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Jadomycin B, an Aurora-B kinase inhibitor discovered through virtual screening

机译:通过虚拟筛选发现的Aurora-B激酶抑制剂Jadomycin B

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Aurora kinases have emerged as promising targets for cancer therapy because of their critical role in mitosis. These kinases are well-conserved in all eukaryotes, and IPL1 gene encodes the single Aurora kinase in budding yeast. In a virtual screening attempt, 22 compounds were identified from nearly 15,000 microbial natural products as potential smallmolecular inhibitors of human Aurora-B kinase. One compound, Jadomycin B, inhibits the growth of ipl1321 temperature-sensitive mutant more dramatically than wild-type yeast cells, raising the possibility that this compound is an Aurora kinase inhibitor. Further in vitro biochemical assay using purified recombinant human Aurora-B kinase shows that Jadomycin B inhibits Aurora-B activity in a dosedependent manner. Our results also indicate that Jadomycin B competes with ATP for the kinase domain, which is consistent with our docking prediction. Like other Aurora kinase inhibitors, Jadomycin B blocks the phosphorylation of histone H3 on Ser10 in vivo. We also present evidence suggesting that Jadomycin B induces apoptosis in tumor cells without obvious effects on cell cycle. All the results indicate that Jadomycin B is a new Aurora-B kinase inhibitor worthy of further investigation.
机译:由于Aurora激酶在有丝分裂中起关键作用,因此已成为有希望的癌症治疗靶标。这些激酶在所有真核生物中都是保守的,并且IPL1基因编码出芽酵母中的单个Aurora激酶。在一次虚拟筛选尝试中,从近15,000种微生物天然产物中鉴定出22种化合物是人Aurora-B激酶的潜在小分子抑制剂。一种化合物Jadomycin B比野生型酵母细胞更能抑制ipl1321温度敏感突变体的生长,从而增加了该化合物是Aurora激酶抑制剂的可能性。使用纯化的重组人Aurora-B激酶的进一步体外生化分析表明,Jadomycin B以剂量依赖性方式抑制Aurora-B活性。我们的结果还表明,Jadomycin B与ATP竞争激酶结构域,这与我们的对接预测一致。像其他Aurora激酶抑制剂一样,贾多霉素B会在体内阻断Ser10上组蛋白H3的磷酸化。我们还提供了证据表明贾多霉素B诱导肿瘤细胞凋亡,而对细胞周期没有明显影响。所有结果表明,贾多霉素B是一种新型的Aurora-B激酶抑制剂,值得进一步研究。

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