Abstract

The objective is to identify and characterize genetic variation in mice for regulatory and structural loci. We have drawn extensively from a diverse sampling of the mouse gene pool by obtaining mice from different geographical regions of the world. Taxonomically, these mice have included house mouse Mus species which are geographically separated but will readily interbreed with laboratory mice. It has also included mouse species trapped in field habitats in Eastern and Western Europe, M. Horbulanus and M spretus, which do not interbreed in the wild but do hybridize with laboratory strains in animal colony conditions. We have also sampled mouse species of the genus Mus which do not interbreed in the field or under laboratory conditions. These resources are currently maintained in breeding colonies at Roswell Park and they have supplied us with an extensive array of genetic variation for gene structure and regulation which is not present among the strains of laboratory mice. We have used resources to identify regulation of gene expression at the level of synthesis and processing of gene products. This proposal describes experimental approaches for extending that work and for characterizing the biochemical and molecular basis of genetic variation for the regulation of glucuronidase expression in subcellular localization and in the kidneys of testosterone treated mice. We are concerned with characterizing the molecular elements involved in gene regulation which act cis. In particular, we would like to known whether developmentally and hormonally regulated genes including, Beta-glucuronidase, RP-2 and Odk, are cis regulated at the level of transcription or RNA stabilization. We have observed substantial differences between Mus species in the hormonal regulation of several genes in mouse kidney. we have proposed experiments to test whether genetic variation is present among Mus species for trans acting regulatory elements and, if so, to characterize the expression of these genes and map them on the mouse gene map. This proposal also extends our use of chemical and X-ray mutagenesis to produce mutations in specific gene products. Experimental approaches are detailed to identify mutations on the X chromosome as well as for autosomal genes. X-chromosome mutations will be recovered for X-chromosome disorders in mice which model disorders of medical concern in humans. A method is proposed for testing mosaic expression of X-chromosome genes in heterozygous females. It provides a simple, economical test which can identify mutational events at up to 100 loci on the X chromosome using a single biochemical assay.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
2R01GM033160-04
Application #
3282529
Study Section
Genetics Study Section (GEN)
Project Start
1983-07-01
Project End
1991-06-30
Budget Start
1986-07-01
Budget End
1987-06-30
Support Year
4
Fiscal Year
1986
Total Cost
Indirect Cost

  Institution

Name
Roswell Park Cancer Institute Corp
Department
Type
DUNS #
City
Buffalo
State
NY
Country
United States
Zip Code
14263

  Publications

Singh, U; Sun, T; Larsson, T et al. (2006) Expression and functional analysis of fibulin-1 (Fbln1) during normal and abnormal placental development of the mouse. Placenta 27:1014-21
Singh, Umashankar; Sun, Tong; Shi, Wei et al. (2005) Expression and functional analysis of genes deregulated in mouse placental overgrowth models: Car2 and Ncam1. Dev Dyn 234:1034-45
Elliott, Rosemary W; Poslinski, Diane; Tabaczynski, Debra et al. (2004) Loci affecting male fertility in hybrids between Mus macedonicus and C57BL/6. Mamm Genome 15:704-10
Elliott, R W; Miller, D R; Pearsall, R S et al. (2001) Genetic analysis of testis weight and fertility in an interspecies hybrid congenic strain for Chromosome X. Mamm Genome 12:45-51
Hemberger, M; Kurz, H; Orth, A et al. (2001) Genetic and developmental analysis of X-inactivation in interspecific hybrid mice suggests a role for the Y chromosome in placental dysplasia. Genetics 157:341-8
Hemberger, M C; Pearsall, R S; Zechner, U et al. (1999) Genetic dissection of X-linked interspecific hybrid placental dysplasia in congenic mouse strains. Genetics 153:383-90
Lueders, K K; Elliott, R W; Marenholz, I et al. (1999) Genomic organization and mapping of the human and mouse neuronal beta2-nicotinic acetylcholine receptor genes. Mamm Genome 10:900-5
LI, W; Elliott, R W; Novak, E K et al. (1999) cDNA sequence and mapping of the mouse Copb gene encoding the beta subunit of the COPI coatomer complex. Somat Cell Mol Genet 25:177-83
Zhao, X F; Colaizzo-Anas, T; Nowak, N J et al. (1998) The mammalian homologue of mago nashi encodes a serum-inducible protein. Genomics 47:319-22
Dal Zotto, L; Quaderi, N A; Elliott, R et al. (1998) The mouse Mid1 gene: implications for the pathogenesis of Opitz syndrome and the evolution of the mammalian pseudoautosomal region. Hum Mol Genet 7:489-99

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