CD127 expression inversely correlates with FoxP3 and suppressive function of human CD4+ T reg cells

Weihong Liu; Amy L. Putnam; Zhou Xu-yu; Gregory L. Szot; Michael R. Lee; Shirley Zhu; Peter A. Gottlieb; Philipp Kapranov; Thomas R. Gingeras; Barbara Fazekas Barbara; Carol Clayberger; David M. Soper; Steven F. Ziegler; Jeffrey A. Bluestone

doi:10.1084/jem.20060772

CD127 expression inversely correlates with FoxP3 and suppressive function of human CD4⁺ T reg cells

Weihong Liu, Amy L. Putnam, Zhou Xu-yu, Gregory L. Szot, Michael R. Lee, Shirley Zhu, Peter A. Gottlieb, Philipp Kapranov, Thomas R. Gingeras, Barbara Fazekas Barbara, Carol Clayberger, David M. Soper, Steven F. Ziegler, Jeffrey A. Bluestone^*

^*Corresponding author for this work

Microbiology-Immunology

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

2146 Scopus citations

Abstract

Regulatory T (T reg) cells are critical regulators of immune tolerance. Most T reg cells are defined based on expression of CD4, CD25, and the transcription factor, FoxP3. However, these markers have proven problematic for uniquely defining this specialized T cell subset in humans. We found that the IL-7 receptor (CD127) is down-regulated on a subset of CD4⁺ T cells in peripheral blood. We demonstrate that the majority of these cells are FoxP3⁺, including those that express low levels or no CD25. A combination of CD4, CD25, and CD127 resulted in a highly purified population of T reg cells accounting for significantly more cells that previously identified based on other cell surface markers. These cells were highly suppressive in functional suppressor assays. In fact, cells separated based solely on CD4 and CD127 expression were anergic and, although representing at least three times the number of cells (including both CD25⁺CD4⁺ and CD25^-CD4⁺ T cell subsets), were as suppressive as the "classic" CD4⁺CD25^hi T reg cell subset. Finally, we show that CD127 can be used to quantitate T reg cell subsets in individuals with type 1 diabetes supporting the use of CD127 as a biomarker for human T reg cells. JEM

Original language	English (US)
Pages (from-to)	1701-1711
Number of pages	11
Journal	Journal of Experimental Medicine
Volume	203
Issue number	7
DOIs	https://doi.org/10.1084/jem.20060772
State	Published - Jul 10 2006

ASJC Scopus subject areas

Immunology and Allergy
Immunology

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10.1084/jem.20060772

Cite this

Liu, W., Putnam, A. L., Xu-yu, Z., Szot, G. L., Lee, M. R., Zhu, S., Gottlieb, P. A., Kapranov, P., Gingeras, T. R., Barbara, B. F., Clayberger, C., Soper, D. M., Ziegler, S. F., & Bluestone, J. A. (2006). CD127 expression inversely correlates with FoxP3 and suppressive function of human CD4⁺ T reg cells. Journal of Experimental Medicine, 203(7), 1701-1711. https://doi.org/10.1084/jem.20060772

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title = "CD127 expression inversely correlates with FoxP3 and suppressive function of human CD4+ T reg cells",

abstract = "Regulatory T (T reg) cells are critical regulators of immune tolerance. Most T reg cells are defined based on expression of CD4, CD25, and the transcription factor, FoxP3. However, these markers have proven problematic for uniquely defining this specialized T cell subset in humans. We found that the IL-7 receptor (CD127) is down-regulated on a subset of CD4+ T cells in peripheral blood. We demonstrate that the majority of these cells are FoxP3+, including those that express low levels or no CD25. A combination of CD4, CD25, and CD127 resulted in a highly purified population of T reg cells accounting for significantly more cells that previously identified based on other cell surface markers. These cells were highly suppressive in functional suppressor assays. In fact, cells separated based solely on CD4 and CD127 expression were anergic and, although representing at least three times the number of cells (including both CD25+CD4+ and CD25-CD4+ T cell subsets), were as suppressive as the {"}classic{"} CD4+CD25hi T reg cell subset. Finally, we show that CD127 can be used to quantitate T reg cell subsets in individuals with type 1 diabetes supporting the use of CD127 as a biomarker for human T reg cells. JEM",

