Abstract

The overall aim of this application is to define parameters in trinucleotide repeats found in humans which confer instability and predisposition to disease. Mutant trinucleotide repeats have been implicated in seven human genetic disorders with neuromuscular effects to date. One of the hallmarks of these mutations is extreme mutability, i.e. the mutations confer hypermutability onto themselves. Mutations of the repeats are involve in altering the severity an/or onset of the disease. Therefore, the mechanisms involved in generating these novel mutations are quite relevant to the study of these disorders. This effort will test the hypothesis that instability in the CCGG repeat found at the FMR1 gene involved in fragile X syndrome is intrinsic to the repeat itself. The alternative hypothesis that other closely linked sequences are involved will also be tested. This will be accomplished through the following aims: 1) Identification of the molecular basis of meiotic instability using empirical studies of stable and unstable repeats found in human families. 2) Development of a model system capable of testing repeat elements for stability. 30 Study of similar repeats in the human and other species' genomes in order to compare and contrast these without the human FMRI repeat. 4) Study of the methylation of CGG repeats in and its role in stability of the repeat during early development. 5) Extension of these studies to other trinucleotide repeats, particularly the CAG repeat found to be unstable in several other human genetic disorders. 6) Provision of medically relevant samples to collaborators interested in the study of trinucleotide repeats using a variety of biochemical and enzymatic measures. Determination of the types of repeats (or other nearby sequences) involved in instability will provide for more accurate forecasting of the behavior of these elements and should allow for improved diagnostic testing. In addition, this information in combination with the studies of the other members of this program project will provide significant insight into the types of replication and/or repair errors underlying the behavior of these sequences. These data will provide new understanding of the basic enzymology and biochemistry underpinning DNA replication and repair in humans, with likely consequences for somatic mutation as well.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Program Projects (P01)
Project #
5P01GM052982-05
Application #
6204270
Study Section
Project Start
1999-07-01
Project End
2001-06-30
Budget Start
1997-10-01
Budget End
1998-09-30
Support Year
5
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
Texas Agrilife Research
Department
Type
DUNS #
110521739
City
College Station
State
TX
Country
United States
Zip Code
77843

  Publications

Vetcher, Alexandre A; Wells, Robert D (2004) Sticky DNA formation in vivo alters the plasmid dimer/monomer ratio. J Biol Chem 279:6434-43
Meservy, James L; Sargent, R Geoffrey; Iyer, Ravi R et al. (2003) Long CTG tracts from the myotonic dystrophy gene induce deletions and rearrangements during recombination at the APRT locus in CHO cells. Mol Cell Biol 23:3152-62
Napierala, Marek; Parniewski, Pawel; Pluciennik, Anna et al. (2002) Long CTG.CAG repeat sequences markedly stimulate intramolecular recombination. J Biol Chem 277:34087-100
Vetcher, Alexandre A; Napierala, Marek; Wells, Robert D (2002) Sticky DNA: effect of the polypurine.polypyrimidine sequence. J Biol Chem 277:39228-34
Pluciennik, Anna; Iyer, Ravi R; Napierala, Marek et al. (2002) Long CTG.CAG repeats from myotonic dystrophy are preferred sites for intermolecular recombination. J Biol Chem 277:34074-86
Peier, Andrea M; Nelson, David L (2002) Instability of a premutation-sized CGG repeat in FMR1 YAC transgenic mice. Genomics 80:423-32
Vetcher, Alexandre A; Napierala, Marek; Iyer, Ravi R et al. (2002) Sticky DNA, a long GAA.GAA.TTC triplex that is formed intramolecularly, in the sequence of intron 1 of the frataxin gene. J Biol Chem 277:39217-27
Tomita, Nobuyuki; Fujita, Ryo; Kurihara, Daichi et al. (2002) Effects of triplet repeat sequences on nucleosome positioning and gene expression in yeast minichromosomes. Nucleic Acids Res Suppl :231-2
Sakamoto, N; Larson, J E; Iyer, R R et al. (2001) GGA*TCC-interrupted triplets in long GAA*TTC repeats inhibit the formation of triplex and sticky DNA structures, alleviate transcription inhibition, and reduce genetic instabilities. J Biol Chem 276:27178-87
Bacolla, A; Pradhan, S; Larson, J E et al. (2001) Recombinant human DNA (cytosine-5) methyltransferase. III. Allosteric control, reaction order, and influence of plasmid topology and triplet repeat length on methylation of the fragile X CGG.CCG sequence. J Biol Chem 276:18605-13

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