Publication
The role of mTOR in memory CD8+ T-cell differentiation
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- Last modified
- 02/20/2025
- Type of Material
- Authors
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Koichi Araki, Emory UniversityBenjamin Alan Youngblood, Emory UniversityRafi Ahmed, Emory University
- Language
- English
- Date
- 2010-05
- Publisher
- Wiley: 12 months
- Publication Version
- Copyright Statement
- © 2010 John Wiley & Sons A/S
- Final Published Version (URL)
- Title of Journal or Parent Work
- ISSN
- 0105-2896
- Volume
- 235
- Issue
- 1
- Start Page
- 234
- End Page
- 243
- Grant/Funding Information
- Work from our laboratory was supported by NIH grants (AI030048 and N01-AI-50025) and Bill and Melinda Gates Foundation Grant (CAVD 38645). B.Y. was supported by a postdoctoral fellowship from the American Cancer Society (PF-09-134-01-MPC).
- Abstract
- The mammalian target of rapamycin (mTOR) is an intracellular kinase that regulates cell growth and metabolism. Its specific inhibitor rapamycin is currently used in transplant recipients as an immunosuppressive drug to prevent allograft rejection. Studies have shown complex and diverse mechanisms for the immunosuppressive effects of rapamycin. The drug has been reported to inhibit T-cell proliferation, induce anergy, modulate T-cell trafficking, promote regulatory T cells, and also prevent maturation of dendritic cells as well as production of type I IFN production. However, several other studies have paradoxically demonstrated immunostimulatory effects of rapamycin by improving antigen presentation and regulating cytokine production from macrophages and myeloid dendritic cells. Recently, it has been shown that rapamycin also exhibits immunostimulatory effects on memory CD8+ T-cell differentiation. The drug improved both quantity and quality of memory CD8+ T cells induced by viral infection and vaccination, showing that mTOR is a major regulator of memory CD8+ T-cell differentiation. These discoveries have implications for the development of novel vaccine regimens. Here we review the role of mTOR in memory CD8+ T-cell differentiation and compare the effect of rapamycin between CD8+ T cells, CD4+ T cells, and dendritic cells. Also we discuss potential application of these findings in a clinical setting.
- Author Notes
- Keywords
- Research Categories
- Biology, Microbiology
- Health Sciences, Immunology
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