Abstract

Nonrandom chromosomal rearrangements are characteristic of human malignant diseases. Experimental evidence obtained recently indicate that the genes located at the breakpoints of the specific rearrangements play an integral role in tumorigenesis. Another factor that has added to the interest in cancer-specific abnormalities is the recent recognition of the remarkable concordance between the breakpoints noted in the nonrandom abnormalities in human tumors, and the recognized chromosomal fragile sites. The subsequent identification of several individuals with malignant diseases characterized by specific abnormalities who were also carriers of a rare fragile site at that chromosomal breakpoint, the observation that expression of fragile sites can mediate chromosomal rearrangements, and the observation that cancer patients express common fragile sites at an elevated level suggest that fragile sites may act as predisposing factors for chromosomal rearrangements in human neoplasia. At present, there are 143 recognized fragile sites (124 of these are the common fragile sites) and 134 cancer- specific breakpoints. An objective of this proposal is to address some of the questions that currently exist regarding the potential role of fragile sites as predisposing factors to malignancy by examining the intraindividual expression of common fragile sites in cancer patients, and by determining whether elevated expression of these sites is a general phenomenon in cancer patients that is induced by a variety of chemical agents. These studies will provide data regarding the frequency of fragile sites in cancer patients, the relationship of specific sites to the chromosomal breakpoints noted in the malignant cells of individual patients, and the role of fragile sites as predisposing factors to neoplasms. Analysis of family members of patients will enable us to examine some of the genetic factors affecting the expression of common fragile sites. Another objective of this proposal is to use several molecular approaches to isolate the DNA sequences located at several fragile sites. Using the cloned sequences, we will examine the relationship of fragile sites and chromosomal breakpoints in cancer cells and begin to study, at the molecular level, the biological behavior of fragile sites, including their propensity for involvement in chromosome rearrangements.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA041644-05
Application #
3182381
Study Section
Pathology B Study Section (PTHB)
Project Start
1986-01-01
Project End
1991-12-31
Budget Start
1990-01-01
Budget End
1990-12-31
Support Year
5
Fiscal Year
1990
Total Cost
Indirect Cost

  Institution

Name
University of Chicago
Department
Type
Schools of Medicine
DUNS #
225410919
City
Chicago
State
IL
Country
United States
Zip Code
60637

  Publications

Lubelsky, Yoav; Sasaki, Takayo; Kuipers, Marjorie A et al. (2011) Pre-replication complex proteins assemble at regions of low nucleosome occupancy within the Chinese hamster dihydrofolate reductase initiation zone. Nucleic Acids Res 39:3141-55
Palakodeti, Aparna; Lucas, Isabelle; Jiang, Yanwen et al. (2010) Impaired replication dynamics at the FRA3B common fragile site. Hum Mol Genet 19:99-110
Jiang, Yanwen; Lucas, Isabelle; Young, David J et al. (2009) Common fragile sites are characterized by histone hypoacetylation. Hum Mol Genet 18:4501-12
Lucas, Isabelle; Palakodeti, Aparna; Jiang, Yanwen et al. (2007) High-throughput mapping of origins of replication in human cells. EMBO Rep 8:770-7
Palakodeti, Aparna; Han, Yu; Jiang, Yanwen et al. (2004) The role of late/slow replication of the FRA16D in common fragile site induction. Genes Chromosomes Cancer 39:71-6
Corbin, Shantel; Neilly, Mary E; Espinosa 3rd, Rafael et al. (2002) Identification of unstable sequences within the common fragile site at 3p14.2: implications for the mechanism of deletions within fragile histidine triad gene/common fragile site at 3p14.2 in tumors. Cancer Res 62:3477-84
Le Beau, M M; Rassool, F V; Neilly, M E et al. (1998) Replication of a common fragile site, FRA3B, occurs late in S phase and is delayed further upon induction: implications for the mechanism of fragile site induction. Hum Mol Genet 7:755-61
Ong, S T; Fong, K M; Bader, S A et al. (1997) Precise localization of the FHIT gene to the common fragile site at 3p14.2 (FRA3B) and characterization of homozygous deletions within FRA3B that affect FHIT transcription in tumor cell lines. Genes Chromosomes Cancer 20:16-23
Rassool, F V; Le Beau, M M; Shen, M L et al. (1996) Direct cloning of DNA sequences from the common fragile site region at chromosome band 3p14.2. Genomics 35:109-17
Vaxillaire, M; Vionnet, N; Vigouroux, C et al. (1994) Search for a third susceptibility gene for maturity-onset diabetes of the young. Studies with eleven candidate genes. Diabetes 43:389-95

Showing the most recent 10 out of 14 publications