Abstract

Human cytomegalovirus (HCMV) is the leading infectious cause of congenital birth defects in the United States, and is an important source of morbidity and mortality for those who are immunocompromised. Since a substantial proportion of HCMV transmission occurs perinatally and in early infancy, an ideal HCMV vaccine would be effective in this age group. A potential limitation of vaccination at this age is the apparent immaturity of CD4 T cell expression of effector molecular, particularly secreted cytokines, e.g., interferon-gamma (IFN-gamma) and tumor necrosis factor (TNF), surface molecules, such as CD40-ligand (CD40-L). Such limitations have not been shown for postnatally acquired HCMV infection.
The first aim of this project is to determine HCMV-specific CD4 T cell expression of effector molecules, particularly secreted cytokines, e.g., interferon-gamma (IFN-gamma) and tumor necrosis factor (TNF), surface molecules, such as CD40-ligand (CD40-L). Such limitations have not been shown for postnatally acquired HCMV infection.
The first aim of this project is to determine HCMV-specific CD4 T cell memory/effector function following primary HCMV infection of infants and adults, and its relationship with other HCMV-specific immune responses, viral clearance, and the establishment of viral latency. It is hypothesized that young infants will have a decreased accumulation of HCMV antigen-specific memory/effector CD4 T cells that can secrete cytokines or express CD40-L compared to adults. We further predict that infant HCMV-specific CD4 T cells will preferentially produce Th2 cytokines that lack anti-viral activity or many inhibit this activity. Responses to HCMV overall, and to the pp65 matrix protein, which appears to be a major target of the CD4 T cell response, will be examined. It will be determined if decreased and/or altered infant CD4 T cell responses are paralleled by decreased serum levels of neutralizing HCMV antibody, prolonged viremia, prolonged urinary viral shedding (all determined by the Clinical Research Core), decreased HCMV-specific CD8 T cell function (Project 2), and decreased antigen-presenting function (APC) (Project 3).
The second aim i s to develop fluorochrome- labeled HLA-DR tetramer molecules containing ppo65 peptides to identify CD4 T cells in infants and adults with specificity for pp65. This will test the hypothesis that infants but not adults have a substantial fraction of CD4 T cells with specificity for pp65 but reduced or absent responsiveness to pp65 antigen. These studies will provide insight into the human CD4 memory/effector T cell response following primary HCMV infection in normal infants and adults, APC function. Since new trials of HCMV vaccines are imminent, these studies may also provide useful immature response predictors for vaccine efficacy, such as prevention of HCMV infection and/or improved maintenance of latency. They may also point out strategies by which protective responses might be augmented by immunotherapy, particularly during infancy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program Projects (P01)
Project #
5P01AI048212-02
Application #
6454157
Study Section
Special Emphasis Panel (ZAI1)
Project Start
2001-07-01
Project End
2002-06-30
Budget Start
Budget End
Support Year
2
Fiscal Year
2001
Total Cost
$187,449
Indirect Cost

  Institution

Name
Stanford University
Department
Type
DUNS #
800771545
City
Stanford
State
CA
Country
United States
Zip Code
94305

  Publications

Lee, Andrew W; Wang, Nan; Hornell, Tara M C et al. (2011) Human cytomegalovirus decreases constitutive transcription of MHC class II genes in mature Langerhans cells by reducing CIITA transcript levels. Mol Immunol 48:1160-7
Zeman, Alenka M; Holmes, Tyson H; Stamatis, Shaye et al. (2007) Humoral and cellular immune responses in children given annual immunization with trivalent inactivated influenza vaccine. Pediatr Infect Dis J 26:107-15
Tu, Wenwei; Potena, Luciano; Stepick-Biek, Pamela et al. (2006) T-cell immunity to subclinical cytomegalovirus infection reduces cardiac allograft disease. Circulation 114:1608-15
Hornell, Tara M C; Burster, Timo; Jahnsen, Frode L et al. (2006) Human dendritic cell expression of HLA-DO is subset specific and regulated by maturation. J Immunol 176:3536-47
Lee, Andrew W; Hertel, Laura; Louie, Ryan K et al. (2006) Human cytomegalovirus alters localization of MHC class II and dendrite morphology in mature Langerhans cells. J Immunol 177:3960-71
Chen, Sharon F; Tu, Wen-Wei; Sharp, Margaret A et al. (2004) Antiviral CD8 T cells in the control of primary human cytomegalovirus infection in early childhood. J Infect Dis 189:1619-27
Tu, Wenwei; Chen, Sharon; Sharp, Margaret et al. (2004) Persistent and selective deficiency of CD4+ T cell immunity to cytomegalovirus in immunocompetent young children. J Immunol 172:3260-7
Drohan, Laura; Harding, James J; Holm, Bari et al. (2004) Selective developmental defects of cord blood antigen-presenting cell subsets. Hum Immunol 65:1356-69
Hertel, Laura; Lacaille, Vashti G; Strobl, Herbert et al. (2003) Susceptibility of immature and mature Langerhans cell-type dendritic cells to infection and immunomodulation by human cytomegalovirus. J Virol 77:7563-74
He, Xiao-Song; Mahmood, Kutubuddin; Maecker, Holden T et al. (2003) Analysis of the frequencies and of the memory T cell phenotypes of human CD8+ T cells specific for influenza A viruses. J Infect Dis 187:1075-84

Showing the most recent 10 out of 12 publications