He W, Huang F C, Hanney B, Souness J, Miller B, Liang G, Mason J, Djuric S
Department of Medicinal Chemistry, SW 8 Rhône-Poulenc Rorer Central Research, 500 Arcola Road, Collegeville, Pennsylvania 19426, USA.
J Med Chem. 1998 Oct 22;41(22):4216-23. doi: 10.1021/jm970575f.
The synthesis and biological activity of a novel series of 2, 2-disubstituted indan-1,3-dione-based PDE4 inhibitors are described. This structurally unique class of PDE4 inhibitors is markedly different from the known PDE4 inhibitors such as RP 73401 (2) and CDP 840 (3). Structure-activity relationship (SAR) studies led to the identification of inhibitors with nanomolar potency and oral activity in a murine endotoxemia model for TNF-alpha inhibition. Unlike other classical PDE4 inhibitors, several analogues were found to be nonemetic in a canine emesis model at intravenous doses of up to 3 mg/kg.
描述了一系列新型基于2,2 - 二取代茚满 - 1,3 - 二酮的PDE4抑制剂的合成及其生物活性。这类结构独特的PDE4抑制剂与已知的PDE4抑制剂如RP 73401(2)和CDP 840(3)明显不同。构效关系(SAR)研究使得在小鼠内毒素血症模型中鉴定出具有纳摩尔效力和口服活性以抑制TNF-α的抑制剂。与其他经典的PDE4抑制剂不同,在犬呕吐模型中,静脉注射剂量高达3 mg/kg时,发现几种类似物无催吐作用。
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