Notch2 Receptor Signaling Controls Functional Differentiation of Dendritic Cells in the Spleen and Intestine

Kanako L. Lewis; Michele L. Caton; Milena Bogunovic; Melanie Greter; Lucja T. Grajkowska; Dennis Ng; Apostolos Klinakis; Israel F. Charo; Steffen Jung; Jennifer L. Gommerman; Ivaylo I. Ivanov; Kang Liu; Miriam Merad; Boris Reizis

doi:https://doi.org/10.1016/j.immuni.2011.08.013

Notch2 Receptor Signaling Controls Functional Differentiation of Dendritic Cells in the Spleen and Intestine

Kanako L. Lewis, Michele L. Caton, Milena Bogunovic, Melanie Greter, Lucja T. Grajkowska, Dennis Ng, Apostolos Klinakis, Israel F. Charo, Steffen Jung, Jennifer L. Gommerman, Ivaylo I. Ivanov, Kang Liu, Miriam Merad, Boris Reizis

Department of Systems Immunology

Weizmann Institute Of Science

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

Abstract

Dendritic cells (DCs) in tissues and lymphoid organs comprise distinct functional subsets that differentiate in situ from circulating progenitors. Tissue-specific signals that regulate DC subset differentiation are poorly understood. We report that DC-specific deletion of the Notch2 receptor caused a reduction of DC populations in the spleen. Within the splenic CD11b(+) DC subset, Notch signaling blockade ablated a distinct population marked by high expression of the adhesion molecule Esam. The Notch-dependent Esamh DC subset required lymphotoxin beta receptor signaling, proliferated in situ, and facilitated CD4(+) T cell priming. The Notch-independent Esam(lo) DCs expressed monocyte-related genes and showed superior cytokine responses. In addition, Notch2 deletion led to the loss of CD11b(+)CD103(+) DCs in the intestinal lamina propria and to a corresponding decrease of IL-17-producing CD4(+) T cells in the intestine. Thus, Notch2 is a common differentiation signal for T cell-priming CD11b(+) DC subsets in the spleen and intestine.

Original language	English
Pages (from-to)	780-791
Number of pages	12
Journal	Immunity
Volume	35
Issue number	5
DOIs	https://doi.org/10.1016/j.immuni.2011.08.013
State	Published - Nov 2011

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Lewis, K. L., Caton, M. L., Bogunovic, M., Greter, M., Grajkowska, L. T., Ng, D., Klinakis, A., Charo, I. F., Jung, S., Gommerman, J. L., Ivanov, I. I., Liu, K., Merad, M., & Reizis, B. (2011). Notch2 Receptor Signaling Controls Functional Differentiation of Dendritic Cells in the Spleen and Intestine. Immunity, 35(5), 780-791. https://doi.org/10.1016/j.immuni.2011.08.013

@article{68510a8b610844288a39e93659ab33f7,

title = "Notch2 Receptor Signaling Controls Functional Differentiation of Dendritic Cells in the Spleen and Intestine",

abstract = "Dendritic cells (DCs) in tissues and lymphoid organs comprise distinct functional subsets that differentiate in situ from circulating progenitors. Tissue-specific signals that regulate DC subset differentiation are poorly understood. We report that DC-specific deletion of the Notch2 receptor caused a reduction of DC populations in the spleen. Within the splenic CD11b(+) DC subset, Notch signaling blockade ablated a distinct population marked by high expression of the adhesion molecule Esam. The Notch-dependent Esamh DC subset required lymphotoxin beta receptor signaling, proliferated in situ, and facilitated CD4(+) T cell priming. The Notch-independent Esam(lo) DCs expressed monocyte-related genes and showed superior cytokine responses. In addition, Notch2 deletion led to the loss of CD11b(+)CD103(+) DCs in the intestinal lamina propria and to a corresponding decrease of IL-17-producing CD4(+) T cells in the intestine. Thus, Notch2 is a common differentiation signal for T cell-priming CD11b(+) DC subsets in the spleen and intestine.",

author = "Lewis, {Kanako L.} and Caton, {Michele L.} and Milena Bogunovic and Melanie Greter and Grajkowska, {Lucja T.} and Dennis Ng and Apostolos Klinakis and Charo, {Israel F.} and Steffen Jung and Gommerman, {Jennifer L.} and Ivanov, {Ivaylo I.} and Kang Liu and Miriam Merad and Boris Reizis",

