Co-inhibition of CD73 and A2AR Adenosine Signaling Improves Anti-tumor Immune Responses

Arabella Young; Shin Foong Ngiow; Deborah S. Barkauskas; Erin Sult; Carl Hay; Stephen J. Blake; Qihui Huang; Jing Liu; Kazuyoshi Takeda; Michele W.L. Teng; Kris Sachsenmeier; Mark J. Smyth

doi:10.1016/j.ccell.2016.06.025

Co-inhibition of CD73 and A2AR Adenosine Signaling Improves Anti-tumor Immune Responses

Arabella Young, Shin Foong Ngiow, Deborah S. Barkauskas, Erin Sult, Carl Hay, Stephen J. Blake, Qihui Huang, Jing Liu, Kazuyoshi Takeda, Michele W.L. Teng, Kris Sachsenmeier, Mark J. Smyth

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337 Citations (Scopus)

Abstract

Preclinical studies targeting the adenosinergic pathway have gained much attention for their clinical potential in overcoming tumor-induced immunosuppression. Here, we have identified that co-blockade of the ectonucleotidase that generates adenosine CD73 and the A2A adenosine receptor (A2AR) that mediates adenosine signaling in leuokocytes, by using compound gene-targeted mice or therapeutics that target these molecules, limits tumor initiation, growth, and metastasis. This tumor control requires effector lymphocytes and interferon-γ, while antibodies targeting CD73 promote an optimal therapeutic response in vivo when engaging activating Fc receptors. In a two-way mixed leukocyte reaction using a fully human anti-CD73, we demonstrated that Fc receptor binding augmented the production of proinflammatory cytokines.

Original language	English
Pages (from-to)	391-403
Number of pages	13
Journal	CANCER CELL
Volume	30
Issue number	3
DOIs	https://doi.org/10.1016/j.ccell.2016.06.025
Publication status	Published - 12 Sept 2016
Externally published	Yes

Keywords

CD73
adenosine
combination therapy
immunotherapy
tumor

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title = "Co-inhibition of CD73 and A2AR Adenosine Signaling Improves Anti-tumor Immune Responses",

abstract = "Preclinical studies targeting the adenosinergic pathway have gained much attention for their clinical potential in overcoming tumor-induced immunosuppression. Here, we have identified that co-blockade of the ectonucleotidase that generates adenosine CD73 and the A2A adenosine receptor (A2AR) that mediates adenosine signaling in leuokocytes, by using compound gene-targeted mice or therapeutics that target these molecules, limits tumor initiation, growth, and metastasis. This tumor control requires effector lymphocytes and interferon-γ, while antibodies targeting CD73 promote an optimal therapeutic response in vivo when engaging activating Fc receptors. In a two-way mixed leukocyte reaction using a fully human anti-CD73, we demonstrated that Fc receptor binding augmented the production of proinflammatory cytokines.",

keywords = "CD73, adenosine, combination therapy, immunotherapy, tumor",

author = "Arabella Young and Ngiow, {Shin Foong} and Barkauskas, {Deborah S.} and Erin Sult and Carl Hay and Blake, {Stephen J.} and Qihui Huang and Jing Liu and Kazuyoshi Takeda and Teng, {Michele W.L.} and Kris Sachsenmeier and Smyth, {Mark J.}",

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AU - Young, Arabella

AU - Ngiow, Shin Foong

AU - Barkauskas, Deborah S.

AU - Sult, Erin

AU - Hay, Carl

AU - Blake, Stephen J.

AU - Huang, Qihui

AU - Liu, Jing

AU - Takeda, Kazuyoshi

AU - Teng, Michele W.L.

AU - Sachsenmeier, Kris

AU - Smyth, Mark J.

PY - 2016/9/12

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N2 - Preclinical studies targeting the adenosinergic pathway have gained much attention for their clinical potential in overcoming tumor-induced immunosuppression. Here, we have identified that co-blockade of the ectonucleotidase that generates adenosine CD73 and the A2A adenosine receptor (A2AR) that mediates adenosine signaling in leuokocytes, by using compound gene-targeted mice or therapeutics that target these molecules, limits tumor initiation, growth, and metastasis. This tumor control requires effector lymphocytes and interferon-γ, while antibodies targeting CD73 promote an optimal therapeutic response in vivo when engaging activating Fc receptors. In a two-way mixed leukocyte reaction using a fully human anti-CD73, we demonstrated that Fc receptor binding augmented the production of proinflammatory cytokines.

AB - Preclinical studies targeting the adenosinergic pathway have gained much attention for their clinical potential in overcoming tumor-induced immunosuppression. Here, we have identified that co-blockade of the ectonucleotidase that generates adenosine CD73 and the A2A adenosine receptor (A2AR) that mediates adenosine signaling in leuokocytes, by using compound gene-targeted mice or therapeutics that target these molecules, limits tumor initiation, growth, and metastasis. This tumor control requires effector lymphocytes and interferon-γ, while antibodies targeting CD73 promote an optimal therapeutic response in vivo when engaging activating Fc receptors. In a two-way mixed leukocyte reaction using a fully human anti-CD73, we demonstrated that Fc receptor binding augmented the production of proinflammatory cytokines.

KW - CD73

KW - adenosine

KW - combination therapy

KW - immunotherapy

KW - tumor

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JO - CANCER CELL

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Co-inhibition of CD73 and A2AR Adenosine Signaling Improves Anti-tumor Immune Responses

Abstract

Keywords

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