author = "Weihong Liu and Putnam, {Amy L.} and Zhou Xu-yu and Szot, {Gregory L.} and Lee, {Michael R.} and Shirley Zhu and Gottlieb, {Peter A.} and Philipp Kapranov and Gingeras, {Thomas R.} and Barbara, {Barbara Fazekas} and Carol Clayberger and Soper, {David M.} and Ziegler, {Steven F.} and Bluestone, {Jeffrey A.}",

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doi = "10.1084/jem.20060772",

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Liu, W, Putnam, AL, Xu-yu, Z, Szot, GL, Lee, MR, Zhu, S, Gottlieb, PA, Kapranov, P, Gingeras, TR, Barbara, BF, Clayberger, C, Soper, DM, Ziegler, SF & Bluestone, JA 2006, 'CD127 expression inversely correlates with FoxP3 and suppressive function of human CD4⁺ T reg cells', Journal of Experimental Medicine, vol. 203, no. 7, pp. 1701-1711. https://doi.org/10.1084/jem.20060772

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T1 - CD127 expression inversely correlates with FoxP3 and suppressive function of human CD4+ T reg cells

AU - Liu, Weihong

AU - Putnam, Amy L.

AU - Xu-yu, Zhou

AU - Szot, Gregory L.

AU - Lee, Michael R.

AU - Zhu, Shirley

AU - Gottlieb, Peter A.

AU - Kapranov, Philipp

AU - Gingeras, Thomas R.

AU - Barbara, Barbara Fazekas

AU - Clayberger, Carol

AU - Soper, David M.

AU - Ziegler, Steven F.

AU - Bluestone, Jeffrey A.

PY - 2006/7/10

Y1 - 2006/7/10

N2 - Regulatory T (T reg) cells are critical regulators of immune tolerance. Most T reg cells are defined based on expression of CD4, CD25, and the transcription factor, FoxP3. However, these markers have proven problematic for uniquely defining this specialized T cell subset in humans. We found that the IL-7 receptor (CD127) is down-regulated on a subset of CD4+ T cells in peripheral blood. We demonstrate that the majority of these cells are FoxP3+, including those that express low levels or no CD25. A combination of CD4, CD25, and CD127 resulted in a highly purified population of T reg cells accounting for significantly more cells that previously identified based on other cell surface markers. These cells were highly suppressive in functional suppressor assays. In fact, cells separated based solely on CD4 and CD127 expression were anergic and, although representing at least three times the number of cells (including both CD25+CD4+ and CD25-CD4+ T cell subsets), were as suppressive as the "classic" CD4+CD25hi T reg cell subset. Finally, we show that CD127 can be used to quantitate T reg cell subsets in individuals with type 1 diabetes supporting the use of CD127 as a biomarker for human T reg cells. JEM

AB - Regulatory T (T reg) cells are critical regulators of immune tolerance. Most T reg cells are defined based on expression of CD4, CD25, and the transcription factor, FoxP3. However, these markers have proven problematic for uniquely defining this specialized T cell subset in humans. We found that the IL-7 receptor (CD127) is down-regulated on a subset of CD4+ T cells in peripheral blood. We demonstrate that the majority of these cells are FoxP3+, including those that express low levels or no CD25. A combination of CD4, CD25, and CD127 resulted in a highly purified population of T reg cells accounting for significantly more cells that previously identified based on other cell surface markers. These cells were highly suppressive in functional suppressor assays. In fact, cells separated based solely on CD4 and CD127 expression were anergic and, although representing at least three times the number of cells (including both CD25+CD4+ and CD25-CD4+ T cell subsets), were as suppressive as the "classic" CD4+CD25hi T reg cell subset. Finally, we show that CD127 can be used to quantitate T reg cell subsets in individuals with type 1 diabetes supporting the use of CD127 as a biomarker for human T reg cells. JEM

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