This study investigated the potential of targeting the enzyme kynurenine monooxygenase (KMO) as a novel non-hormonal therapy for endometriosis. The key findings are:
KMO is expressed in epithelial cells of human endometriosis lesions and in corresponding lesions in a mouse model of endometriosis.
Oral administration of the KMO inhibitor KNS898 in mice resulted in a dose-dependent inhibition of KMO activity, as evidenced by increased levels of the KMO substrate kynurenine and its metabolite kynurenic acid, and decreased levels of the cytotoxic metabolite 3-hydroxykynurenine.
In the mouse model of endometriosis, KMO inhibition with KNS898 reduced the number of endometriosis-like lesions that developed, even when treatment was started one week after the initiation of lesions.
KMO inhibition also improved visceral hyperalgesia (reduced mechanical allodynia) and restored normal cage exploration behavior in mice with endometriosis, suggesting an improvement in pain-related symptoms.
The histopathology of the experimental endometriosis lesions was similar to that observed in human endometriosis, and KMO expression was localized to the epithelial layers of the lesions in both human and mouse samples.
In conclusion, these results indicate that KMO inhibition is a promising new non-hormonal therapeutic approach for the treatment of endometriosis, as it can reduce lesion development and improve pain-related symptoms in a preclinical model.
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by Higgins,B., ... a las www.biorxiv.org 05-15-2024
https://www.biorxiv.org/content/10.1101/2024.05.13.593856v1Consultas más profundas