Abstract

The last twenty years have witnessed the rapid advance of the application of genetic engineering techniques to increasingly complex organisms: first, single-cell microbial and eukaryotic culture systems; next, plants; and, finally, multi-cellular whole animal systems. The whole animal, as represented by various species of laboratory animals, is generally recognized as an essential tool for medical research. Laboratory animals offer a far closer approximation to the human organism than cell culture systems. Moreover, an understanding of integrative biology (e.g., the developmental and tissue-specific regulation of gene expression) can be achieved only through in vivo, whole animal studies. To this end, the laboratory mouse is presently the most widely used, available, and economical animal model used in biomedical research and, in particular, genetic engineering and transgenic-related research. In addition to the many traditional mutant mouse strains, thousands of additional strains of mice have been created in recent years through transgenic technology. This Core proposal provides a centralized AAALAC- certified resource for the production of pathogen-free transgenic (including DNA microinjection, ES cell transfer and mitochondrial transfer) mouse models. Trained professionals will provide high standards of performance, quality and timely production efficiency. For the individual projects outlined in this program project, this approach means availability of highly specialized services at reasonable costs, maximizing sponsored program dollars and investigator efforts. Furthermore, transgenic and transmitochondrial mice created by DNA microinjection, ES cell transfer, or evolving technologies will be crucial components of this program project.
The specific aims of this Core will be to efficiently create genetically- engineered transgenic (including transmitochondrial and ES cell """"""""knockout"""""""") mice for individual projects utilizing state-of-the-art technologies including: a) established DNA microinjection technology, b) established ES cell transfer procedures, and c) initiation of mitochondrial transfer techniques.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Center for Research Resources (NCRR)
Type
Research Program Projects (P01)
Project #
5P01RR011105-02
Application #
5225934
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
2
Fiscal Year
1996
Total Cost
Indirect Cost

  Publications

Elgavish, Ada; Wood, Philip A; Pinkert, Carl A et al. (2004) Transgenic mouse with human mutant p53 expression in the prostate epithelium. Prostate 61:26-34
Fukuchi, K; Hart, M; Yan, Z et al. (2004) Transgenic mice overexpressing both amyloid beta-protein and perlecan in pancreatic acinar cells. Histol Histopathol 19:845-52
Hart, M; Li, L; Tokunaga, T et al. (2001) Overproduction of perlecan core protein in cultured cells and transgenic mice. J Pathol 194:262-9
Yancey, A L; Watson, H L; Cartner, S C et al. (2001) Gender is a major factor in determining the severity of mycoplasma respiratory disease in mice. Infect Immun 69:2865-71
Kurtz, D M; Tian, L; Gower, B A et al. (2000) Transgenic studies of fatty acid oxidation gene expression in nonobese diabetic mice. J Lipid Res 41:2063-70
Fukuchi, K; Li, L; Hart, M et al. (2000) Accumulation of amyloid-beta protein in exocrine glands of transgenic mice overexpressing a carboxyl terminal portion of amyloid protein precursor. Int J Exp Pathol 81:231-9
Cartner, S C; Lindsey, J R; Gibbs-Erwin, J et al. (1998) Roles of innate and adaptive immunity in respiratory mycoplasmosis. Infect Immun 66:3485-91
Li, L; Perry, R; Wu, J et al. (1998) Polymorphic tetranucleotide repeat site within intron 7 of the beta-amyloid precursor protein gene and its lack of association with Alzheimer's disease. Hum Genet 103:86-9
Fukuchi, K; Pham, D; Hart, M et al. (1998) Amyloid-beta deposition in skeletal muscle of transgenic mice: possible model of inclusion body myopathy. Am J Pathol 153:1687-93
Fukuchi, K; Hart, M; Li, L (1998) Alzheimer's disease and heparan sulfate proteoglycan. Front Biosci 3:d327-37

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