Small-molecule factor B inhibitor for the treatment of complement-mediated diseases.
Anna SchubartKaren AndersonNello MainolfiHolger SellnerTakeru EharaChristopher M AdamsAengus Mac SweeneySha-Mei LiaoMaura CrowleyAmanda Littlewood-EvansSophie SarretGrazyna WieczorekLudovic PerrotValérie DubostThierry FlandreYuzhou ZhangRichard J H SmithAntonio M RisitanoRajeshri G KarkiChun ZhangEric ValeurFinton SirockinBernd GerhartzPaulus ErbelNicola HughesThomas M SmithFrederic CuminUpendra A ArgikarBörje HaraldssonMuneto MogiRichard SedraniChristian WiesmannBruce JaffeeJürgen MaibaumStefanie FlohrRichard HarrisonJoerg EderPublished in: Proceedings of the National Academy of Sciences of the United States of America (2019)
Dysregulation of the alternative complement pathway (AP) predisposes individuals to a number of diseases including paroxysmal nocturnal hemoglobinuria, atypical hemolytic uremic syndrome, and C3 glomerulopathy. Moreover, glomerular Ig deposits can lead to complement-driven nephropathies. Here we describe the discovery of a highly potent, reversible, and selective small-molecule inhibitor of factor B, a serine protease that drives the central amplification loop of the AP. Oral administration of the inhibitor prevents KRN-induced arthritis in mice and is effective upon prophylactic and therapeutic dosing in an experimental model of membranous nephropathy in rats. In addition, inhibition of factor B prevents complement activation in sera from C3 glomerulopathy patients and the hemolysis of human PNH erythrocytes. These data demonstrate the potential therapeutic value of using a factor B inhibitor for systemic treatment of complement-mediated diseases and provide a basis for its clinical development.