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对恶性细胞具有选择性毒性的细胞毒性3,5-双(亚苄基)哌啶-4-酮和N-酰基类似物。

Cytotoxic 3,5-bis(benzylidene)piperidin-4-ones and N-acyl analogs displaying selective toxicity for malignant cells.

作者信息

Pati Hari N, Das Umashankar, Quail J Wilson, Kawase Masami, Sakagami Hiroshi, Dimmock Jonathan R

机构信息

College of Pharmacy and Nutrition, University of Saskatchewan, 110 Science Place, Saskatoon Saskatchewan S7N 5C9, Canada.

出版信息

Eur J Med Chem. 2008 Jan;43(1):1-7. doi: 10.1016/j.ejmech.2007.03.010. Epub 2007 Apr 3.

Abstract

A series of 3,5-bis(benzylidene)piperidin-4-ones 1, 1-acryloyl-3,5-bis(benzylidene)piperidin-4-ones 2 and adducts of 2 with sodium 2-mercaptoethanesulfonate (mesna), namely series 3, were prepared as candidate cytotoxic agents. These compounds were examined against neoplastic HSC-2, HSC-4 and HL-60 cells as well as HGF, HPC and HPLF normal cell lines and many of the compounds displayed selective toxicity for malignant cells. The CC50 values of the analogs in series 2 towards the cancer cell lines were mainly submicromolar. The relative potencies, selectivity and logP values were in the order of 2>1>3. The sulfonic acid group of a representative compound in series 3 was replaced by a thiol function to produce 4 leading to substantial increases in cytotoxic potencies and hydrophobicity indicating that the presence of a hydrophilic sulfonic acid group was disadvantageous in terms of potency. Molecular modeling suggested that the superior cytotoxicity of various members of series 1-3 over an acyclic analog 5 may have been due to the greater torsion angles theta1 and theta2 created between the arylidene aryl rings and the adjacent olefinic groups in series 1-3.

摘要

制备了一系列3,5-双(亚苄基)哌啶-4-酮1、1-丙烯酰基-3,5-双(亚苄基)哌啶-4-酮2以及2与2-巯基乙磺酸钠(美司钠)的加合物,即系列3,作为候选细胞毒性剂。对这些化合物针对肿瘤性HSC-2、HSC-4和HL-60细胞以及HGF、HPC和HPLF正常细胞系进行了检测,许多化合物对恶性细胞表现出选择性毒性。系列2中类似物对癌细胞系的CC50值主要为亚微摩尔级。相对效力、选择性和logP值的顺序为2>1>3。将系列3中代表性化合物的磺酸基团替换为硫醇官能团以生成4,导致细胞毒性效力和疏水性大幅增加,这表明亲水性磺酸基团的存在对效力不利。分子建模表明,系列1-3的各种成员相对于无环类似物5具有更高的细胞毒性,可能是由于系列1-3中芳叉基芳环与相邻烯基之间产生了更大的扭转角θ1和θ2。

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