Abstract

This proposal seeks 3 years of support to complete functional analyses of a 50 Mb region of mouse Chromosome 5 comprising nearly 2% of the mouse genome. Under previous funding, mutations were induced by randomly mutagenizing the genome with ethylnitrosourea (ENU), and selecting those on proximal Chr 5 using a breeding scheme that exploited a chromosome inversion called rump-white (Rw). A set of deletion complexes spanning much of the Rw region was created to aid in the genetic analysis of these mutations. Though screens were conducted for several phenotypes, embryonic lethal mutations (total of 34, representing 32 complementation groups) were the largest class recovered. Additionally, two male mutations causing infertility, one causing deafness, and 2 affecting behavior were recovered. The lethal mutations act throughout development, from pre-implantation through birth. The mutant phenotypes include: failure of the inner cell mass to proliferate; abnormal placental formation; gastrulation defects; homeotic-like skeletal transformations; craniofacial abnormalities; and cardiovascular defects. Genetic mapping experiments have localized most of these mutations to relatively small intervals within the Rw region. Thus far, 5 lethals and 1 infertility allele have been cloned. This proposal has two specific aims. The first is to positionally clone the remaining infertility mutation and 20 of the lethal alleles. The second is to complete a gross phenotypic characterization of this lethal mutation set, using analytic methods appropriate for various embryological stages. In combination, these experiments will link the molecular defects to mutant phenotypes, and thereby illuminate genetic mechanisms of normal mammalian development. Many of the uncloned mutations currently map to regions containing none or few known lethal genes, ensuring that several new essential genes or functional elements will be identified. This establishment of phenotype/genotype relationships will pave the way for more detailed investigations by ourselves and the mammalian development community. Overall, these experiments will eventually provide an unbiased glimpse into the functional elements encoded by a representative region of the genome. The project uses the mouse as model to identify important genes affecting embryonic development and fertility in humans. Ultimately, we anticipate this work will assist treatment of certain male infertilities, increase our understanding of the genes required for normal embryonic development, and potentially lead to improved genetic diagnosis of certain birth defects. ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Project (R01)
Project #
2R01HD035984-10A2
Application #
7315530
Study Section
Genomics, Computational Biology and Technology Study Section (GCAT)
Program Officer
Coulombe, James N
Project Start
1997-12-22
Project End
2010-07-31
Budget Start
2007-08-01
Budget End
2008-07-31
Support Year
10
Fiscal Year
2007
Total Cost
$323,476
Indirect Cost

  Institution

Name
Cornell University
Department
Other Basic Sciences
Type
Schools of Veterinary Medicine
DUNS #
872612445
City
Ithaca
State
NY
Country
United States
Zip Code
14850

  Publications

Ching, Yung-Hao; Wilson, Lawriston A; Schimenti, John C (2010) An allele separating skeletal patterning and spermatogonial renewal functions of PLZF. BMC Dev Biol 10:33
Ching, Yung-Hao; Munroe, Robert J; Moran, Jennifer L et al. (2010) High resolution mapping and positional cloning of ENU-induced mutations in the Rw region of mouse chromosome 5. BMC Genet 11:106
Munroe, Robert J; Prabhu, Vinay; Acland, Greg M et al. (2009) Mouse H6 Homeobox 1 (Hmx1) mutations cause cranial abnormalities and reduced body mass. BMC Dev Biol 9:27
Mu, Weipeng; Wang, Wei; Schimenti, John C (2008) An allelic series uncovers novel roles of the BRCT domain-containing protein PTIP in mouse embryonic vascular development. Mol Cell Biol 28:6439-51
Suarez, Susan S; Marquez, Becky; Harris, Tanya P et al. (2007) Different regulatory systems operate in the midpiece and principal piece of the mammalian sperm flagellum. Soc Reprod Fertil Suppl 65:331-4
Howell, Gareth R; Shindo, Mami; Murray, Stephen et al. (2007) Mutation of a ubiquitously expressed mouse transmembrane protein (Tapt1) causes specific skeletal homeotic transformations. Genetics 175:699-707
Harris, Tanya; Marquez, Becky; Suarez, Susan et al. (2007) Sperm motility defects and infertility in male mice with a mutation in Nsun7, a member of the Sun domain-containing family of putative RNA methyltransferases. Biol Reprod 77:376-82
Wilson, Lawriston; Ching, Yung-Hao; Farias, Michael et al. (2005) Random mutagenesis of proximal mouse chromosome 5 uncovers predominantly embryonic lethal mutations. Genome Res 15:1095-105
Symula, Derek J; Zhu, Yiwen; Schimenti, John C et al. (2004) Functional annotation of mouse mutations in embryonic stem cells by use of expression profiling. Mamm Genome 15:1-13
Shima, Naoko; Hartford, Suzanne A; Duffy, Ted et al. (2003) Phenotype-based identification of mouse chromosome instability mutants. Genetics 163:1031-40

Showing the most recent 10 out of 12 publications