Department of Chemistry, Roger Adams Laboratory, University of Illinois, Urbana, 61801, United States.
ACS Comb Sci. 2012 Jan 9;14(1):44-50. doi: 10.1021/co2001372. Epub 2011 Oct 28.
Procaspase-Activating Compound 1 (PAC-1) is an ortho-hydroxy N-acyl hydrazone that enhances the enzymatic activity of procaspase-3 in vitro and induces apoptosis in cancer cells. An analogue of PAC-1, called S-PAC-1, was evaluated in a veterinary clinical trial in pet dogs with lymphoma and found to have considerable potential as an anticancer agent. With the goal of identifying more potent compounds in this promising class of experimental therapeutics, a combinatorial library based on PAC-1 was created, and the compounds were evaluated for their ability to induce death of cancer cells in culture. For library construction, 31 hydrazides were condensed in parallel with 27 aldehydes to create 837 PAC-1 analogues, with an average purity of 91%. The compounds were evaluated for their ability to induce apoptosis in cancer cells, and through this work, six compounds were discovered to be substantially more potent than PAC-1 and S-PAC-1. These six hits were further evaluated for their ability to relieve zinc-mediated inhibition of procaspase-3 in vitro. In general, the newly identified hit compounds are two- to four-fold more potent than PAC-1 and S-PAC-1 in cell culture, and thus have promise as experimental therapeutics for treatment of the many cancers that have elevated expression levels of procaspase-3.
前胱冬酶激活化合物 1(PAC-1)是一种邻位羟基亚氨甲酰腙,它能增强体外前胱冬酶-3 的酶活性,并诱导癌细胞凋亡。PAC-1 的一种类似物,称为 S-PAC-1,在一项针对患有淋巴瘤的宠物犬的兽医临床试验中进行了评估,被发现具有作为抗癌剂的相当大的潜力。为了在这一有前途的实验治疗药物类别中确定更有效的化合物,我们创建了一个基于 PAC-1 的组合文库,并评估了这些化合物在培养的癌细胞中诱导死亡的能力。为了文库的构建,31 个腙与 27 个醛平行缩合,共合成了 837 个 PAC-1 类似物,平均纯度为 91%。我们评估了这些化合物诱导癌细胞凋亡的能力,通过这项工作,发现有 6 种化合物的活性明显强于 PAC-1 和 S-PAC-1。这 6 个命中化合物进一步评估了其在体外缓解锌介导的前胱冬酶-3 抑制的能力。总的来说,新鉴定的命中化合物在细胞培养中比 PAC-1 和 S-PAC-1 分别强 2 到 4 倍,因此有望作为治疗许多表达水平升高的前胱冬酶-3 的癌症的实验治疗药物。
