Abstract

Aging is associated with a decline in T cell mediated functions, which contributes to a higher incidence of, and morbidity and mortality from, infectious diseases and tumors. The age-related defect in T cells has been shown to be due to intrinsic declines in T cell function, as well as increased production of prostaglandin (PG)E2, a T cell suppressive factor, by macrophages (Mphi). We demonstrated that the increased PGE2 production was due to ceramide mediated upregulation of cyclooxygenase 2 (COX-2) transcription, a key regulatory enzyme in PGE2 synthesis. The signaling mechanism through which ceramide upregulates COX 2 expression, however, is not known and needs to be investigated. We further showed that vitamin E (E) supplementation improves T cell mediated function by two distinct mechanisms: a) by decreasing PGE2 production, thus reducing macrophage Mphi mediated suppression, and b) by directly enhancing T cell function, independent of its effect on Mphi PGE2 production. E exerts its effect by improving the ability of naive T cells from old mice to produce IL-2 and progress through cell division cycles. The mechanism of E-induced enhancement of naive T cell function is not known and needs to be determined. Thus, the specific aims of this proposal are: 1) To determine the signaling pathway involved in ceramide-induced upregulation of COX-2 expression in old Mphi. To accomplish this goal, we will test the hypothesis that ceramide upregulates COX-2 expression in old macrophages through enhancing PKC-zeta activity, leading to increased IkappaB phosphorylation, and thus degradation. This in turn will increase NFkappaB activation and COX-2 expression. 2) To determine the mechanism of E-induced increase in the function of old naive T cells. To accomplish this goal, we will test the hypothesis that E enhances naive T cell function in old mice by increasing their ability to form an effective immune synapse at the site of T cell receptor (TCR) and antigen contact. This, in turn, will lead to improved TCR-associated signal transduction, and subsequent, IL-2 production in old mice. We propose that E induces its effect by changing the redistribution of key TCR associated signaling molecules in membrane lipid domains, known as lipid rafts, by one or both of the following mechanisms: a) increasing palmitoylation of key signaling molecules associated with TCR-mediated activation, and b) changing the structure of the lipid component of lipid rafts. These experiments will elucidate the mechanism of the age-related dysregulation of macrophages and T cells, as well as their normalization by E. This, in turn, will help in designing practical nutritional interventions to reverse and/or delay the age-associated dysregulation of immune and inflammatory responses as well as diseases associated with it.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Project (R01)
Project #
5R01AG009140-12
Application #
6948782
Study Section
Geriatrics and Rehabilitation Medicine (GRM)
Program Officer
Fuldner, Rebecca A
Project Start
2003-09-30
Project End
2008-08-31
Budget Start
2005-09-01
Budget End
2006-08-31
Support Year
12
Fiscal Year
2005
Total Cost
$280,000
Indirect Cost

  Institution

Name
Tufts University
Department
Type
Organized Research Units
DUNS #
039318308
City
Boston
State
MA
Country
United States
Zip Code
02111

  Publications

Molano, Alberto; Huang, Zhaofeng; Marko, Melissa G et al. (2012) Age-dependent changes in the sphingolipid composition of mouse CD4+ T cell membranes and immune synapses implicate glucosylceramides in age-related T cell dysfunction. PLoS One 7:e47650
Sempértegui, Fernando; Estrella, Bertha; Tucker, Katherine L et al. (2011) Metabolic syndrome in the elderly living in marginal peri-urban communities in Quito, Ecuador. Public Health Nutr 14:758-67
Dao, Maria C; Meydani, Simin Nikbin (2009) Micronutrient status, immune response and infectious disease in elderly of less developed countries. Sight Life Mag 3:6-15
Hamer, Davidson H; Sempertegui, Fernando; Estrella, Bertha et al. (2009) Micronutrient deficiencies are associated with impaired immune response and higher burden of respiratory infections in elderly Ecuadorians. J Nutr 139:113-9
Marko, Melissa G; Pang, Hoan-Jen E; Ren, Zhihong et al. (2009) Vitamin E reverses impaired linker for activation of T cells activation in T cells from aged C57BL/6 mice. J Nutr 139:1192-7
Meydani, Simin Nikbin; Wu, Dayong (2008) Nutrition and age-associated inflammation: implications for disease prevention. JPEN J Parenter Enteral Nutr 32:626-9
Wu, Dayong; Meydani, Simin Nikbin (2008) Age-associated changes in immune and inflammatory responses: impact of vitamin E intervention. J Leukoc Biol 84:900-14
Meydani, Simin Nikbin; Wu, Dayong (2007) Age-associated inflammatory changes: role of nutritional intervention. Nutr Rev 65:S213-6
Wu, Dayong; Ren, Zhihong; Pae, Munkyong et al. (2007) Aging up-regulates expression of inflammatory mediators in mouse adipose tissue. J Immunol 179:4829-39
Marko, Melissa G; Ahmed, Tanvir; Bunnell, Stephen C et al. (2007) Age-associated decline in effective immune synapse formation of CD4(+) T cells is reversed by vitamin E supplementation. J Immunol 178:1443-9

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