Uludağ Damla, Bay Sadık, Sucu Bilgesu Onur, Şavluğ İpek Özgecan, Mohr Thomas, Güzel Mustafa, Karakaş Nihal
Cancer Research Center, Research Institute for Health Sciences and Technologies (SABITA), İstanbul Medipol University, İstanbul, Turkey.
Regenerative and Restorative Medicine Research Center (REMER), Research Institute for Health Sciences and Technologies (SABITA), İstanbul Medipol University, İstanbul, Turkey.
Front Pharmacol. 2022 May 23;13:828400. doi: 10.3389/fphar.2022.828400. eCollection 2022.
Change in the energy metabolism of cancer cells, which display significant differences compared to normal cells, is a rising phenomenon in developing new therapeutic approaches against cancers. One of the metabolic enzymes, hexokinase-II (HK-II) is involved in glycolysis, and inhibiting the HK-II activity may be a potential metabolic target for cancer therapy as most of the drugs in clinical use act on DNA damage. Methyl jasmonate (MJ) is one of the compounds blocking HK-II activity in cancer cells. In a previous study, we showed that the novel MJ analogs inhibit HK-II activity through VDAC detachment from the mitochondria. In this study, to evaluate the potential of targeting HK-2 activity, through patient cohort analysis, we first determined HK-2 expression levels and prognostic significance in highly lethal glioblastoma (GBM) brain tumor. We then examined the therapeutic effects of the novel analogs in the GBM cells. Here, we report that, among all, compound-10 (C-10) showed significant therapeutic efficacy as compared to MJ which is in use for preclinical and clinical studies. Afterward, we analyzed cell death triggered by C-10 in two different GBM cell lines. We found that C-10 treatment increased the apoptotic/necrotic cells and autophagy in GBM cells. The newly developed analog, C-10, was found to be lethal against GBM by the activation of cell death authorities, mostly in a necrotic and autophagic fashion at the early stages of the treatment. Considering that possibly decreased intracellular ATP levels by C-10 mediated inhibition of HK-2 activity and disabled VDAC interaction, a more detailed analysis of HK-2 inhibition-mediated cell death can provide a deep understanding of the mechanism of action on the oncosis/necroptosis axis. These findings provide an option to design clinically relevant and effective novel HK-II inhibitors and suggest novel MJ analogs to further study them as potential anticancer agents against GBM.
癌细胞的能量代谢与正常细胞相比存在显著差异,在开发新的癌症治疗方法中,这一现象日益受到关注。代谢酶之一的己糖激酶-II(HK-II)参与糖酵解,抑制HK-II活性可能是癌症治疗的一个潜在代谢靶点,因为目前临床使用的大多数药物作用于DNA损伤。茉莉酸甲酯(MJ)是一种能够阻断癌细胞中HK-II活性的化合物。在之前的一项研究中,我们表明新型MJ类似物通过使电压依赖性阴离子通道(VDAC)从线粒体上脱离来抑制HK-II活性。在本研究中,为了评估靶向HK-2活性的潜力,我们通过患者队列分析,首先确定了HK-2在高致死性胶质母细胞瘤(GBM)脑肿瘤中的表达水平及其预后意义。然后,我们研究了新型类似物对GBM细胞的治疗效果。在此,我们报告称,在所有药物中,与用于临床前和临床研究的MJ相比,化合物10(C-10)显示出显著的治疗效果。随后,我们分析了C-10在两种不同GBM细胞系中引发的细胞死亡。我们发现C-10处理增加了GBM细胞中的凋亡/坏死细胞以及自噬。新开发的类似物C-10被发现通过激活细胞死亡机制对GBM具有致死性,主要在治疗早期以坏死和自噬的方式起作用。考虑到C-10介导的HK-2活性抑制可能会降低细胞内ATP水平并破坏VDAC相互作用,对HK-2抑制介导的细胞死亡进行更详细的分析可以深入了解其对胀亡/坏死性凋亡轴的作用机制。这些发现为设计临床相关且有效的新型HK-II抑制剂提供了一个选择,并建议对新型MJ类似物进行进一步研究,以将其作为针对GBM的潜在抗癌药物。
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