Abstract

The overall goal of these proposed studies is to determine the genetic significance and molecular basis for instability of common fragile sites. Common fragile sites are specific and constant regions on chromosomes that appear as gaps or breaks when DNA replication is perturbed, and which display a number of characteristics of unstable and highly recombinogenic DNA in vitro. Only one common fragile site, FRA3B at 3p14.2, has been investigated on the molecular level, and recent data strongly suggests that this instability is also seen in vivo. This fragile site extends over a large region of at least 200 kb. The mechanism of the fragility remains unknown but does not appear to be associated with CCG repeat expansion as are other cloned fragile sites. FRA3B is now known to lie within the FHIT gene. This gene has been shown to be highly unstable and contain deletions in a number of tumors and tumor cell lines, and as a result, FHIT has been proposed to be a tumor suppressor gene. Dr. Glover suggests that FRA3B is mechanistically associated with, or causes, this instability. The fact that FRA3B is associated with a highly mutable gene in cancer leads to the hypothesis that other common fragile sites may also be associated with genes, and that these fragile site regions and associated genes may also show a high rate of instability in tumor cells. The test of this hypothesis, additional studies on the mechanisms responsible for fragility and studies on the evolutionary aspects of common fragile sites are the major aims of this proposal. The P.I. proposes to clone and characterize additional common fragile sites, determine if they are associated with genes and if they are unstable in tumor cells. He will investigate the mouse Fhit gene for similar instability in tumors and presence of a fragile site as one test of the hypothesis that deletions in the FHIT gene are caused by FRA3B and to study the significance of FHIT deletions in cancer. To study the mechanisms of instability, Dr. Glover will analyze and compare sequences form new fragile site regions and will also investigate the influence of p53 and DNA repair/replication pathway mutations on fragile site expression and genome instability at fragile site loci. In addition, the evolution of specific common fragile sites will be traced to determine if they are conserved or if sequences critical for expression have diverged, and to explore if they are involved in chromosome rearrangements during evolution.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA043222-14
Application #
6149954
Study Section
Mammalian Genetics Study Section (MGN)
Program Officer
Pelroy, Richard
Project Start
1986-07-01
Project End
2003-01-31
Budget Start
2000-02-01
Budget End
2001-01-31
Support Year
14
Fiscal Year
2000
Total Cost
$265,486
Indirect Cost

  Institution

Name
University of Michigan Ann Arbor
Department
Pediatrics
Type
Schools of Medicine
DUNS #
791277940
City
Ann Arbor
State
MI
Country
United States
Zip Code
48109

  Publications

Arlt, Martin F; Glover, Thomas W (2010) Inhibition of topoisomerase I prevents chromosome breakage at common fragile sites. DNA Repair (Amst) 9:678-89
Ragland, Ryan L; Arlt, Martin F; Hughes, Elizabeth D et al. (2009) Mice hypomorphic for Atr have increased DNA damage and abnormal checkpoint response. Mamm Genome 20:375-85
Howlett, Niall G; Harney, Julie A; Rego, Meghan A et al. (2009) Functional interaction between the Fanconi Anemia D2 protein and proliferating cell nuclear antigen (PCNA) via a conserved putative PCNA interaction motif. J Biol Chem 284:28935-42
Arlt, Martin F; Mulle, Jennifer G; Schaibley, Valerie M et al. (2009) Replication stress induces genome-wide copy number changes in human cells that resemble polymorphic and pathogenic variants. Am J Hum Genet 84:339-50
Ragland, Ryan L; Glynn, Michael W; Arlt, Martin F et al. (2008) Stably transfected common fragile site sequences exhibit instability at ectopic sites. Genes Chromosomes Cancer 47:860-72
Durkin, Sandra G; Ragland, Ryan L; Arlt, Martin F et al. (2008) Replication stress induces tumor-like microdeletions in FHIT/FRA3B. Proc Natl Acad Sci U S A 105:246-51
Durkin, Sandra G; Glover, Thomas W (2007) Chromosome fragile sites. Annu Rev Genet 41:169-92
Durkin, S G; Arlt, M F; Howlett, N G et al. (2006) Depletion of CHK1, but not CHK2, induces chromosomal instability and breaks at common fragile sites. Oncogene 25:4381-8
Miller, C T; Lin, L; Casper, A M et al. (2006) Genomic amplification of MET with boundaries within fragile site FRA7G and upregulation of MET pathways in esophageal adenocarcinoma. Oncogene 25:409-18
Glover, Thomas W (2006) Common fragile sites. Cancer Lett 232:4-12

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