首页> 外文期刊>Cancer biology & therapy >SU11248 (sunitinib) directly inhibits the activity of mammalian 5'-AMP-activated protein kinase (AMPK).
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SU11248 (sunitinib) directly inhibits the activity of mammalian 5'-AMP-activated protein kinase (AMPK).

机译:SU11248(舒尼替尼)直接抑制哺乳动物5'-AMP激活的蛋白激酶(AMPK)的活性。

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AMPK has been termed the fuel sensor of mammalian cells because it directly responds to the depletion of the fuel molecule ATP. In previous work, we found that AMPK is strongly activated by tumor-like hypoxia and glucose deprivation, independently of the oxygen response system associated with HIF-1. We also observed high levels of AMPK activity in tumor cells in vivo, using different model tumors. These findings suggested the hypothesis that modulation of AMPK activity could have therapeutic value for the treatment of solid tumors. To investigate this hypothesis, we have been conducting a SAR study of potential small-molecule modulators of AMPK activity. Here we report that the chemotherapeutic drug SU11248 (sunitinib) is at least as potent an inhibitor of AMPK as compound C, which is a commonly used experimental direct inhibitor of the enzyme. We also provide a computational model of the binding pose of SU11248 to an AMPKalpha subunit, which suggests a structural basis for the affinity of the drug for the ATP site of the catalytic domain. The ability of SU11248 to inhibit AMPK has potential clinical significance--there may be populations of SU11248-treated patients in which AMPK activity is inhibited in normal as well as in tumor tissue.
机译:AMPK被称为哺乳动物细胞的燃料传感器,因为它直接响应燃料分子ATP的消耗。在以前的工作中,我们发现AMPK被类似肿瘤的缺氧和葡萄糖剥夺强烈激活,而与HIF-1相关的氧气反应系统无关。我们还观察到了使用不同模型肿瘤的体内肿瘤细胞中高水平的AMPK活性。这些发现提出了这样的假设,即AMPK活性的调节对于实体瘤的治疗可能具有治疗价值。为了研究该假设,我们一直在进行AMPK活性的潜在小分子调节剂的SAR研究。在这里,我们报道化学治疗药物SU11248(舒尼替尼)至少是AMPK的有效抑制剂,而AMPK是化合物C的常用实验直接抑制剂。我们还提供了SU11248与AMPKalpha亚基结合姿势的计算模型,这为药物对催化域ATP位点的亲和力提供了结构基础。 SU11248抑制AMPK的能力具有潜在的临床意义-可能有SU11248治疗的患者群体在正常以及肿瘤组织中均抑制了AMPK活性。

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