NCI   NIH
Mouse Models of Human Cancers Consortium
Search: 
Site Map
Upcoming Events/Meetings  
Calendar
Sources of Mouse Models  
NCI’s Mouse Repository  Opens in New Window: NCI’s Mouse Repository
Mutant Mouse Regional Resource Centers (MMRRC)  Opens in New Window: Mutant Mouse Regional Resource Centers (MMRRC)
The Jackson Laboratory  Opens in New Window: The Jackson Laboratory
Tools for Mouse Modelers  
Cancer Model Database (caMOD)  Opens in New Window: Cancer Model Database (caMOD)
Cancer Image Database (caIMAGE)  Opens in New Window: Cancer Image Database (caIMAGE)
caELMIR  Opens in New Window: caELMIR
Cancer Array Informatics (caArray)  Opens in New Window: Cancer Array Informatics (caArray)
Cancer Biomedical Informatics Grid (caBIG™)  Opens in New Window: Cancer Biomedical Informatics Grid (caBIG™)
Mouse Genome Informatics (MGI)  Opens in New Window: Mouse Genome Informatics (MGI)
Cancer Genome Anatomy Project (CGAP)  Opens in New Window: Cancer Genome Anatomy Project (CGAP)
Related Links  
NCI Center for Bioinformatics (NCICB)  Opens in New Window: NCI Center for Bioinformatics (NCICB)
Specialized Programs of Research Excellence (SPORE)  Opens in New Window: Specialized Programs of Research Excellence (SPORE)
National Center for Biotechnology Information (NCBI)  Opens in New Window: National Center for Biotechnology Information (NCBI)
The Integrative Cancer Biology Program (ICBP)  Opens in New Window: The Integrative Cancer Biology Program (ICBP)

skip top level navigationHome Mouse Models Experimental Therapeutics Resources MMHCC Communication Bioinformatics Learning Tools  

  Emice  >  MMHCC  >  Organization  >  Members  >  Abstracts  >  Coffey :


Coffey, Robert J, M.D.
MOUSE MODELS OF HUMAN CANCER

MOUSE MODELS OF HUMAN CANCER

PREVENTION AND METASTASIS:  FINAL FRONTIERS IN COLON CANCER

 

Based on our work in the first cycle of the MMHCC, we proposed to address two major remaining frontiers in mouse models of colorectal cancer (CRC) – opportunities afforded by a novel prevention strategy and challenges posed by liver metastasis, the major cause of mortality for individuals with CRC.

 

Project I will elucidate the role of gut flora in the pathogenesis of mouse models of CRC utilizing the gnotobiotic facility at UNC.  Increasing evidence strongly supports the role of the enteric flora in cancer initiation and progression.  We will investigate the role of enteric flora in maintaining GI homeostasis and the role of normal flora and selected pathogens in inducing colon tumors in Smad3 null mice.  We will use our germfree/gnotobiotic facility to test a standardized flora that appears to be pathology neutral, and compare with mice inoculated with Helicobacter hepaticus.  We will also test various mouse colonies showing varying tumor susceptibilities and tumor distributions using a novel enteric flora profiling technique that we have developed.  We propose to capitalize on this unique symbiotic relationship between enteric flora and colonic mucosa by engineering designer flora to crate ‘turbo-biotics,’ probiotic bacteria that have unique characteristics that may afford a novel and safe preventive approach to CRC.  

 

PI:  David Threadgill, Ph.D.

University of North Carolina

 

In Project 2, we will overcome a major obstacle in developing s robust model of CRC with liver metastasis – obstruction of the colonic lumen leading to bleeding and death before the tumor invades and metastasizes.  We will build upon two non-obstructing mouse models of CRC that we have identified – a colony of SMAD3 null mice that develop tumors only in the cecum and carcinogen-treated MOLF mice that develop sessile (flat) colonic tumors.  Utilizing mouse colon cancer cell lines that can be injected into the cecum of syngeneic mice and selected for liver metastasis, we propose bold new selection schemes and a candidate approach; genes that are identified will then be introduced into our two non-obstructing m=models to achieve our stated goal.  Employment of sophisticated imaging technologies available at VUMC will aid in this approach.

 

PI:  Robert Coffey, M.D.

 

In Project 3, we propose to advance progress made during the first cycle of the MMHCC.  Using two classical mouse mutants, we demonstrated iterative use of EGF receptor (EGFR) signaling in intestinal neoplasia, in order to evaluate current and future therapeutic agents targeting the EGFR axis, we propose to humanize mouse EGFR.  This approach will allow us to identify and validate targets of different agents that block the EGFR axis using microarray and unique proteomic capabilities coupled to strong bioinformatics support.  Finally, we are continuing efforts to model pancreatic ductal carcinoma in the mouse.  We have linked EGFR and Notch signaling and propose studies to elucidate roles for perturbed Notch signaling in pancreatic cancer.

 

PI:  Robert Coffey, M.D.

 

Although this proposal is GI-centric, the overarching goals of the bold projects with their underlying provocative hypotheses involve strategies (prevention) and processes (metastasis) central to neoplasia, and, coupled with our unique institutional capabilities, we anticipate productive interactions with other MMHCC and SPORE groups.

 

 

 
skip footer navigation
 CONTACT US PRIVACY NOTICE DISCLAIMER ACCESSIBILITY APPLICATION SUPPORT  
National Cancer Institute Department of Health and Human Services National Institutes of Health FirstGov.gov