Abstract

Protective immunity, whether induced by infection or by vaccination, relies on the generation of memory B &T cells in sufficient quantity, and of sufficient quality. The success of this process is heavily dependent on """"""""help"""""""" that is provided by CD4+ T cells. CD4+ T cells play a central role in orchestrating the adaptive immune response but the mechanism by which their abundance is regulated, the importance of recurrent antigen contact, and the means by which they provide help to CD8+ T cells all remain uncertain. The overall goals of this application are (i) to continue our studies of how CD4+ T cell quantity and quality are regulated in vivo by IFN?, and how they are affected by in vivo contact with persistent virus antigen (Aims 1 &2);and (ii) to investigate how CD4+ T cells provide the help that is required for the development of good antiviral CD8+ T cell memory (Aims 3 &4).
Aim 1. To determine how direct IFN? signaling exerts its profound effects on the abundance of primary and memory CD4+ T cells. We have shown that CD4+ T cells that can respond directly to IFN? are 100- fold more abundant in the memory pool. We will determine when the effect of IFN? is exerted;what changes in gene expression occur as a result;and which cells produce this important cytokine.
Aim 2. To evaluate the effects of prolonged MHC class II antigen presentation on CD4+ T cell quantity and quality. It is well-established that, during chronic infection, persistent antigen can dramatically alter the T cell response. However, the issue of antigen persistence is much less well-defined in models of acute viral infection. We have found that MHC class II presents virus antigen for weeks after acute virus infection. We shall measure the effects of persistent antigen on CD4+ T cell functions. Does antigen- driven IFN? production sculpt the CD4+ T cell response? Aim 3. To investigate the help that is provided by virus-specific and non-specific CD4+ T cells. My lab was among the first to show that CD4+ T cells played a key role in establishing CD8+ T cell memory following acute virus infection, an observation that has been confirmed and extended by a number of labs. Surprisingly, CD4+ T cells seem to be able to provide help to CD8+ T cells in a non-specific (""""""""noncognate"""""""") fashion. We shall compare the helpfulness of CD4+ T cells that are specific for a viral epitope, with the helpfulness of CD4+ T cells that cannot recognize the virus.
Aim 4. To determine if IFN? is a key mediator of CD4+ T cell help.
The final Aim draws together two threads: (i) the fact that CD4+ T cell help is required for the development of good CD8+ T cell memory and (ii) our recent finding that IFN? is vitally important for the development of CD8+ T cell memory. Might IFN? be the """"""""link"""""""" by which CD4+ T cells help the development of CD8+ T cell memory? Is the role of IFN? the same for specific &non-specific CD4+ helper T cells?

Public Health Relevance

CD4+ T cells play a central role in regulating the immune response to infection and vaccination. Surprisingly, we do not know exactly what they do, and how they do it. Indeed, some recent data suggest that vaccines might work quite well even if they do not stimulate CD4+ T cell responses. This grant application investigates several of the questions surrounding the important, but poorly-understood, cells.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI052351-07
Application #
7744046
Study Section
Virology - B Study Section (VIRB)
Program Officer
Ferguson, Stacy E
Project Start
2002-09-15
Project End
2013-12-31
Budget Start
2010-01-01
Budget End
2010-12-31
Support Year
7
Fiscal Year
2010
Total Cost
$469,013
Indirect Cost

  Institution

Name
Scripps Research Institute
Department
Type
DUNS #
781613492
City
La Jolla
State
CA
Country
United States
Zip Code
92037

  Publications

Hosking, Martin P; Flynn, Claudia T; Whitton, J Lindsay (2014) Antigen-specific naive CD8+ T cells produce a single pulse of IFN-? in vivo within hours of infection, but without antiviral effect. J Immunol 193:1873-85
Hosking, Martin P; Flynn, Claudia T; Botten, Jason et al. (2013) CD8+ memory T cells appear exhausted within hours of acute virus infection. J Immunol 191:4211-22
Misumi, Ichiro; Alirezaei, Mehrdad; Eam, Boreth et al. (2013) Differential T cell responses to residual viral antigen prolong CD4+ T cell contraction following the resolution of infection. J Immunol 191:5655-68
Alirezaei, Mehrdad; Kemball, Christopher C; Whitton, J Lindsay (2011) Autophagy, inflammation and neurodegenerative disease. Eur J Neurosci 33:197-204
Whitmire, Jason K; Eam, Boreth; Whitton, J Lindsay (2009) Mice deficient in stem cell antigen-1 (Sca1, Ly-6A/E) develop normal primary and memory CD4+ and CD8+ T-cell responses to virus infection. Eur J Immunol 39:1494-504
Whitmire, Jason K; Benning, Nicola; Eam, Boreth et al. (2008) Increasing the CD4+ T cell precursor frequency leads to competition for IFN-gamma thereby degrading memory cell quantity and quality. J Immunol 180:6777-85
Liu, Fei; Whitton, J Lindsay (2005) Cutting edge: re-evaluating the in vivo cytokine responses of CD8+ T cells during primary and secondary viral infections. J Immunol 174:5936-40