2018
DOI: 10.1158/1535-7163.mct-17-1104
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Characterization of the Selective Indoleamine 2,3-Dioxygenase-1 (IDO1) Catalytic Inhibitor EOS200271/PF-06840003 Supports IDO1 as a Critical Resistance Mechanism to PD-(L)1 Blockade Therapy

Abstract: Tumors use indoleamine 2,3-dioxygenase-1 (IDO1) as a major mechanism to induce an immunosuppressive microenvironment. IDO1 expression is upregulated in many cancers and considered to be a resistance mechanism to immune checkpoint therapies. IDO1 is induced in response to inflammatory stimuli such as IFNg and promotes immune tolerance by depleting tryptophan and producing tryptophan catabolites, including kynurenine, in the tumor microenvironment. This leads to effector T-cell anergy and enhanced T reg function… Show more

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Cited by 72 publications
(51 citation statements)
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“…As positive control demonstrating the repressive effect of the IDO1 product kynurenine, we show that treatment of PBMC cultures with kynurenine significantly inhibited CD4 + and CD8 + T cell proliferation (Fig. S3A, B), in line with its documented repressive effect on T cells [74][75][76].…”
Section: Rescue Of T Cell Proliferation Upon Pharmacological Inhibitisupporting
confidence: 64%
“…As positive control demonstrating the repressive effect of the IDO1 product kynurenine, we show that treatment of PBMC cultures with kynurenine significantly inhibited CD4 + and CD8 + T cell proliferation (Fig. S3A, B), in line with its documented repressive effect on T cells [74][75][76].…”
Section: Rescue Of T Cell Proliferation Upon Pharmacological Inhibitisupporting
confidence: 64%
“…Anti-PD1 therapy is, to date, one of the most effective anticancer immunotherapies. Despite this success, a significant number of patients develop, or will develop, resistance to this therapy [2][3][4][5] . Innate resistance to anti-PD1 therapy is found in 60% of melanoma patients 6 , and 25% develop resistance after an initial phase of objective response 7 .…”
Section: Introductionmentioning
confidence: 99%
“…96 In several preclinical tumor models in mice, PF-06840003 strongly reduced intratumoral Kyn levels and inhibited tumor growth in both monotherapy and, with an increased efficacy, in combinatorial regimens with PD-L1 or CTLA4 blockers. 97 Recently, BGB-5777, a potent CNS-penetrating IDO1 inhibitor, enabled a durable survival benefit in a fraction of patients with advanced glioblastoma when combined with nivolumab and radiation therapy. 98,99…”
Section: Pf-06840003 and Bgs-5777mentioning
confidence: 99%