Requirement for T-cell apoptosis in the induction of peripheral transplantation tolerance

Andrew D. Wells; Xian Chang Li; Yongsheng Li; Matthew C. Walsh; Xin Xiao Zheng; Zihao Wu; Gabriel Nuñez; Aimin Tang; Mohamed Sayegh; Wayne W. Hancock; Terry B. Strom; Laurence A. Turka

doi:10.1038/15260

Requirement for T-cell apoptosis in the induction of peripheral transplantation tolerance

Andrew D. Wells, Xian Chang Li, Yongsheng Li, Matthew C. Walsh, Xin Xiao Zheng, Zihao Wu, Gabriel Nuñez, Aimin Tang, Mohamed Sayegh, Wayne W. Hancock, Terry B. Strom, Laurence A. Turka

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Abstract

The mechanisms of allograft tolerance have been classified as deletion, anergy, ignorance and suppression/regulation. Deletion has been implicated in central tolerance, whereas peripheral tolerance has generally been ascribed to clonal anergy and/or active immunoregulatory states. Here, we used two distinct systems to assess the requirement for T-cell deletion in peripheral tolerance induction. In mice transgenic for Bcl-x(L), T cells were resistant to passive cell death through cytokine withdrawal, whereas T cells from interleukin-2-deficient mice did not undergo activation-induced cell death. Using either agents that block co-stimulatory pathways or the immunosuppressive drug rapamycin, which we have shown here blocks the proliferative component of interleukin-2 signaling but does not inhibit priming for activation-induced cell death, we found that mice with defective passive or active T-cell apoptotic pathways were resistant to induction of transplantation tolerance. Thus, deletion of activated T cells through activation-induced cell death or growth factor withdrawal seems necessary to achieve peripheral tolerance across major histocompatibility complex barriers.

Original language	English (US)
Pages (from-to)	1303-1307
Number of pages	5
Journal	Nature Medicine
Volume	5
Issue number	11
DOIs	https://doi.org/10.1038/15260
State	Published - Nov 1999

ASJC Scopus subject areas

Biochemistry, Genetics and Molecular Biology(all)

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title = "Requirement for T-cell apoptosis in the induction of peripheral transplantation tolerance",

abstract = "The mechanisms of allograft tolerance have been classified as deletion, anergy, ignorance and suppression/regulation. Deletion has been implicated in central tolerance, whereas peripheral tolerance has generally been ascribed to clonal anergy and/or active immunoregulatory states. Here, we used two distinct systems to assess the requirement for T-cell deletion in peripheral tolerance induction. In mice transgenic for Bcl-x(L), T cells were resistant to passive cell death through cytokine withdrawal, whereas T cells from interleukin-2-deficient mice did not undergo activation-induced cell death. Using either agents that block co-stimulatory pathways or the immunosuppressive drug rapamycin, which we have shown here blocks the proliferative component of interleukin-2 signaling but does not inhibit priming for activation-induced cell death, we found that mice with defective passive or active T-cell apoptotic pathways were resistant to induction of transplantation tolerance. Thus, deletion of activated T cells through activation-induced cell death or growth factor withdrawal seems necessary to achieve peripheral tolerance across major histocompatibility complex barriers.",

author = "Wells, {Andrew D.} and Li, {Xian Chang} and Yongsheng Li and Walsh, {Matthew C.} and Zheng, {Xin Xiao} and Zihao Wu and Gabriel Nu{\~n}ez and Aimin Tang and Mohamed Sayegh and Hancock, {Wayne W.} and Strom, {Terry B.} and Turka, {Laurence A.}",

note = "Funding Information: Acknowledgments This work was supported by the National Kidney Foundation of America (X.C.L.), the Juvenile Diabetes Foundation (X.X.Z., T.B.S., M.H.S. and L.A.T.), the American Heart Association (L.A.T.) and the National Institutes of Health (AI-34665, AI-37691, AI-37798, AI-41521, AI-42298 and CA09140).",

year = "1999",

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doi = "10.1038/15260",

language = "English (US)",

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AU - Wells, Andrew D.

AU - Li, Xian Chang

AU - Li, Yongsheng

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AU - Zheng, Xin Xiao

AU - Wu, Zihao

AU - Nuñez, Gabriel

AU - Tang, Aimin

AU - Sayegh, Mohamed

AU - Hancock, Wayne W.

AU - Strom, Terry B.

AU - Turka, Laurence A.

N1 - Funding Information: Acknowledgments This work was supported by the National Kidney Foundation of America (X.C.L.), the Juvenile Diabetes Foundation (X.X.Z., T.B.S., M.H.S. and L.A.T.), the American Heart Association (L.A.T.) and the National Institutes of Health (AI-34665, AI-37691, AI-37798, AI-41521, AI-42298 and CA09140).

PY - 1999/11

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N2 - The mechanisms of allograft tolerance have been classified as deletion, anergy, ignorance and suppression/regulation. Deletion has been implicated in central tolerance, whereas peripheral tolerance has generally been ascribed to clonal anergy and/or active immunoregulatory states. Here, we used two distinct systems to assess the requirement for T-cell deletion in peripheral tolerance induction. In mice transgenic for Bcl-x(L), T cells were resistant to passive cell death through cytokine withdrawal, whereas T cells from interleukin-2-deficient mice did not undergo activation-induced cell death. Using either agents that block co-stimulatory pathways or the immunosuppressive drug rapamycin, which we have shown here blocks the proliferative component of interleukin-2 signaling but does not inhibit priming for activation-induced cell death, we found that mice with defective passive or active T-cell apoptotic pathways were resistant to induction of transplantation tolerance. Thus, deletion of activated T cells through activation-induced cell death or growth factor withdrawal seems necessary to achieve peripheral tolerance across major histocompatibility complex barriers.

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Requirement for T-cell apoptosis in the induction of peripheral transplantation tolerance

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