Structure-based optimization of type III indoleamine 2,3-dioxygenase 1 (IDO1) inhibitors

被引:2
|
作者
Roehrig, Ute F. [1 ]
Majjigapu, Somi Reddy [1 ,2 ]
Vogel, Pierre [2 ]
Reynaud, Aline [3 ]
Pojer, Florence [3 ]
Dilek, Nahzli [1 ]
Reichenbach, Patrick [4 ]
Ascencao, Kelly [1 ,6 ]
Irving, Melita [4 ]
Coukos, George [4 ]
Michielin, Olivier [1 ,5 ]
Zoete, Vincent [1 ,4 ]
机构
[1] SIB Swiss Inst Bioinformat, Mol Modeling Grp, CH-1015 Lausanne, Switzerland
[2] Ecole Polytech Fed Lausanne EPFL, Lab Glycochem & Asymmetr Synth, Lausanne, Switzerland
[3] Ecole Polytech Fed Lausanne EPFL, Prot Prod & Struct Core Facil, Sch Life Sci, Lausanne, Switzerland
[4] Dept Oncol UNIL CHUV, Ludwig Lausanne Branch, Epalinges, Switzerland
[5] Univ Hosp Lausanne CHUV, Dept Oncol, Ludwig Canc Res Lausanne Branch, CH-1011 Lausanne, Switzerland
[6] Univ Fribourg, Fac Sci & Med, Chair Pharmacol, Fribourg, Switzerland
关键词
Cancer immunotherapy; structure-based drug design; tryptophan metabolism; X-ray crystallography; IMIDAZOLEISOINDOLE DERIVATIVES; TRYPTOPHAN DEGRADATION; BIOLOGICAL EVALUATION; CRYSTAL-STRUCTURES; POTENT INHIBITORS; RATIONAL DESIGN; HIGHLY POTENT; DISCOVERY; PROTEIN; CYCLOADDITION;
D O I
10.1080/14756366.2022.2089665
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
The haem enzyme indoleamine 2,3-dioxygenase 1 (IDO1) catalyses the rate-limiting step in the kynurenine pathway of tryptophan metabolism and plays an essential role in immunity, neuronal function, and ageing. Expression of IDO1 in cancer cells results in the suppression of an immune response, and therefore IDO1 inhibitors have been developed for use in anti-cancer immunotherapy. Here, we report an extension of our previously described highly efficient haem-binding 1,2,3-triazole and 1,2,4-triazole inhibitor series, the best compound having both enzymatic and cellular IC50 values of 34 nM. We provide enzymatic inhibition data for almost 100 new compounds and X-ray diffraction data for one compound in complex with IDO1. Structural and computational studies explain the dramatic drop in activity upon extension to pocket B, which has been observed in diverse haem-binding inhibitor scaffolds. Our data provides important insights for future IDO1 inhibitor design.
引用
收藏
页码:1773 / 1811
页数:39
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