T Lymphocytes Negatively Regulate Lymph Node Lymphatic Vessel Formation

Raghu P. Kataru; Honsoul Kim; Cholsoon Jang; Dong Kyu Choi; Bong Ihn Koh; Minah Kim; Sudheer Gollamudi; Yun Keun Kim; Seung Hyo Lee; Gou Young Koh

doi:10.1016/j.immuni.2010.12.016

T Lymphocytes Negatively Regulate Lymph Node Lymphatic Vessel Formation

Raghu P. Kataru, Honsoul Kim, Cholsoon Jang, Dong Kyu Choi, Bong Ihn Koh, Minah Kim, Sudheer Gollamudi, Yun Keun Kim, Seung Hyo Lee, Gou Young Koh

School of Life Science and Biotechnology

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

192 Scopus citations

Abstract

Lymph node lymphatic vessels (LNLVs) serve as a conduit to drain antigens from peripheral tissues to within the lymph nodes. LNLV density is known to be positively regulated by vascular endothelial growth factors secreted by B cells, macrophages, and dendritic cells (DCs). Here, we show that LNLV formation was negatively regulated by T cells. In both steady and inflammatory states, the density of LNLVs was increased in the absence of T cells but decreased when T cells were restored. Interferon-γ secretion by T cells suppressed lymphatic-specific genes in lymphatic endothelial cells and consequently caused marked reduction in LNLV formation. When T cells were depleted, recruitment of antigen-carrying DCs to LNs was augmented, reflecting a compensatory mechanism for antigen presentation to T cells through increased LNLVs. Thus, T cells maintain the homeostatic balance of LNLV density through a negative paracrine action of interferon-γ.

Original language	English
Pages (from-to)	96-107
Number of pages	12
Journal	Immunity
Volume	34
Issue number	1
DOIs	https://doi.org/10.1016/j.immuni.2010.12.016
State	Published - 28 Jan 2011

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title = "T Lymphocytes Negatively Regulate Lymph Node Lymphatic Vessel Formation",

abstract = "Lymph node lymphatic vessels (LNLVs) serve as a conduit to drain antigens from peripheral tissues to within the lymph nodes. LNLV density is known to be positively regulated by vascular endothelial growth factors secreted by B cells, macrophages, and dendritic cells (DCs). Here, we show that LNLV formation was negatively regulated by T cells. In both steady and inflammatory states, the density of LNLVs was increased in the absence of T cells but decreased when T cells were restored. Interferon-γ secretion by T cells suppressed lymphatic-specific genes in lymphatic endothelial cells and consequently caused marked reduction in LNLV formation. When T cells were depleted, recruitment of antigen-carrying DCs to LNs was augmented, reflecting a compensatory mechanism for antigen presentation to T cells through increased LNLVs. Thus, T cells maintain the homeostatic balance of LNLV density through a negative paracrine action of interferon-γ.",

author = "Kataru, {Raghu P.} and Honsoul Kim and Cholsoon Jang and Choi, {Dong Kyu} and Koh, {Bong Ihn} and Minah Kim and Sudheer Gollamudi and Kim, {Yun Keun} and Lee, {Seung Hyo} and Koh, {Gou Young}",

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doi = "10.1016/j.immuni.2010.12.016",

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T1 - T Lymphocytes Negatively Regulate Lymph Node Lymphatic Vessel Formation

AU - Kataru, Raghu P.

AU - Kim, Honsoul

AU - Jang, Cholsoon

AU - Choi, Dong Kyu

AU - Koh, Bong Ihn

AU - Kim, Minah

AU - Gollamudi, Sudheer

AU - Kim, Yun Keun

AU - Lee, Seung Hyo

AU - Koh, Gou Young

PY - 2011/1/28

Y1 - 2011/1/28

N2 - Lymph node lymphatic vessels (LNLVs) serve as a conduit to drain antigens from peripheral tissues to within the lymph nodes. LNLV density is known to be positively regulated by vascular endothelial growth factors secreted by B cells, macrophages, and dendritic cells (DCs). Here, we show that LNLV formation was negatively regulated by T cells. In both steady and inflammatory states, the density of LNLVs was increased in the absence of T cells but decreased when T cells were restored. Interferon-γ secretion by T cells suppressed lymphatic-specific genes in lymphatic endothelial cells and consequently caused marked reduction in LNLV formation. When T cells were depleted, recruitment of antigen-carrying DCs to LNs was augmented, reflecting a compensatory mechanism for antigen presentation to T cells through increased LNLVs. Thus, T cells maintain the homeostatic balance of LNLV density through a negative paracrine action of interferon-γ.

AB - Lymph node lymphatic vessels (LNLVs) serve as a conduit to drain antigens from peripheral tissues to within the lymph nodes. LNLV density is known to be positively regulated by vascular endothelial growth factors secreted by B cells, macrophages, and dendritic cells (DCs). Here, we show that LNLV formation was negatively regulated by T cells. In both steady and inflammatory states, the density of LNLVs was increased in the absence of T cells but decreased when T cells were restored. Interferon-γ secretion by T cells suppressed lymphatic-specific genes in lymphatic endothelial cells and consequently caused marked reduction in LNLV formation. When T cells were depleted, recruitment of antigen-carrying DCs to LNs was augmented, reflecting a compensatory mechanism for antigen presentation to T cells through increased LNLVs. Thus, T cells maintain the homeostatic balance of LNLV density through a negative paracrine action of interferon-γ.

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DO - 10.1016/j.immuni.2010.12.016

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AN - SCOPUS:78751688024

SN - 1074-7613

VL - 34

SP - 96

EP - 107

JO - Immunity

JF - Immunity

IS - 1

ER -

T Lymphocytes Negatively Regulate Lymph Node Lymphatic Vessel Formation

Abstract

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