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Analytical Characterization of Methyl-beta-Cyclodextrin for Pharmacological Activity to Reduce Lysosomal Cholesterol Accumulation in Niemann-Pick Disease Type C1 Cells

机译:药理活性甲基β-环糊精的分析表征,从而降低奈曼肝型C1细胞溶酶体胆固醇积累

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摘要

Methyl-beta-cyclodextrin (M beta CD) reduces lysosomal cholesterol accumulation in Niemann-Pick disease type C1 (NPC1) patient fibroblasts. However, the pharmacological activity of M beta CD reported by different laboratories varies. To determine the potential causes of this variation, we analyzed the mass spectrum characteristics, pharmacological activity of three preparations of M beta CDs, and the protein expression profiles of NPC1 patient fibroblasts after treatment with different sources of M beta CDs. Our data revealed varied mass spectrum profiles and pharmacological activities on the reduction of lysosomal cholesterol accumulation in NPC1 fibroblasts for these three preparations of M beta CDs obtained from different batches and different sources. Furthermore, a proteomic analysis showed the differences of these three M beta CD preparations on amelioration of dysregulated protein expression levels in NPC1 cells. The results demonstrate the importance of prescreening of different cyclodextrin preparations before use as a therapeutic agent. A combination of mass spectrum analysis, measurement of pharmacological activity, and proteomic profiling provides an effective analytical procedure for characterization of cyclodextrins for therapeutic applications.
机译:甲基 - β-环糊精(MβCD)降低了奈曼肝型C1(NPC1)患者成纤维细胞中的溶酶体胆固醇积累。然而,不同实验室报道的MβCD的药理活性变化。为了确定这种变化的潜在原因,我们分析了MβCds的三种制剂的质谱特性,三种制剂的药理活性,以及​​用不同来源的MβCds处理后NPC1患者成纤维细胞的蛋白表达谱。我们的数据揭示了多种质谱谱和药理学活性,关于从不同批次和不同来源获得的MβCd的这三种制剂的NPC1成纤维细胞中溶酶体胆固醇积累的减少。此外,蛋白质组学分析显示了这三种βCd制剂对NPC1细胞中具有疑难蛋白表达水平的改善的差异。结果证明了在用作治疗剂之前使用不同环糊精制剂的预算。质谱分析,药理活性测量和蛋白质组学分析的组合提供了一种有效的分析方法,用于治疗应用的环糊精。

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