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Targeting VDAC-bound hexokinase II: A promising approach for concomitant anti-cancer therapy

机译:靶向VDAC结合的己糖激酶II:伴随抗癌治疗的有前途的方法

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Introduction: Enhancement of glucose metabolism and repression of oxidative phosphorylation followed by the Warburg effect is the common hallmark of cancer cells. Hexokinase II (HKII) plays a dual role-first, HKII up-regulation results in increased glycolysis rates. Second, association of VDAC and HKII contributes to inhibition of apoptosis through repression of the formation of mitochondrial permeability transition pores. Areas covered: In this review, the role of HKII in evasion of apoptosis, aspects of HKII expression regulation, novel approaches targeting HKII and VDAC-HKII complexes and their application areas are discussed. Expert opinion: The dual role of HKII in cancer cells makes it an attractive target for anti-cancer therapy. Several agents, either synthetic or plant-derived, that target hexokinase and induce VDAC-HK complex dissociation have been identified to date. Targeting hexokinase, HK-VDAC complexes as well as other glycolytic proteins not only improves the efficacy of commonly used drugs. The most prominent benefit of this approach is the ability to overcome drug resistance, for example, to cisplatin or sorafenib. In some cases, it could create an insurmountable challenge for selection of appropriate therapy. Future studies and trials should address the issue of how to transfer these approaches into clinical practice.
机译:简介:增强葡萄糖代谢和抑制氧化磷酸化以及随后的Warburg效应是癌细胞的共同特征。己糖激酶II(HKII)首先扮演双重角色,HKII上调导致糖酵解速率增加。其次,VDAC和HKII的缔合通过抑制线粒体通透性过渡孔的形成而有助于抑制细胞凋亡。涵盖的领域:在这篇综述中,讨论了HKII在逃避凋亡中的作用,HKII表达调控的方面,靶向HKII和VDAC-HKII复合物的新方法及其应用领域。专家意见:HKII在癌细胞中的双重作用使其成为抗癌治疗的诱人靶标。迄今为止,已经鉴定了几种靶向己糖激酶并诱导VDAC-HK复合物解离的合成或植物来源的试剂。靶向己糖激酶,HK-VDAC复合物以及其他糖酵解蛋白不仅可以提高常用药物的功效。这种方法最显着的好处是能够克服对顺铂或索拉非尼的耐药性。在某些情况下,选择合适的疗法可能会带来难以克服的挑战。未来的研究和试验应解决如何将这些方法应用于临床的问题。

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