| Literature DB >> 29111717 |
Stefano Crosignani1, Patrick Bingham2, Pauline Bottemanne1, Hélène Cannelle1, Sandra Cauwenberghs1, Marie Cordonnier1, Deepak Dalvie2, Frederik Deroose3, Jun Li Feng2, Bruno Gomes1, Samantha Greasley2, Stephen E Kaiser2, Manfred Kraus2, Michel Négrerie4, Karen Maegley2, Nichol Miller2, Brion W Murray2, Manfred Schneider1, James Soloweij2, Albert E Stewart2, Joseph Tumang2, Vince R Torti2, Benoit Van Den Eynde5, Martin Wythes2.
Abstract
Tumors use tryptophan-catabolizing enzymes such as indoleamine 2,3-dioxygenase (IDO-1) to induce an immunosuppressive environment. IDO-1 is induced in response to inflammatory stimuli and promotes immune tolerance through effector T-cell anergy and enhanced Treg function. As such, IDO-1 is a nexus for the induction of a key immunosuppressive mechanism and represents an important immunotherapeutic target in oncology. Starting from HTS hit 5, IDO-1 inhibitor 6 (EOS200271/PF-06840003) has been developed. The structure-activity relationship around 6 is described and rationalized using the X-ray crystal structure of 6 bound to human IDO-1, which shows that 6, differently from most of the IDO-1 inhibitors described so far, does not bind to the heme iron atom and has a novel binding mode. Clinical candidate 6 shows good potency in an IDO-1 human whole blood assay and also shows a very favorable ADME profile leading to favorable predicted human pharmacokinetic properties, including a predicted half-life of 16-19 h.Entities:
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Year: 2017 PMID: 29111717 DOI: 10.1021/acs.jmedchem.7b00974
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446