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苯并吡喃酮类似物的细胞毒性及紫檀芪和苯并吡喃酮的代谢途径。

Cytotoxicity of phenylpironetin analogs and the metabolic fate of pironetin and phenylpironetin.

机构信息

Department of Medicinal Chemistry and Institute for Therapeutics Discovery and Development, College of Pharmacy, University of Minnesota, 717 Delaware Street SE, MN 55414, United States.

Department of Medicinal Chemistry and Institute for Therapeutics Discovery and Development, College of Pharmacy, University of Minnesota, 717 Delaware Street SE, MN 55414, United States.

出版信息

Bioorg Chem. 2022 Aug;125:105915. doi: 10.1016/j.bioorg.2022.105915. Epub 2022 May 27.

Abstract

To improve pironetin's metabolic stability we prepared four analogs by replacing its C12-14 segment with an aryl group. The antiproliferative activity of phenyl analog 4 was reduced two-fold and dihydroxy-4-fluorophenyl analog 5 was slightly more effective against OVCAR5 and A2780 ovarian cancer cell lines compared with the parent compound pironetin (1). The activity of 4-fluorophenyl analog 6 was reduced 3-fold in both cell lines. The activity of 7-O-methyl analog 7 was reduced 36-fold in OVCAR5 cells and 47-fold and A2780 cells, compared with pironetin. Phenylpironetin (4) was rapidly metabolized by mouse and human liver microsomes. We identified 17 human metabolites for phenyl analog 4 and 14 human metabolites for pironetin. Metabolism occurred at the C12-13 moiety, the α,β-unsaturated lactone and the side chains of the molecules (C6-C11 segments). The significant extent of oxidative metabolism suggests that it may not be possible to attain a metabolically stable pironetin analog by structural modifications of the parent compound.

摘要

为了提高皮罗替尼的代谢稳定性,我们通过用芳基取代其 C12-14 片段制备了四个类似物。苯类似物 4 的抗增殖活性降低了两倍,而二羟基-4-氟苯类似物 5 对 OVCAR5 和 A2780 卵巢癌细胞系的活性比母体化合物皮罗替尼(1)略高。4-氟苯类似物 6 在两种细胞系中的活性降低了 3 倍。7-O-甲基类似物 7 在 OVCAR5 细胞中的活性降低了 36 倍,在 A2780 细胞中的活性降低了 47 倍,与皮罗替尼相比。苯皮罗替尼(4)在小鼠和人肝微粒体中被迅速代谢。我们鉴定出苯类似物 4 的 17 个人类代谢物和皮罗替尼的 14 个人类代谢物。代谢发生在 C12-13 部分、α,β-不饱和内酯和分子的侧链(C6-C11 部分)上。氧化代谢的显著程度表明,通过母体化合物的结构修饰,可能无法获得代谢稳定的皮罗替尼类似物。

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