Abstract

Function of Core C: The primary function of Core C will be to generate, screen, and provide the investigators with genetically altered strains of mice that can be utilized as murine models for influenza infection. To accomplish this goal the core will: (a) coordinate the breeding and weaning of inbred mouse strains required by the individual projects, (b) genetically type the mice utilized in the murine models of influenza, (c) produce new inbred strains of mice required for individual projects, (d) produce and characterize the influenza viral stocks, and (e) generate survival curves for these viral stocks in the mouse strains utilized by the individual projects. This resource will be heavily utilized by Project 1 """"""""The role of CD8 T cells in Lung Immunity"""""""", Project 2 """"""""CD4 T cell protection and pathology in the lung"""""""", Project 3 """"""""CD8+ T cell memory to respiratory virus infections"""""""" and Project 4 """"""""T cell responses of nasal mucosa and lymphoid tissues"""""""". The core unit leader is Dr. Frances Lund who is an Assistant Member at the Trudeau Institute and currently is the Scientific Director of the Trudeau Animal facilities. The Trudeau Institute is well known for its expertise in animal models of infectious disease and for its excellent mouse breeding facility. The mouse breeding facility at the Trudeau Institute has all of the resources required to produce the animals required for this Program Project as it currently breeds over 130 different strains of mice including a large number of T cell receptor transgenic, cytokine deficient, and other genetically altered knockout (KO) strains of mice. Approximately half of the strains of mice bred at the Trudeau Institute must be genetically typed and Dr. Lund's lab currently performs the genotypic screening of many of these strains. Additionally, Dr. Lund's lab also performs screening for a number of the ongoing genetic backcrossing projects at the Institute. Thus, Dr. Lund's laboratory has the expertise and the experience required to fulfill the function of Core C.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Program Projects (P01)
Project #
5P01HL063925-02
Application #
6565125
Study Section
Heart, Lung, and Blood Program Project Review Committee (HLBP)
Project Start
2001-12-01
Project End
2002-11-30
Budget Start
Budget End
Support Year
2
Fiscal Year
2002
Total Cost
Indirect Cost

  Institution

Name
Trudeau Institute, Inc.
Department
Type
DUNS #
City
Saranac Lake
State
NY
Country
United States
Zip Code
12983

  Publications

Ely, Kenneth H; Roberts, Alan D; Kohlmeier, Jacob E et al. (2007) Aging and CD8+ T cell immunity to respiratory virus infections. Exp Gerontol 42:427-31
Wiley, James A; Tighe, Michael P; Harmsen, Allen G (2005) Upper respiratory tract resistance to influenza infection is not prevented by the absence of either nasal-associated lymphoid tissue or cervical lymph nodes. J Immunol 175:3186-96
Powell, Timothy J; Brown, Deborah M; Hollenbaugh, Joseph A et al. (2004) CD8+ T cells responding to influenza infection reach and persist at higher numbers than CD4+ T cells independently of precursor frequency. Clin Immunol 113:89-100
Brown, Deborah M; Roman, Eulogia; Swain, Susan L (2004) CD4 T cell responses to influenza infection. Semin Immunol 16:171-7
Cauley, Linda S; Cookenham, Tres; Hogan, Robert J et al. (2003) Renewal of peripheral CD8+ memory T cells during secondary viral infection of antibody-sufficient mice. J Immunol 170:5597-606
Woodland, David L; Dutton, Richard W (2003) Heterogeneity of CD4(+) and CD8(+) T cells. Curr Opin Immunol 15:336-42
Blackman, Marcia A; Rouse, Barry T; Chisari, Frank V et al. (2002) Viral immunology: challenges associated with the progression from bench to clinic. Trends Immunol 23:565-7
Arnold, Paula Y; Vignali, Kate M; Miller, Timothy B et al. (2002) Reliable generation and use of MHC class II:gamma2aFc multimers for the identification of antigen-specific CD4(+) T cells. J Immunol Methods 271:137-51
Cauley, Linda S; Hogan, Robert J; Woodland, David L (2002) Memory T-cells in non-lymphoid tissues. Curr Opin Investig Drugs 3:33-6
Wiley, J A; Hogan, R J; Woodland, D L et al. (2001) Antigen-specific CD8(+) T cells persist in the upper respiratory tract following influenza virus infection. J Immunol 167:3293-9