口服生物可利用的肝脏选择性硬脂酰辅酶A去饱和酶(SCD)抑制剂。
Orally bioavailable, liver-selective stearoyl-CoA desaturase (SCD) inhibitors.
作者信息
Koltun Dmitry O, Vasilevich Natalya I, Parkhill Eric Q, Glushkov Andrei I, Zilbershtein Timur M, Mayboroda Elena I, Boze Melanie A, Cole Andrew G, Henderson Ian, Zautke Nathan A, Brunn Sandra A, Chu Nancy, Hao Jia, Mollova Nevena, Leung Kwan, Chisholm Jeffrey W, Zablocki Jeff
机构信息
Department of Medicinal Chemistry, CV Therapeutics, Inc, Palo Alto, CA 94304, USA.
出版信息
Bioorg Med Chem Lett. 2009 Jun 1;19(11):3050-3. doi: 10.1016/j.bmcl.2009.04.004. Epub 2009 Apr 8.
We discovered a structurally novel SCD (Delta9 desaturase) inhibitor 4a (CVT-11,563) that has 119 nM potency in a human cell-based (HEPG2) SCD assay and selectivity against Delta5 and Delta6 desaturases. This compound has 90% oral bioavailability (rat) and excellent plasma exposure (dAUC 935 ng h/mL). Additionally, 4a shows moderately selective liver distribution (three times vs plasma and adipose tissue) and relatively low brain penetration. In a five-day study (high sucrose diet, rat) compound 4a significantly reduced SCD activity as determined by GC analysis of fatty acid composition in plasma and liver. We describe the discovery of 4a from HTS hit 1 followed by scaffold replacement and SAR studies focused on DMPK properties.
我们发现了一种结构新颖的硬脂酰辅酶A去饱和酶(Delta9去饱和酶)抑制剂4a(CVT-11,563),它在基于人细胞(HEPG2)的硬脂酰辅酶A去饱和酶检测中具有119 nM的效力,并且对Delta5和Delta6去饱和酶具有选择性。该化合物具有90%的口服生物利用度(大鼠)和出色的血浆暴露量(药时曲线下面积为935 ng h/mL)。此外,4a显示出适度的肝脏选择性分布(相对于血浆和脂肪组织为三倍)以及相对较低的脑渗透。在一项为期五天的研究(高蔗糖饮食,大鼠)中,通过气相色谱分析血浆和肝脏中的脂肪酸组成确定,化合物4a显著降低了硬脂酰辅酶A去饱和酶的活性。我们描述了从高通量筛选命中物1开始发现4a的过程,随后进行了支架替换以及专注于药物代谢动力学性质的构效关系研究。
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