Full-length in meso structure and mechanism of rat kynurenine 3-monooxygenase inhibition

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作者
Shinya Mimasu
Hiroaki Yamagishi
Satoshi Kubo
Mie Kiyohara
Toshihiro Matsuda
Toshiko Yahata
Heather A. Thomson
Christopher D. Hupp
Julie Liu
Takao Okuda
Kenichi Kakefuda
机构
[1] Astellas Pharma. Inc.,Drug Discovery Research
[2] X-Chem Inc.,Electronic Materials Department
[3] Idemitsu Kosan Co.,Formulation, Tsukuba Laboratory
[4] Ltd.,undefined
[5] Civetta Therapeutics,undefined
[6] Nemoto Science Co.,undefined
[7] Ltd,undefined
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The structural mechanisms of single-pass transmembrane enzymes remain elusive. Kynurenine 3-monooxygenase (KMO) is a mitochondrial protein involved in the eukaryotic tryptophan catabolic pathway and is linked to various diseases. Here, we report the mammalian full-length structure of KMO in its membrane-embedded form, complexed with compound 3 (identified internally) and compound 4 (identified via DNA-encoded chemical library screening) at 3.0 Å resolution. Despite predictions suggesting that KMO has two transmembrane domains, we show that KMO is actually a single-pass transmembrane protein, with the other transmembrane domain lying laterally along the membrane, where it forms part of the ligand-binding pocket. Further exploration of compound 3 led to identification of the brain-penetrant compound, 5. We show that KMO is dimeric, and that mutations at the dimeric interface abolish its activity. These results will provide insight for the drug discovery of additional blood-brain-barrier molecules, and help illuminate the complex biology behind single-pass transmembrane enzymes.
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