Abstract

The long-term human immune response to pathogens results from development of immune memory. This process is vital for health, and understanding how memory is formed and evolves is essential for rational approaches to vaccine development and vaccination. In man, how memory T cells are generated or maintained during the adult years, and how the number and type of T cell changes with re-exposure to pathogen are still poorly understood. Furthermore, how populations of humans respond to the same pathogen and to pathogen re-exposure has not been investigated at a basic level. In the Center Grant we investigate the memory response of cytotoxic, helper, and gamma/delta T cells to influenza. This pathogen is involved in recurring epidemics. It is derived from a large avian pool of viruses that by recombination in pigs can move from birds to man. Thus, the virus could be manipulated to select for more pathogenic types. In this Center Grant we will investigate the hypothesis that most T cell memory is derived from a robust network of T cells that was generated when the thymus was generating a large number of naive T cells. Using influenza as our model pathogen, we will investigate how memory T cells that are studied from blood relate to memory cells in the lung. By analyzing memory T cell repertoires in a cohort of individuals over a number of years, and correlating the results with the risk of exposure to influenza, we should develop a detailed understanding of how the complex network of memory T cells change with time and with pathogen re-exposure. The Center Grant consists of four scientific projects that approach the above issues from the point of view of: 1) Class I HLA-restricted memory T cell responses from blood. 2) Class II HLA-restricted memory T cell responses from blood. 3) Responses of T cells from bronchial alveolar lavages in comparison with those from blood. These studies will also include analyzing the possible role of gamma/delta T cells in the response. 4) Modeling the nature of the responding repertoires and generating a molecular description of the epidemiology of influenza. These studies will be supported by a number of cores that are responsible for providing common samples, common testing and common reagents. Four technical aims are proposed for advancing repertoire analysis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program--Cooperative Agreements (U19)
Project #
5U19AI062627-05
Application #
7494624
Study Section
Special Emphasis Panel (ZAI1-PA-I (S1))
Program Officer
Quill, Helen R
Project Start
2004-09-15
Project End
2010-08-31
Budget Start
2008-09-01
Budget End
2010-08-31
Support Year
5
Fiscal Year
2008
Total Cost
$2,321,915
Indirect Cost

  Institution

Name
Bloodcenter of Wisconsin, Inc.
Department
Type
DUNS #
057163172
City
Milwaukee
State
WI
Country
United States
Zip Code
53233

  Publications

Alarcon Falconi, T M; Cruz, M S; Naumova, E N (2018) The shift in seasonality of legionellosis in the USA. Epidemiol Infect 146:1824-1833
Yassai, Maryam B; Demos, Wendy; Gorski, Jack (2017) Structural and Mechanistic Implications of Rearrangement Frequencies within Human TCRBV Genes. J Immunol 199:1142-1152
Gil, Anna; Yassai, Maryam B; Naumov, Yuri N et al. (2015) Narrowing of human influenza A virus-specific T cell receptor ? and ? repertoires with increasing age. J Virol 89:4102-16
Zhou, Vivian; Yassai, Maryam B; Regunathan, Jeyarani et al. (2013) The functional CD8 T cell memory recall repertoire responding to the influenza A M1(58-66) epitope is polyclonal and shows a complex clonotype distribution. Hum Immunol 74:809-17
Bonacci, Benedetta; Edwards, Brandon; Jia, Shuang et al. (2012) Requirements for growth and IL-10 expression of highly purified human T regulatory cells. J Clin Immunol 32:1118-28
Kumar, Pawan; Bartoszek, Allison E; Moran, Thomas M et al. (2012) High-throughput detection method for influenza virus. J Vis Exp :
Levy, H; Wang, X; Kaldunski, M et al. (2012) Transcriptional signatures as a disease-specific and predictive inflammatory biomarker for type 1 diabetes. Genes Immun 13:593-604
Petrova, Galina; Ferrante, Andrea; Gorski, Jack (2012) Cross-reactivity of T cells and its role in the immune system. Crit Rev Immunol 32:349-72
Petrova, Galina V; Gorski, Jack (2012) Cross-reactive responses to modified M1??-?? peptides by CD8? T cells that use noncanonical BV genes can describe unknown repertoires. Eur J Immunol 42:3001-8
Baumgartner, Christina K; Yagita, Hideo; Malherbe, Laurent P (2012) A TCR affinity threshold regulates memory CD4 T cell differentiation following vaccination. J Immunol 189:2309-17

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