Matrix metalloproteinases (MMPs) have been the subject of intense research because of their roles in tumor metastasis and in the rise and spread of degenerative diseases such as osteo- and rheumatoid arthritis. A preliminary class of 140 druglike, small-molecule matrix metalloproteinase-3 inhibitors, intended as starting scaffolds for optimization and synthesis, has been designed in silico using a series of highly predictive three-dimensional quantitative structure-activity relationship models, including comparative molecular field analysis and comparative molecular similarity indices analysis, with docking and scoring. Thalidomide was chosen as the skeleton on which to base the new lead series, as it moderately inhibits MMP-3, is antiangiogenic, and lends itself easily to structural modifications. Most of the new compounds demonstrate medium to high predicted biological activity and good bioavailability as estimated by the octanol-water partition coefficient ClogP. Compound 102 in particular exhibits extremely favorable predicted activity against MMP-3; is moderately bioavailable; satisfies Lipinski's Rule of Five; and shows promise for further optimization, synthesis, and experimental evaluation as a potential adjunct anticancer or antirheumatic therapeutic.

译文

:基质金属蛋白酶(MMP)由于其在肿瘤转移中以及在变性疾病(例如骨和类风湿性关节炎)的发生和扩散中的作用而受到了广泛的研究。已在计算机上使用一系列高度预测的三维定量结构-活性关系模型(包括比较分子场)在计算机上设计了初步的140类药物样小分子基质金属蛋白酶3抑制剂,旨在作为优化和合成的起始支架。分析和比较分子相似性指数分析,以及对接和评分。选择沙利度胺作为新铅系列的基础,因为它能适度抑制MMP-3,具有抗血管生成作用,并易于进行结构修饰。正如辛醇-水分配系数ClogP所估计的那样,大多数新化合物都具有中等至较高的预测生物活性和良好的生物利用度。特别地,化合物102对MMP-3表现出非常有利的预测活性。具有中等生物利用度;满足Lipinski的五法则;并有望进一步优化,合成和进行实验评估,作为潜在的辅助抗癌药或抗风湿药。

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