首页> 外文期刊>Journal of Alzheimer's disease: JAD >Intravenous anesthetic diazepam does not induce amyloid-beta peptide oligomerization but diazepam co-administered with halothane oligomerizes amyloid-beta peptide: an NMR study.
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Intravenous anesthetic diazepam does not induce amyloid-beta peptide oligomerization but diazepam co-administered with halothane oligomerizes amyloid-beta peptide: an NMR study.

机译:一项NMR研究表明,静脉麻醉药地西epa不会诱导淀粉样β肽寡聚,但与氟烷共同使用的地西epa会使淀粉样β肽低聚。

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Amyloid-beta peptide (Abeta) oligomerization has a profound role in Alzheimer's disease pathophysiology. Biophysical studies have shown that smaller sized inhaled anesthetics promote oligomerization by inducing perturbation of three critical amino acid residues (G29, A30, and I31) located in the helix-loop-helix domain of Abeta. In this present experimental study, using state-of-the-art nuclear magnetic resonance, we have monitored the influence of a larger sized intravenous anesthetic, diazepam, as well as diazepam co-administered with halothane, on Abeta. It was concluded that diazepam (in isolation) does not interact with the G29, A30, and I31 residues, and no Abeta oligomerization occurs in the presence of 0.101 mM diazepam, even after 63 days. However, when diazepam was co-administered with halothane, profound Abeta oligomerization is observed. These results strengthen the hypothesis that the presence of smaller molecular sized anesthetic is instrumental in promoting Abeta oligomerization even when co-administered with a larger sized anesthetic, namely diazepam.
机译:淀粉样蛋白β肽(Abeta)寡聚在阿尔茨海默氏病的病理生理学中具有重要作用。生物物理研究表明,较小尺寸的吸入麻醉药通过引起对Abeta螺旋-环-螺旋结构域中的三个关键氨基酸残基(G29,A30和I31)的扰动来促进寡聚。在本实验研究中,我们使用最先进的核磁共振技术,监测了较大剂量的静脉麻醉药地西epa以及与氟烷共同使用的地西epa对Abeta的影响。结论是,地西epa(单独)不与G29,A30和I31残基相互作用,即使存在63天,在存在0.101 mM地西epa的情况下也没有发生Abeta寡聚。但是,当地西epa与氟烷并用时,会观察到严重的Abeta低聚。这些结果加强了以下假设:即使与较大尺寸的麻醉剂(地西epa)同时使用,较小分子麻醉剂的存在也有助于促进Abe​​ta寡聚。

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