Anti-Inflammatory Effects of LJP 1586 [Z-3-Fluoro-2-(4-methoxybenzyl)allylamine Hydrochloride], an Amine-Based Inhibitor of Semicarbazide-Sensitive Amine Oxidase Activity

doi:10.1124/jpet.107.131672

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Journal of Pharmacology And Experimental Therapeutics Fast Forward
First published on November 9, 2007; DOI: 10.1124/jpet.107.131672

0022-3565/08/3242-867-875$20.00
JPET 324:867-875, 2008

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INFLAMMATION, IMMUNOPHARMACOLOGY, AND ASTHMA

Anti-Inflammatory Effects of LJP 1586 [Z-3-Fluoro-2-(4-methoxybenzyl)allylamine Hydrochloride], an Amine-Based Inhibitor of Semicarbazide-Sensitive Amine Oxidase Activity

Anne M. O'Rourke, Eric Y. Wang, Andrew Miller, Erika M. Podar, Kelly Scheyhing, Li Huang, Christina Kessler, Hongfeng Gao, Huong-Thu Ton-Nu, Mary T. MacDonald, David S. Jones, and Matthew D. Linnik

La Jolla Pharmaceutical Company, San Diego, California

Semicarbazide-sensitive amine oxidase (SSAO, amine oxidase,copper-containing 3, and vascular adhesion protein-1) is a copper-containingenzyme that catalyzes the oxidative deamination of primary aminesto an aldehyde, ammonia, and hydrogen peroxide. SSAO is alsoinvolved in leukocyte migration to sites of inflammation, andthe enzymatic activity of SSAO is essential to this role. Thus,inhibition of SSAO enzyme activity represents a target for thedevelopment of small molecule anti-inflammatory compounds. Here,we have characterized the novel SSAO inhibitor, Z-3-fluoro-2-(4-methoxybenzyl)allylaminehydrochloride (LJP 1586), and assessed its anti-inflammatoryactivity. LJP 1586 is a potent inhibitor of rodent and humanSSAO activity, with IC₅₀ values between 4 and 43 nM. The selectivityof LJP 1586 was confirmed with a broad panel of receptors andenzymes that included the monoamine oxidases A and B. Oral administrationof LJP 1586 resulted in complete inhibition of rat lung SSAO,with an ED₅₀ between 0.1 and 1 mg/kg, and a pharmacodynamichalf-life of greater than 24 h. In a mouse model of inflammatoryleukocyte trafficking oral dosing with LJP 1586 resulted insignificant dose-dependent inhibition of neutrophil accumulation,with an effect comparable to that of anti-leukocyte function-associatedantigen-1 antibody. In a rat model of LPS-induced lung inflammation,administration of 10 mg/kg LJP 1586 resulted in a 55% significantreduction in transmigrated cells recovered by bronchoalveolarlavage. The results demonstrate that a selective, orally activesmall molecule inhibitor of SSAO is an effective anti-inflammatorycompound in vivo and provide further support for SSAO as a therapeuticanti-inflammatory target.

Received September 13, 2007; accepted November 8, 2007.

Address correspondence to: Anne M. O'Rourke, La Jolla Pharmaceutical Company, 6455 Nancy Ridge Drive, San Diego, CA 92121. E-mail: anne.orourke{at}ljpc.com