Mitigation of cardiovascular toxicity in a series of CSF-1R inhibitors, and the identification of AZD7507

Bioorg Med Chem Lett. 2013 Aug 15;23(16):4591-6. doi: 10.1016/j.bmcl.2013.06.031.

David A Scott ¹, Les A Dakin, Kevin Daly, David J Del Valle, R Bruce Diebold, Lisa Drew, Jayachandran Ezhuthachan, Thomas W Gero, Claude A Ogoe, Charles A Omer, Sean P Redmond, Galina Repik, Kumar Thakur, Qing Ye, Xiaolan Zheng

Affiliations

Affiliation

1 AstraZeneca R&D Boston, Oncology iMED, 35 Gatehouse Drive, Waltham, MA 02451, USA. Electronic address: david.scott@astrazeneca.com.

PMID: 23842474 DOI: 10.1016/j.bmcl.2013.06.031

Abstract

The potent and selective 3-amido-4-anilinoquinoline CSF-1R inhibitor AZ683 suffered from cardiovascular liabilities, which were linked to the off-target activities of the compound and ion channel activity in particular. Less basic and less lipophilic examples from both the quinoline and cinnoline series demonstrated cleaner secondary pharmacology profiles. Cinnoline 31 retained the required potency and oral PK profile, and was progressed through the safety screening cascade to be nominated into development as AZD7507.

Keywords

CSF-1R; Inhibitor; Kinase.

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Description

Target

Research Area
HY-117244

AZD7507

99.45%, c-Fms抑制剂

c-Fms

Cancer

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MedChemExpress (MCE) 只为有资质的科研机构、医药企业基于科学研究或药证申报的用途提供医药研发服务，不为任何个人或者非科研性质的、非用于药证申报使用等其他用途提供服务。沪(浦)应急管危经许[2021]201709(QFYS)

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Mitigation of cardiovascular toxicity in a series of CSF-1R inhibitors, and the identification of AZD7507

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