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Development of Noviomimetics that Modulate Molecular Chaperones and Manifest Neuroprotective Effects

机译:调节分子伴侣和明显神经保护作用的仿拟药物的开发。

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摘要

Heat shock protein 90 (Hsp90) is a chaperone under investigation for the treatment of cancer and neurodegenerative diseases. Neuroprotective Hsp90 C-terminal inhibitors derived from novobiocin (novologues) include KU-32 and KU-596. These novologues modulate molecular chaperones and result in an induction of Heat Shock Protein 70 (Hsp70). “Noviomimetics” replace the synthetically complex noviose sugar with a simple cyclohexyl moiety to maintain biological efficacy as compared to novologues KU-596 and KU-32. In this study, we further explore the development of noviomimetics and evaluate their efficacy using a luciferase refolding assay, immunoblot analysis, a c-jun assay, and an assay measuring mitochondrial bioenergetics. These new noviomimetics were designed and synthesized and were found to induce Hsp70 and result in improved biological activity. Noviomimetics >39e and >40a were found to potently induce Hsp70 and in very promising effects in cellular assays.
机译:热休克蛋白90(Hsp90)是一种正在研究中的用于治疗癌症和神经退行性疾病的伴侣蛋白。衍生自新霉素(novologues)的神经保护性Hsp90 C-末端抑制剂包括KU-32和KU-596。这些创新分子调节分子伴侣,并导致诱导热休克蛋白70(Hsp70)。与酚醛清毒剂KU-596和KU-32相比,“拟诺维药物”用一个简单的环己基部分取代了合成复杂的酚醛新糖,以保持生物学功效。在这项研究中,我们进一步探索仿拟药物的开发,并使用荧光素酶复性测定,免疫印迹分析,c-jun测定和测量线粒体生物能的测定来评估其功效。设计并合成了这些新的仿拟药物,并发现它们可诱导Hsp70并改善生物学活性。研究人员发现,仿拟药物> 39e 和> 40a 可以有效诱导Hsp70,并且在细胞分析中具有非常有希望的效果。

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