Discovery of potent inhibitors of the lysophospholipase autotaxin

Discovery of potent inhibitors of the lysophospholipase autotaxin

[Display omitted] The autotaxin–lysophosphatidic acid (ATX–LPA) axis has been implicated in several disease conditions including inflammation, fibrosis and cancer. This makes ATX an attractive drug target and its inhibition may lead to useful therapeutic agents. Through a high throughput screen (HTS...

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Veröffentlicht in:Bioorganic & medicinal chemistry letters 2016-11, Vol.26 (22), p.5403-5410
Hauptverfasser: Shah, Pritom, Cheasty, Anne, Foxton, Caroline, Raynham, Tony, Farooq, Muddasar, Gutierrez, Irene Farre, Lejeune, Aurore, Pritchard, Michelle, Turnbull, Andrew, Pang, Leon, Owen, Paul, Boyd, Susan, Stowell, Alexandra, Jordan, Allan, Hamilton, Niall M., Hitchin, James R., Stockley, Martin, MacDonald, Ellen, Quesada, Mar Jimenez, Trivier, Elisabeth, Skeete, Jana, Ovaa, Huib, Moolenaar, Wouter H., Ryder, Hamish
Format: Artikel
Sprache:eng
Schlagworte:
Animals
Antineoplastic Agents - chemistry
Antineoplastic Agents - pharmacokinetics
Antineoplastic Agents - pharmacology
Autotaxin (ATX)
Cancer
Crystallography, X-Ray
Enzyme Inhibitors - chemistry
Enzyme Inhibitors - pharmacokinetics
Enzyme Inhibitors - pharmacology
Humans
Lysophosphatidic acid (LPA)
Lysophosphatidylcholine (LPC)
Lysophospholipase - antagonists & inhibitors
Lysophospholipase - metabolism
Lysophospholipids - metabolism
Mice
Molecular Docking Simulation
Molecular Targeted Therapy
Neoplasms - drug therapy
Neoplasms - enzymology
Phosphoric Diester Hydrolases - metabolism
Pyridines - chemistry
Pyridines - pharmacokinetics
Pyridines - pharmacology
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Zusammenfassung:[Display omitted] The autotaxin–lysophosphatidic acid (ATX–LPA) axis has been implicated in several disease conditions including inflammation, fibrosis and cancer. This makes ATX an attractive drug target and its inhibition may lead to useful therapeutic agents. Through a high throughput screen (HTS) we identified a series of small molecule inhibitors of ATX which have subsequently been optimized for potency, selectivity and developability properties. This has delivered drug-like compounds such as 9v (CRT0273750) which modulate LPA levels in plasma and are suitable for in vivo studies. X-ray crystallography has revealed that these compounds have an unexpected binding mode in that they do not interact with the active site zinc ions but instead occupy the hydrophobic LPC pocket extending from the active site of ATX together with occupying the LPA ‘exit’ channel.
ISSN:0960-894X
1464-3405
DOI:10.1016/j.bmcl.2016.10.036