypes of both loss and overexpression of Scp160p in yeast; 93) to identify biochemically both protein and RNA species with which Scp160p associated in vivo, as well as to identify genetically other loci in yeast whose products interact, either physically or functionally, with Scp160p, and (4) to express vertebrate FMRP proteins in yeast, to study both the localization and macromolecular interactions of these proteins with endogenous yeast proteins and/or FNAs, and to probe the capacity of these vertebrate FMRP sequences to complement deletion of the corresponding yeast endogenous sequences. Combined, these studies should provide information that is meaningful not only in terms of the basic science of expression and function of FMRP-like sequences in yeast, but also because insights gained from this work should provide a useful framework for interpreting the potentially much more complex data derived from studies of FMRP function in mammalian cells and tissues.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Program Projects (P01)
Project #
1P01HD035576-01
Application #
6241407
Study Section
Project Start
1997-09-10
Project End
1998-07-31
Budget Start
1996-10-01
Budget End
1997-09-30
Support Year
1
Fiscal Year
1997
Total Cost
Indirect Cost

  Institution

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

  Publications

Spath, Marian A; Feuth, Ton B; Smits, Arie P T et al. (2011) Predictors and risk model development for menopausal age in fragile X premutation carriers. Genet Med 13:643-50
Spath, M A; Feuth, T B; Allen, E G et al. (2011) Intra-individual stability over time of standardized anti-Mullerian hormone in FMR1 premutation carriers. Hum Reprod 26:2185-91
Wang, Houping; Dictenberg, Jason B; Ku, Li et al. (2008) Dynamic association of the fragile X mental retardation protein as a messenger ribonucleoprotein between microtubules and polyribosomes. Mol Biol Cell 19:105-14
Allen, E G; Sullivan, A K; Marcus, M et al. (2007) Examination of reproductive aging milestones among women who carry the FMR1 premutation. Hum Reprod 22:2142-52
Anido, Aimee; Carlson, Lisa M; Sherman, Stephanie L (2007) Attitudes toward fragile X mutation carrier testing from women identified in a general population survey. J Genet Couns 16:97-104
Smith, Karen T; Nicholls, Robert D; Reines, Daniel (2006) The gene encoding the fragile X RNA-binding protein is controlled by nuclear respiratory factor 2 and the CREB family of transcription factors. Nucleic Acids Res 34:1205-15
Garber, Kathryn; Smith, Karen T; Reines, Danny et al. (2006) Transcription, translation and fragile X syndrome. Curr Opin Genet Dev 16:270-5
Li, Wen; Xia, Jin-tang; Feng, Yue (2006) Microtubule stability and MAP1B upregulation control neuritogenesis in CAD cells. Acta Pharmacol Sin 27:1119-26
Anido, Aimee; Carlson, Lisa M; Taft, Lisa et al. (2005) Women's attitudes toward testing for fragile X carrier status: a qualitative analysis. J Genet Couns 14:295-306
Nakamoto, Mika; Jin, Peng; O'Donnell, William T et al. (2005) Physiological identification of human transcripts translationally regulated by a specific microRNA. Hum Mol Genet 14:3813-21

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