Therapeutic use of IL-2 to enhance antiviral T-cell responses in vivo

被引:0
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作者
Joseph N. Blattman
Jason M. Grayson
E. John Wherry
Susan M. Kaech
Kendall A. Smith
Rafi Ahmed
机构
[1] Emory Vaccine Center,Division of Immunology, Department of Medicine
[2] Emory University School of Medicine,undefined
[3] Weill Medical College,undefined
[4] Cornell University,undefined
来源
Nature Medicine | 2003年 / 9卷
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摘要
Interleukin (IL)-2 is currently used to enhance T-cell immunity but can have both positive and negative effects on T cells. To determine whether these opposing results are due to IL-2 acting differently on T cells depending on their stage of differentiation, we examined the effects of IL-2 therapy during the expansion, contraction and memory phases of the T-cell response in lymphocytic choriomeningitis virus (LCMV)–infected mice. IL-2 treatment during the expansion phase was detrimental to the survival of rapidly dividing effector T cells. In contrast, IL-2 therapy was highly beneficial during the death phase, resulting in increased proliferation and survival of virus-specific T cells. IL-2 treatment also increased proliferation of resting memory T cells in mice that controlled the infection. Virus-specific T cells in chronically infected mice also responded to IL-2 resulting in decreased viral burden. Thus, timing of IL-2 administration and differentiation status of the T cell are critical parameters in designing IL-2 therapies.
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页码:540 / 547
页数:7
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