Abstract

The Animal Models Core (AMC) will support all of the research projects in the program by providing thenecessary genetically modified mice and producing low-passage in vivo human gastro-intestinal cancerexplants in mice. One mission of the AMC will be to maintain mice for long-term studies to evaluatepredisposition to cancer. A second mission of the AMC will be maintaining stocks of the genetically modifiedstrains (e.g., elf, eif/Smad4, Smad4, Smad3, Cdk4-R24C mutant, cdk4 null mutant, htert knockout), and tobreed these strains together to produce fetuses of double and triple mutant homozygous genotypes. Workingwith the Tissue Core B, these fetuses will be used as a source of embryonic fibroblasts and tumor cells bythe projects. Pups with the desired double or triple mutant genotypes will constitute a large fraction of theprogeny. To provide a continuous supply in support of the research projects a large amount of breeding,coupled with genotype analysis to identify the appropriate individuals will be required. A third mission of theAMC will be to provide synergy between the clinicians and projects testing anti-cancer drug therapies. Thissynergy will be in the form of producing, and providing husbandry of mice harboring genetic backgroundspredisposed to making tumors or nude mice xenografted with human tumor tissues for propagating lowpassagetumors. All mice will be produced and housed under barrier conditions that ensure continuingspecific pathogen free status, Centralization of the production and care of these mice under the AMC willlimit the number of individuals handling the animals, thereby further safeguarding their health. Moreover, bycentralizing the production and dispensation of these genetically valuable animals, the animal core will beable to coordinate usage among the different projects, avoid wastage, and achieve an economy of scale thatwill permit these studies to be completed at less expense than if undertaken separately. A final mission ofthe AMC will be to serve as a synergistic hub for all projects and cores.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
1P01CA130821-01A1
Application #
7534179
Study Section
Special Emphasis Panel (ZCA1-RPRB-O (M1))
Project Start
2008-05-01
Project End
2013-08-31
Budget Start
2008-09-10
Budget End
2009-08-31
Support Year
1
Fiscal Year
2008
Total Cost
$124,532
Indirect Cost

  Institution

Name
Georgetown University
Department
Type
DUNS #
049515844
City
Washington
State
DC
Country
United States
Zip Code
20057

  Publications

Korkut, Anil; Zaidi, Sobia; Kanchi, Rupa S et al. (2018) A Pan-Cancer Analysis Reveals High-Frequency Genetic Alterations in Mediators of Signaling by the TGF-? Superfamily. Cell Syst 7:422-437.e7
Chen, Jian; Zaidi, Sobia; Rao, Shuyun et al. (2018) Analysis of Genomes and Transcriptomes of Hepatocellular Carcinomas Identifies Mutations and Gene Expression Changes in the Transforming Growth Factor-? Pathway. Gastroenterology 154:195-210
Lin, Shu-Hong; Raju, Gottumukkala S; Huff, Chad et al. (2018) The somatic mutation landscape of premalignant colorectal adenoma. Gut 67:1299-1305
Rao, Shuyun; Zaidi, Sobia; Banerjee, Jaideep et al. (2017) Transforming growth factor-? in liver cancer stem cells and regeneration. Hepatol Commun 1:477-493
Zhou, Xin; Patel, Darshan; Sen, Sabyasachi et al. (2017) Poly-ADP-ribose polymerase inhibition enhances ischemic and diabetic wound healing by promoting angiogenesis. J Vasc Surg 65:1161-1169
Gu, Shoujun; Nguyen, Bao-Ngoc; Rao, Shuyun et al. (2017) Alcohol, stem cells and cancer. Genes Cancer 8:695-700
Chen, Jian; Shukla, Vivek; Farci, Patrizia et al. (2017) Loss of the transforming growth factor-? effector ?2-Spectrin promotes genomic instability. Hepatology 65:678-693
Shin, Joshua; Mishra, Viveka; Glasgow, Eric et al. (2017) PRAJA is overexpressed in glioblastoma and contributes to neural precursor development. Genes Cancer 8:640-649
Long, Yin; Sanchez-Espiridion, Beatriz; Lin, Moubin et al. (2017) Global and targeted serum metabolic profiling of colorectal cancer progression. Cancer 123:4066-4074
Mitra, Abhisek; Yan, Jun; Xia, Xueqing et al. (2017) IL6-mediated inflammatory loop reprograms normal to epithelial-mesenchymal transition+ metastatic cancer stem cells in preneoplastic liver of transforming growth factor beta-deficient ?2-spectrin+/- mice. Hepatology 65:1222-1236

Showing the most recent 10 out of 139 publications