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Design and Synthesis of Bouchardatine Derivatives as a Novel AMP-Activated Protein Kinase Activator for the Treatment of Colorectal Cancer

机译:新型AMP活化蛋白激酶激活剂Bouchardatine衍生物的设计与合成用于治疗结直肠癌

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摘要

Metabolic reprogramming is a crucial hallmark of tumorigenesis. Modulating the reprogrammed energy metabolism is an attractive anticancer therapeutic strategy. We previously found a natural product, bouchardatine, modulated aerobic metabolism and inhibited proliferation in the colorectal cancer cell (CRC). Herein, we designed and synthesized a new series of bouchardatine derivatives to discover more potential modulators. We applied the dual-parametric high-content screening (HCS) to evaluate their AMP-activated protein kinase (AMPK) modulation and CRC proliferation inhibition effect simultaneously. And we found their antiproliferation activities were highly correlated to AMPK activation. Among them, 18a was identified with nanomole-level antiproliferation activities against several CRCs. Interestingly, the evaluation found that 18a selectively upregulated oxidative phosphorylation (OXPHOS) and inhibited proliferation by modulating energy metabolism. Additionally, this compound effectively inhibited the RKO xenograft growth along with AMPK activation. In conclusion, our study identified 18a as a promising candidate for CRC treatment and suggested a novel anti-CRC strategy by AMPK activating and OXPHOS upregulating.
机译:代谢重编程是肿瘤发生的关键标志。调节重新编程的能量代谢是一种有吸引力的抗癌治疗策略。我们之前发现了一种天然产物,bouchardatine,调节有氧代谢并抑制结直肠癌细胞(CRC)的增殖。在此,我们设计并合成了一系列新的bouchardatine衍生物,以发现更多潜在的调节剂。采用双参数高内涵筛选(HCS)技术,同时评价其AMP活化蛋白激酶(AMPK)调节和CRC增殖抑制作用。我们发现它们的抗增殖活性与AMPK激活高度相关。其中,18a被鉴定为对几种CRCs具有纳米摩尔水平的抗增殖活性,有趣的是,评估发现18a选择性上调氧化磷酸化(OXPHOS)并通过调节能量代谢抑制增殖。此外,该化合物有效抑制了RKO异种移植物的生长以及AMPK的激活。总之,我们的研究将 18a 确定为有希望的 CRC 治疗候选者,并提出了一种通过激活 AMPK 和 OXPHOS 上调来治疗 CRC 的新型抗 CRC 策略。

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