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

Joseph N. Blattman; Jason M. Grayson; E. John Wherry; Susan M. Kaech; Kendall A. Smith; Rafi Ahmed

doi:10.1038/nm866

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

Joseph N. Blattman, Jason M. Grayson, E. John Wherry, Susan M. Kaech, Kendall A. Smith, Rafi Ahmed

Research output: Contribution to journal › Article › peer-review

319 Scopus citations

Abstract

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.

Original language	English (US)
Pages (from-to)	540-547
Number of pages	8
Journal	Nature Medicine
Volume	9
Issue number	5
DOIs	https://doi.org/10.1038/nm866
State	Published - May 1 2003
Externally published	Yes

ASJC Scopus subject areas

Biochemistry, Genetics and Molecular Biology(all)

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title = "Therapeutic use of IL-2 to enhance antiviral T-cell responses in vivo",

abstract = "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.",

author = "Blattman, {Joseph N.} and Grayson, {Jason M.} and Wherry, {E. John} and Kaech, {Susan M.} and Smith, {Kendall A.} and Rafi Ahmed",

note = "Funding Information: Acknowledgments We thank P.L. Mahar and other members of the Ahmed lab for helpful suggestions and technical assistance, and B.D. Evavold, P.D. Greenberg and L.E. Cheng for critical reading of this manuscript. This work was supported by National Institutes of Health grants AI30048 (to R.A.) and A151181 (to K.A.S.), the Cancer Research Institute/James E. Siegel Perpetual Fellowship Award (to J.N.B.), National Research Service Award 1F32AI0249-01A1 (to J.M.G.), a fellowship from the Cancer Research Institute (to E.J.W.), and the Cancer Research Fund of the Damon Runyon Cancer Research Foundation (DRG-1570 to S.M.K.).",

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N1 - Funding Information: Acknowledgments We thank P.L. Mahar and other members of the Ahmed lab for helpful suggestions and technical assistance, and B.D. Evavold, P.D. Greenberg and L.E. Cheng for critical reading of this manuscript. This work was supported by National Institutes of Health grants AI30048 (to R.A.) and A151181 (to K.A.S.), the Cancer Research Institute/James E. Siegel Perpetual Fellowship Award (to J.N.B.), National Research Service Award 1F32AI0249-01A1 (to J.M.G.), a fellowship from the Cancer Research Institute (to E.J.W.), and the Cancer Research Fund of the Damon Runyon Cancer Research Foundation (DRG-1570 to S.M.K.).

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N2 - 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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Therapeutic use of IL-2 to enhance antiviral T-cell responses in vivo

Abstract

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