Abstract

The function of the Animal Model Core is to provide complete services in the production and characterization of all forms of transgenic and mutant mice and stem cell lines and to centralize these functions together with other embryo micromanipulation and transfer activities for economies of space and scale. To accomplish this goal, the Core will perform the following: generation, culture, and cytogenetic monitoring of embryonic stem (ES) cell lines; transfection of cloned DNA into ES cells for the production of transgenic and homologously recombined cells; selection of transfected ES cells and injection into preimplantation embryos (8 cell- and blastocyst) to produce ES cell chimeras; injection of cloned DNA into fertilized oocytes for the production of transgenic animals; transfer of transgenic embryos or of transgenic or homologously-recombined ES cell chimeras into pseudopregnant foster females; initial characterization of transgenic and mutant progeny;establishment and maintenance of the initial breeding stock of transgenic and mutant mice; maintenance of breeding stocks of mutant mice imported from elsewhere. All mice used and generated will be housed in the UCSF Transgenic Facility. This facility is a new, shared, multi-user barrier facility constructed inside the UCSF Animal Care Facility for the purpose of studies on transgenic mice. A micromanipulation and ES cell culture station will be established to carry out all technical work required to generate transgenic and mutant mice. Routine cytogenetic monitoring and tests for chimera formation and germ line transmission will be undertaken for all stem cell lines used, and the media and LIF (leukemia inhibitory factor) required for stem cell culture will be routinely tested to determine optimal conditions for stem cell growth. Similarly, monitoring of the media used for preimplantation embryo culture will also be carried out. The personnel of the core will undertake an active program to educate all investigators related to this grant in the approaches required for the construction of transgenic and homologous- recombination """"""""knockout"""""""" mice. When appropriate, the core will work with investigators to develop net approaches to the construction of such animals.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Center Core Grants (P30)
Project #
5P30DK047766-04
Application #
5210843
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
4
Fiscal Year
1996
Total Cost
Indirect Cost

  Publications

Hawgood, Samuel; Ochs, Matthias; Jung, Anja et al. (2002) Sequential targeted deficiency of SP-A and -D leads to progressive alveolar lipoproteinosis and emphysema. Am J Physiol Lung Cell Mol Physiol 283:L1002-10
Lalwani, Anil K; Han, Jay J; Castelein, Caley M et al. (2002) In vitro and in vivo assessment of the ability of adeno-associated virus-brain-derived neurotrophic factor to enhance spiral ganglion cell survival following ototoxic insult. Laryngoscope 112:1325-34
Xu, Z; Jablons, D M; Gruenert, D C (2001) Expression sequence tag-specific full-length cDNA cloning: actin cDNAs. Gene 263:265-72
Gum Jr, J R; Hicks, J W; Gillespie, A M et al. (2001) Mouse intestinal goblet cells expressing SV40 T antigen directed by the MUC2 mucin gene promoter undergo apoptosis upon migration to the villi. Cancer Res 61:3472-9
Colosimo, A; Goncz, K K; Novelli, G et al. (2001) Targeted correction of a defective selectable marker gene in human epithelial cells by small DNA fragments. Mol Ther 3:178-85
Goncz, K K; Colosimo, A; Dallapiccola, B et al. (2001) Expression of DeltaF508 CFTR in normal mouse lung after site-specific modification of CFTR sequences by SFHR. Gene Ther 8:961-5
Colosimo, A; Goncz, K K; Holmes, A R et al. (2000) Transfer and expression of foreign genes in mammalian cells. Biotechniques 29:314-8, 320-2, 324 passim
Camargo, F D; Huey-Louie, D A; Finn, A V et al. (2000) Germline incorporation of a replication-defective adenoviral vector in mice does not alter immune responses to adenoviral vectors. Mol Ther 2:496-504
Hirota, S; de Ilarduya, C T; Barron, L G et al. (1999) Simple mixing device to reproducibly prepare cationic lipid-DNA complexes (lipoplexes). Biotechniques 27:286-90
Holmes, A R; Dohrman, A F; Ellison, A R et al. (1999) Intracellular compartmentalization of DNA fragments in cultured airway epithelial cells mediated by cationic lipids. Pharm Res 16:1020-5

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