Author: Wang, Xuejian; Jing, Fanbo; Zhu, Huawei; Fang, Hao; Zhang, Jian; Xu, Wenfang
Title: Activity screening and structure–activity relationship of the hit compounds targeting APN/CD13 Cord-id: 031u33fy Document date: 2011_3_9
ID: 031u33fy
Snippet: Aminopeptidase N (APN) plays an important role in tumor progression, which participates in the progress such as proliferation, attachment, angiogenesis, and tumor invasion. All of this makes APN as a good chemical therapeutic antiâ€tumor target. In this study, a series of chemically synthesized APN inhibitors were tested for the antiâ€tumor activities, and three most effective compounds were chosen according to the MTT assay. Then, the enzyme inhibitory, antiâ€tumor, specificity, angiogenesis
Document: Aminopeptidase N (APN) plays an important role in tumor progression, which participates in the progress such as proliferation, attachment, angiogenesis, and tumor invasion. All of this makes APN as a good chemical therapeutic antiâ€tumor target. In this study, a series of chemically synthesized APN inhibitors were tested for the antiâ€tumor activities, and three most effective compounds were chosen according to the MTT assay. Then, the enzyme inhibitory, antiâ€tumor, specificity, angiogenesis, and invasion were determined to evaluate the activity of these three compounds. All compounds can markedly inhibit the enzyme activity of APN, angiogenesis of endothelial cells, and the invasion of ESâ€2 cells. And it had little effect on the viability of K562 which express low level of APN. This data indicated that the tested compounds were APN hit compounds. We also did kinetic assay to determine the inhibition constant and constructed a threeâ€dimensional quantitative structure–activity relationship model to analyze the structure–activity relationship to direct the further design of novel APN inhibitors as antiâ€tumor agents. These data demonstrate that the tested compounds can be developed as novel candidates of anticancer agent.
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