note = "American Asthma Foundation; NIH [AI072571, DK085329, AI007161, HD055165]; CIHR/IRSC [67157]We thank U. Klein, A. Efstratiadis, F. Radtke, T. Gridley, and W. Pear for mouse strains; A. Capobianco, D. Lin, and A. Ferrante for animal donations; M. Lahoud for antibodies; and J. Ericson for Immgen data. Supported by the American Asthma Foundation (B.R.), NIH grants AI072571 (B.R.) and DK085329 (I.I.I.), NIH training grants AI007161 (K.L.L.) and HD055165 (M.L.C.), and CIHR/IRSC award MOP #67157 (J.L.G.).",

year = "2011",

month = nov,

doi = "https://doi.org/10.1016/j.immuni.2011.08.013",

language = "الإنجليزيّة",

volume = "35",

pages = "780--791",

journal = "Immunity",

issn = "1074-7613",

publisher = "Cell Press",

number = "5",

}

TY - JOUR

T1 - Notch2 Receptor Signaling Controls Functional Differentiation of Dendritic Cells in the Spleen and Intestine

AU - Lewis, Kanako L.

AU - Caton, Michele L.

AU - Bogunovic, Milena

AU - Greter, Melanie

AU - Grajkowska, Lucja T.

AU - Ng, Dennis

AU - Klinakis, Apostolos

AU - Charo, Israel F.

AU - Jung, Steffen

AU - Gommerman, Jennifer L.

AU - Ivanov, Ivaylo I.

AU - Liu, Kang

AU - Merad, Miriam

AU - Reizis, Boris

N1 - American Asthma Foundation; NIH [AI072571, DK085329, AI007161, HD055165]; CIHR/IRSC [67157]We thank U. Klein, A. Efstratiadis, F. Radtke, T. Gridley, and W. Pear for mouse strains; A. Capobianco, D. Lin, and A. Ferrante for animal donations; M. Lahoud for antibodies; and J. Ericson for Immgen data. Supported by the American Asthma Foundation (B.R.), NIH grants AI072571 (B.R.) and DK085329 (I.I.I.), NIH training grants AI007161 (K.L.L.) and HD055165 (M.L.C.), and CIHR/IRSC award MOP #67157 (J.L.G.).

PY - 2011/11

Y1 - 2011/11

N2 - Dendritic cells (DCs) in tissues and lymphoid organs comprise distinct functional subsets that differentiate in situ from circulating progenitors. Tissue-specific signals that regulate DC subset differentiation are poorly understood. We report that DC-specific deletion of the Notch2 receptor caused a reduction of DC populations in the spleen. Within the splenic CD11b(+) DC subset, Notch signaling blockade ablated a distinct population marked by high expression of the adhesion molecule Esam. The Notch-dependent Esamh DC subset required lymphotoxin beta receptor signaling, proliferated in situ, and facilitated CD4(+) T cell priming. The Notch-independent Esam(lo) DCs expressed monocyte-related genes and showed superior cytokine responses. In addition, Notch2 deletion led to the loss of CD11b(+)CD103(+) DCs in the intestinal lamina propria and to a corresponding decrease of IL-17-producing CD4(+) T cells in the intestine. Thus, Notch2 is a common differentiation signal for T cell-priming CD11b(+) DC subsets in the spleen and intestine.

AB - Dendritic cells (DCs) in tissues and lymphoid organs comprise distinct functional subsets that differentiate in situ from circulating progenitors. Tissue-specific signals that regulate DC subset differentiation are poorly understood. We report that DC-specific deletion of the Notch2 receptor caused a reduction of DC populations in the spleen. Within the splenic CD11b(+) DC subset, Notch signaling blockade ablated a distinct population marked by high expression of the adhesion molecule Esam. The Notch-dependent Esamh DC subset required lymphotoxin beta receptor signaling, proliferated in situ, and facilitated CD4(+) T cell priming. The Notch-independent Esam(lo) DCs expressed monocyte-related genes and showed superior cytokine responses. In addition, Notch2 deletion led to the loss of CD11b(+)CD103(+) DCs in the intestinal lamina propria and to a corresponding decrease of IL-17-producing CD4(+) T cells in the intestine. Thus, Notch2 is a common differentiation signal for T cell-priming CD11b(+) DC subsets in the spleen and intestine.

U2 - https://doi.org/10.1016/j.immuni.2011.08.013

DO - https://doi.org/10.1016/j.immuni.2011.08.013

M3 - مقالة

SN - 1074-7613

VL - 35

SP - 780

EP - 791

JO - Immunity

JF - Immunity

IS - 5

ER -

Notch2 Receptor Signaling Controls Functional Differentiation of Dendritic Cells in the Spleen and Intestine

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