Abstract

State the application's broad, long-term objectives and specific aims, making reference to the health relatedness of the project. Describe concisely the researchdesign and methods for achieving these goals. Avoid summariesof past accomplishmentsand the use of the first person. Thisabstract is meant to serve as a succinct and accurate description of the proposed work when separated from the application. If the application is funded, this description, as is, will become public information. Therefore, do not include proprietary/confidential information. DO NOT EXCEED THE SPACE PROVIDED. The importance of genetically-engineered mice (GEM) as models of human health and disease has been unequivocally demonstrated. Because of the importance of GEM in biomedical research, the numbers of GEM lines have grown exponentially over the last five years; this astronomical growth is predicted to continue. Recognizing the scientific importance of sharing mice among investigators, the NIH developed a mouse sharing policy which states that mouse lines generated with the aid of NIH funding must be distributed and shared with the scientific community. To accomplish this goal, the NIH funded the establishment of four regional Mutant Mouse Resource and Research Centers (MMRRCs) in 1999 and 2000. This application is a competitive renewal for the Missouri/Harlan (M/H) MMRRC.
Specific Aims of the proposal are: (1) To improve the efficiencies of the MMRRC service functions while continuing to provide the scientific community with a mutant mouse repository and distribution center of the highest quality. To accomplish this, we will employ state-of-the-art cryopreservationand reanimation (reestablishment of lines after cryopreservation) technologies, such as intracytoplasmicsperm injection (ICSI), nuclear transfer (NT) ovarian tissue (OT) transplantation (OTT) and injection of NT derived embryonic stem cells (ntES cells) into tetraploid embryos (ntES/4N). Using these approaches we will be able to more efficiently import, cryopreserve and reanimate lines at a cost approximately 10% of current, traditional embryo cryopreservation based approaches. (2) To conduct research aimed at increasing the value of the MMRRC. Research will include projects aimed at improving assisted reproductive technologies (ARTs) used for reanimation of mouse lines, development of biosensors for detection of pathogens and health surveillance of mutant mouse colonies, and development of new genetic and ARTs that will revolutionize the speed and efficiency with which congenic strains of mice are made. The proposed approach to the operation of the M/H MMRRC represents a new paradigm for mouse repositories. Recognizing the continued exponential growth of GEM, a new paradigm is mandatory; existing mouse resource centers simply cannot archive all of the important mouse lines using traditional methodology. Furthermore, the proposed research projects will result in even greater efficiencies for the MMRRC and the development of newtechnologies useful to the entire scientific community. PERFORMANCE SITE(S) (organization, city, state) University of Missouri-Columbia 1600E. Rollins Columbia, MO 65211 KEY PERSONNEL. See instructions. Use continuation pages as needed to provide the required information in the format shown below. Start with Principal Investigator. List all other key personnel in alphabetical order, last name first. Name Organization Role on Project John K. Critser University of Missouri-Columbia Co-Pi Lela K. Riley University of Missouri-Columbia Co-Pi Robert Russell Harlan Sprague Dawley Co-Pi (Subcontract) Craig Franklin University of Missouri-Columbia Co-l Beth Bauer University of Missouri-Columbia Co-l Elizabeth Bryda University of Missouri-Columbia Co-l Shubra Gangapadahyay University of Missouri-Columbia Co-l Sheila Grant University of Missouri-Columbia Co-l Tom Davis Harlan Sprague Dawley Co-l (Subcontract) Jack R. McGinley Harlan Sprague Dawley Co-l (Subcontract) Keith Latham Temple University, School of Medicine Consultant Andras Nagy University of Toronto Consultant Kevin Eggan Harvard University Consultant Disclosure PermissionStatement. Applicable to SBIR/STTR Only. See instructions. Q Yes CH No PHS 398 (Rev. 05/01) Page _2 Form Page 2 Principal Investigator/Program Director (Last,first, middle): Critser. John K. and Rjlev. Lela K. The name of the principal investigator/program director must be provided at the top of each printed page and each continuation page. RESEARCH GRANT

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Center for Research Resources (NCRR)
Type
Animal (Mammalian and Nonmammalian) Model, and Animal and Biological Materials Resource Cooperative Agreements (U42)
Project #
3U42RR014821-07S2
Application #
7268164
Study Section
Special Emphasis Panel (ZRR1)
Program Officer
Mirochnitchenko, Oleg
Project Start
2000-05-01
Project End
2010-04-30
Budget Start
2006-08-08
Budget End
2007-04-30
Support Year
7
Fiscal Year
2006
Total Cost
$150,000
Indirect Cost

  Institution

Name
University of Missouri-Columbia
Department
Veterinary Sciences
Type
Schools of Veterinary Medicine
DUNS #
153890272
City
Columbia
State
MO
Country
United States
Zip Code
65211

  Publications

Benson, James D; Benson, Charles T; Critser, John K (2014) Mathematical model formulation and validation of water and solute transport in whole hamster pancreatic islets. Math Biosci 254:64-75
Kashuba, Corinna M; Benson, James D; Critser, John K (2014) Rationally optimized cryopreservation of multiple mouse embryonic stem cell lines: I--Comparative fundamental cryobiology of multiple mouse embryonic stem cell lines and the implications for embryonic stem cell cryopreservation protocols. Cryobiology 68:166-75
Kashuba, Corinna M; Benson, James D; Critser, John K (2014) Rationally optimized cryopreservation of multiple mouse embryonic stem cell lines: II--Mathematical prediction and experimental validation of optimal cryopreservation protocols. Cryobiology 68:176-84
Rosenfeld, Cheryl S; Sieli, Paizlee T; Warzak, Denise A et al. (2013) Maternal exposure to bisphenol A and genistein has minimal effect on A(vy)/a offspring coat color but favors birth of agouti over nonagouti mice. Proc Natl Acad Sci U S A 110:537-42
Agca, Yuksel (2012) Genome resource banking of biomedically important laboratory animals. Theriogenology 78:1653-65
Benson, James D; Chicone, Carmen C; Critser, John K (2012) Analytical optimal controls for the state constrained addition and removal of cryoprotective agents. Bull Math Biol 74:1516-30
Korampally, Venumadhav; Mamidi, Vamshi Krishna; Harris, Bryant et al. (2011) Sub-minute formation of supported nanoporous mesoscale patterns programmed by surface energy. J Colloid Interface Sci 364:546-54
Benson, James D; Chicone, Carmen C; Critser, John K (2011) A general model for the dynamics of cell volume, global stability, and optimal control. J Math Biol 63:339-59
Hillhouse, Andrew E; Myles, Matthew H; Taylor, Jeremy F et al. (2011) Quantitative trait loci in a bacterially induced model of inflammatory bowel disease. Mamm Genome 22:544-55
Han, Xu; Liu, Yang; Critser, John K (2010) Determination of the quaternary phase diagram of the water-ethylene glycol-sucrose-NaCl system and a comparison between two theoretical methods for synthetic phase diagrams. Cryobiology 61:52-7

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