首页> 外文期刊>The Journal of investigative dermatology. >A Hexokinase 2 Modulator for Field-Directed Treatment of Experimental Actinic Keratoses
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A Hexokinase 2 Modulator for Field-Directed Treatment of Experimental Actinic Keratoses

机译:一种六酮酶2调节剂,用于实地导向治疗实验型光型角膜

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Overexpression of hexokinase 2, and its binding to VDAC1 on the outer mitochondrial membrane of cancer cells, is key to their metabolic reprogramming to aerobic glycolysis, which enables them to proliferate. We describe Comp-1, an allosteric small molecule that selectively detaches hexokinase 2 from the mitochondria. Detachment of hexokinase 2 reduces glycolysis and triggers apoptosis in cancer cells, without affecting hexokinase 1-expressing normal cells. The anti-cancer activity of Comp-1 was demonstrated in the UVB-damaged skin model in SKH-1 mice. Topical treatment with Comp-1 led to 70% reduction in lesion number and area. This in vivo efficacy was obtained without local skin reactions or other safety findings. Mechanism-related pharmacodynamic markers, including hexokinase 2 and cleaved caspase 3 levels, are affected by Comp-1 treatment in vivo. Good Laboratory Practice toxicology studies in minipigs for 28 days and 13 weeks established no systemic toxicities and minimal dermal reaction for once-daily application of up to 20% and 15% ointment strengths, respectively. Thus, Comp-1 may address a significant unmet medical need for a non-irritating efficacious topical actinic keratosis treatment.
机译:六酮酶2的过度表达及其与癌细胞外部线粒体膜上的Vdac1的结合,是它们代谢重编程对有氧糖溶解的关键,这使得它们能够增殖。我们描述了COMP-1,一种从线粒体选择性地分离六酮酶2的变构小分子。六酮酶2的脱离减少了糖酵解和触发癌细胞的细胞凋亡,而不影响表达六激酶1的正常细胞。在SKH-1小鼠的UVB受损的皮肤模型中证明了COMP-1的抗癌活性。具有COMP-1的局部处理导致病变数和区域减少了70%。在没有局部皮肤反应或其他安全结果的情况下获得体内疗效。有关的药效学标记,包括六酮酶2和切割的Caspase 3水平,受到体内COMP-1处理的影响。良好的实验室实践毒理学研究MINIPIGS 28天和13周,没有制定全身毒性,并且每天施用高达20%和15%的软膏强度的最小皮肤反应。因此,COMP-1可以解决对非刺激性局部局部光学角化症治疗的显着未满足的医疗需求。

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