赖氨酰氧化酶
化学
弹性蛋白
细胞外基质
酶
生物化学
纤维化
生物
遗传学
病理
医学
作者
Alison D. Findlay,Jonathan S. Foot,Alberto Buson,Mandar Deodhar,Andrew Jarnicki,Philip M. Hansbro,Gang Liu,Heidi Schilter,Craig I. Turner,Wenbin Zhou,Wolfgang Jarolimek
标识
DOI:10.1021/acs.jmedchem.9b01283
摘要
Lysyl oxidase-like 2 (LOXL2) is a secreted enzyme that catalyzes the formation of cross-links in extracellular matrix proteins, namely, collagen and elastin, and is indicated in fibrotic diseases. Herein, we report the identification and subsequent optimization of a series of indole-based fluoroallylamine inhibitors of LOXL2. The result of this medicinal chemistry campaign is PXS-5120A (12k), a potent, irreversible inhibitor that is >300-fold selective for LOXL2 over LOX. PXS-5120A also shows potent inhibition of LOXL3, an emerging therapeutic target for lung fibrosis. Key to the development of this compound was the utilization of a compound oxidation assay. PXS-5120A was optimized to show negligible substrate activity in vitro for related amine oxidase family members, leading to metabolic stability. PXS-5120A, in a pro-drug form (PXS-5129A, 12o), displayed anti-fibrotic activity in models of liver and lung fibrosis, thus confirming LOXL2 as an important target in diseases where collagen cross-linking is implicated.
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