A small-molecule inhibitor of lectin-like oxidized LDL receptor-1 acts by stabilizing an inactive receptor tetramer state

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作者
Gisela Schnapp
Heike Neubauer
Frank H. Büttner
Sandra Handschuh
Iain Lingard
Ralf Heilker
Klaus Klinder
Jürgen Prestle
Rainer Walter
Michael Wolff
Markus Zeeb
Francois Debaene
Herbert Nar
Dennis Fiegen
机构
[1] Boehringer Ingelheim Pharma GmbH & Co. KG,
[2] NovAliX,undefined
[3] BioParc,undefined
[4] Aptuit (Verona) Srl,undefined
[5] an Evotec Company,undefined
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The C-type lectin family member lectin-like oxidized LDL receptor-1 (LOX-1) has been object of intensive research. Its modulation may offer a broad spectrum of therapeutic interventions ranging from cardiovascular diseases to cancer. LOX-1 mediates uptake of oxLDL by vascular cells and plays an important role in the initiation of endothelial dysfunction and its progression to atherosclerosis. So far only a few compounds targeting oxLDL-LOX-1 interaction are reported with a limited level of characterization. Here we describe the identification and characterization of BI-0115, a selective small molecule inhibitor of LOX-1 that blocks cellular uptake of oxLDL. Identified by a high throughput screening campaign, biophysical analysis shows that BI-0115 binding triggers receptor inhibition by formation of dimers of the homodimeric ligand binding domain. The structure of LOX-1 bound to BI-0115 shows that inter-ligand interactions at the receptor interfaces are key to the formation of the receptor tetramer thereby blocking oxLDL binding.
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