Abstract

Funds are requested in support of travel and/or registration costs for scientists attending the Genetic Toxicology Gordon Research Conference to be held at Oxford University (Queens College) from August 1-6, 1999. In the broadest terms, the field of Genetic Toxicology is dedicated to understanding how genetic damage occurs and how it can be prevented. Genetic Toxicology thus relies on information drawn from a wide variety of disciplines, including cell/molecular/structural biology, biochemistry, DNA repair, mutagenesis, recombination, meiosis, carcinogenesis, risk evaluation, and molecular epidemiology. This conference is designed to bring together researchers from each of these disciplines. The participants of this bi-annual conference are expected to number about 130 and are drawn from basic scientists in academia, industry, government, and federal regulatory agencies from around the world. The introductory session will be comprised of three special lectures aimed at providing a historical as well as a current perspective to the field of Genetic Toxicology; the highly distinguished lecturers are John Cairns, Bernard Strauss and Evelyn Witkin. Each of the following eight sessions will have a session chair, speakers and a discussion leader, all of whom are experts in some of the aforementioned disciplines. The sessions are designed not only to facilitate the dissemination of the most recent research findings relevant to Genetic Toxicology, but also to stimulate extensive and relevant discussion among the entire audience. Briefly, the sessions will cover the following areas: (i) Structural aspects of protein:DNA interactions that influence genotoxicity; (ii) Interactions of the DNA mismatch repair pathway with DNA base lesions; (iii) Transcription coupled BER and NER; (iv) DNA recombination; (v) Meiosis: crossover between basic biology and risk evaluation; (vi) Signal transduction and inducible responses to genotoxic agents; (vii) Genome alterations: adducts, and mutations; (viii) Genetic susceptibility and molecular epidemiology. In addition, there will be four Poster Sessions for all conference participants to share details of their latest research in any area of Genetic Toxicology. Together, these sessions are designed to address questions related to Genetic Toxicology ranging from the most basic discipline of structural biology using purified proteins and DNA, through to human population-based studies. Such human population-based studies must be fueled by information gleaned from all of the other disciplines that contribute to our understanding of how genomes are damaged, and our understanding of how living organisms endeavor to prevent such damage.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Conference (R13)
Project #
1R13ES010067-01
Application #
2910998
Study Section
Special Emphasis Panel (ZES1-JPM-B (R5))
Program Officer
Grotzinger, Karen R
Project Start
1999-08-01
Project End
1999-12-31
Budget Start
1999-08-01
Budget End
1999-12-31
Support Year
1
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
Gordon Research Conferences
Department
Type
DUNS #
City
West Kingston
State
RI
Country
United States
Zip Code
02892

  Publications

Russell, Liane B; Hunsicker, Patricia R; Russell, William L (2007) Comparison of the genetic effects of equimolar doses of ENU and MNU: while the chemicals differ dramatically in their mutagenicity in stem-cell spermatogonia, both elicit very high mutation rates in differentiating spermatogonia. Mutat Res 616:181-95
Selby, Paul B; Earhart, Vicki S; Raymer, G Douglas (2005) The influence of dominant lethal mutations on litter size and body weight and the consequent impact on transgenerational carcinogenesis. Mutat Res 578:382-94
Selby, Paul B; Earhart, Vicki S; Garrison, Edna M et al. (2004) Description of first germinal mosaic mutation identified in dominant skeletal mutation experiments and considerations about how to deal with this kind of spontaneous mutation in analyses. Mutat Res 545:109-15
Michaud, E J; van Vugt, M J; Bultman, S J et al. (1994) Differential expression of a new dominant agouti allele (Aiapy) is correlated with methylation state and is influenced by parental lineage. Genes Dev 8:1463-72
Michaud, E J; Bultman, S J; Klebig, M L et al. (1994) A molecular model for the genetic and phenotypic characteristics of the mouse lethal yellow (Ay) mutation. Proc Natl Acad Sci U S A 91:2562-6
Russell, L B (1994) Role of mouse germ-cell mutagenesis in understanding genetic risk and in generating mutations that are prime tools for studies in modern biology. Environ Mol Mutagen 23 Suppl 24:23-9
Metallinos, D L; Oppenheimer, A J; Rinchik, E M et al. (1994) Fine structure mapping and deletion analysis of the murine piebald locus. Genetics 136:217-23
Moyer, J H; Lee-Tischler, M J; Kwon, H Y et al. (1994) Candidate gene associated with a mutation causing recessive polycystic kidney disease in mice. Science 264:1329-33
Kwon, H Y; Bultman, S J; Loffler, C et al. (1994) Molecular structure and chromosomal mapping of the human homolog of the agouti gene. Proc Natl Acad Sci U S A 91:9760-4
Bultman, S J; Klebig, M L; Michaud, E J et al. (1994) Molecular analysis of reverse mutations from nonagouti (a) to black-and-tan (a(t)) and white-bellied agouti (Aw) reveals alternative forms of agouti transcripts. Genes Dev 8:481-90

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