SUMMARY
Endometriosis is a common and debilitating neuro-inflammatory disorder that is associated with chronic pain. Definitive diagnosis is based on the presence of endometrial-like tissue (lesions) in sites outside the uterus. Kynurenine monooxygenase (KMO) is a mitochondrial enzyme of tryptophan metabolism that regulates inflammation and immunity. Here, we show that KMO is expressed in epithelial cells in human endometriosis tissue lesions and in corresponding lesions in a mouse model of endometriosis. In mice, oral treatment with the potent KMO inhibitor KNS898 induced a biochemical state of KMO blockade with accumulation of kynurenine, diversion to kynurenic acid and ablation of 3-hydroxykynurenine production. In the mouse model of endometriosis, KMO inhibition improved histological outcomes and endometriosis pain-like behaviours, even when KNS898 treatment commenced one week after initiation of lesions. Taken together, these results suggest that KMO blockade is a promising new non-hormonal therapeutic modality for endometriosis.
Competing Interest Statement
The following authors have interests to declare: S.P.W., D.J.M. are co-founders of Kynos Therapeutics Ltd. D.J.M. is a Board Member of Kynos. The University of Edinburgh controls Patents WO2015/091647, WO2016/097144, WO2016/188827 that relate to inhibitors of KMO inhibitors, and include the compound used in this paper. The remaining authors declare no competing interests
Footnotes
↵† Indicates senior authors.
Revised manuscript after peer review at eLife