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Cell-Based Identification of New IDO1 Modulator Chemotypes

机译:基于细胞的新IDO1调制器趋化型识别

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摘要

The immunoregulatory enzyme idoleamine-2,3-dioxygenase (IDO1) strengthens cancer immune escape, and inhibition of IDO1 by means of new chemotypes and mechanisms of action is considered a promising opportunity for IDO1 inhibitor discovery. IDO1 is a cofactor-binding, redox-sensitive protein, which calls for monitoring of IDO1 activity in its native cellular environment. We developed a new, robust fluorescence-based assay amenable to high throughput, which detects kynurenine in cells. Screening of a ca. 150 000-member compound library discovered unprecedented, potent IDO1 modulators with different mechanisms of action, including direct IDO1 inhibitors, regulators of IDO1 expression, and inhibitors of heme synthesis. Three IDO1-modulator chemotypes were identified that bind to apo-IDO1 and compete with the heme cofactor. Our new cell-based technology opens up novel opportunities for medicinal chemistry programs in immuno-oncology.
机译:免疫调节酶idoleamine-2,3-双加氧酶(IDO1)增强了癌症免疫逃逸,通过新的化学类型和作用机制抑制IDO1被认为是发现IDO1抑制剂的一个很有希望的机会。IDO1是一种辅因子结合的氧化还原敏感蛋白,需要在其固有的细胞环境中监测IDO1的活性。我们开发了一种新的、基于荧光的高通量检测方法,用于检测细胞中的犬尿氨酸。对一个约15万成员的化合物文库进行筛选,发现了前所未有的、有效的IDO1调节剂,具有不同的作用机制,包括直接IDO1抑制剂、IDO1表达调节剂和血红素合成抑制剂。确定了三种IDO1调节剂化学类型,它们与apo-IDO1结合并与血红素辅因子竞争。我们基于细胞的新技术为免疫肿瘤学的药物化学项目提供了新的机会。

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