Santos M Amélia, Marques Sérgio M, Tuccinardi Tiziano, Carelli Paolo, Panelli Laura, Rossello Armando
Centro de Química Estrutural, Instituto Superior Técnico, Rua Rovisco Pais 1, 1049-001 Lisboa, Portugal.
Bioorg Med Chem. 2006 Nov 15;14(22):7539-50. doi: 10.1016/j.bmc.2006.07.011. Epub 2006 Jul 27.
As the matrix metalloproteinases (MMPs) can be massively up-regulated in degenerative tissues and degrade the extracellular matrix, these key enzymes are promising targets for the therapy of cancer and other degenerative diseases. Here, we are presenting a series of new non-peptidic hydroxamate-based matrix metalloproteinase inhibitors, MMPIs, incorporating the iminodiacetic (IDA) hydroxamic acid scaffold, as mimics of truncated peptidic MMPIs. A series of alkylaryl and sulfonylaryl groups, on the IDA basic scaffold, was investigated with the aim of improving potency and selectivity against MMPs involved in degenerative diseases. The sulfonamide based IDA derivatives studied (compounds B1-B3) showed to be potent (nM range) against deep S1' pocket MMPs enzymes (i.e., MMP-2).
由于基质金属蛋白酶(MMPs)在退行性组织中可大量上调并降解细胞外基质,这些关键酶是癌症和其他退行性疾病治疗的有前景的靶点。在此,我们展示了一系列新的基于异羟肟酸的非肽类基质金属蛋白酶抑制剂(MMPIs),其包含亚氨基二乙酸(IDA)异羟肟酸支架,作为截短肽类MMPIs的模拟物。在IDA基本支架上研究了一系列烷基芳基和磺酰芳基基团,目的是提高对参与退行性疾病的MMPs的效力和选择性。所研究的基于磺酰胺的IDA衍生物(化合物B1 - B3)对深部S1'口袋MMPs酶(即MMP - 2)显示出强效(纳摩尔范围)。
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