Targeting Indoleamine 2,3-Dioxygenase in Cancer Models Using the Novel Small Molecule Inhibitor NTRC 3883-0

Overview

Journal Front Immunol

Specialty Allergy & Immunology

Date 2021 Feb 15

PMID 33584686

Citations 12

Authors

Yvonne Grobben

Jos de Man

Antoon M van Doornmalen

Michelle Muller

Nicole Willemsen-Seegers

Diep Vu-Pham

Winfried R Mulder

Martine B W Prinsen

Joeri de Wit

Jan Gerard Sterrenburg

Freek van Cauter

Judith E den Ouden

Anne M Van Altena

Leon F Massuger

Joost C M Uitdehaag

Rogier C Buijsman

Guido J R Zaman

Affiliations

Soon will be listed here.

Abstract

Indoleamine 2,3-dioxygenase (IDO1) is a key regulator of immune suppression by catalyzing the oxidation of L-tryptophan. IDO1 expression has been related to poor prognosis in several cancers and to resistance to checkpoint immunotherapies. We describe the characterization of a novel small molecule IDO1 inhibitor, NTRC 3883-0, in a panel of biochemical and cell-based assays, and various cancer models. NTRC 3883-0 released the inhibitory effect of IDO1 on CD8-positive T cell proliferation in co-cultures of IDO1-overexpressing cells with healthy donor lymphocytes, demonstrating its immune modulatory activity. In a syngeneic mouse model using IDO1-overexpressing B16F10 melanoma cells, NTRC 3883-0 effectively counteracted the IDO1-induced modulation of L-tryptophan and L-kynurenine levels, demonstrating its target modulation. Finally, we studied the expression and activity of IDO1 in primary cell cultures established from the malignant ascites of ovarian cancer patients. In these cultures, IDO1 expression was induced upon stimulation with IFNγ, and its activity could be inhibited by NTRC 3883-0. Based on these results, we propose the use of ascites cell-based functional assays for future patient stratification. Our results are discussed in light of the recent discontinuation of clinical trials of more advanced IDO1 inhibitors and the reconsideration of IDO1 as a valid drug target.

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