Methyl-β-cyclodextrin (MβCD) reduces lysosomal cholesterol accumulation in Niemann-Pick disease type C1 (NPC1) patient fibroblasts. However, the pharmacological activity of MβCD 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 MβCDs, and the protein expression profiles of NPC1 patient fibroblasts after treatment with different sources of MβCDs. 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 MβCDs obtained from different batches and different sources. Furthermore, a proteomic analysis showed the differences of these three MβCD 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.

译文

:甲基-β-环糊精(MβCD)减少Niemann-Pick疾病C1型(NPC1)患者成纤维细胞中的溶酶体胆固醇蓄积。然而,不同实验室报道的MβCD的药理活性是不同的。为了确定这种变化的潜在原因,我们分析了三种MβCDs制剂的质谱特征,药理活性以及不同来源的MβCDs治疗后NPC1患者成纤维细胞的蛋白表达谱。我们的数据揭示了这三种制备自不同批次和不同来源的MβCD制剂在减少NPC1成纤维细胞中溶酶体胆固醇蓄积方面的不同质谱图和药理活性。此外,蛋白质组学分析显示了这三种MβCD制剂在改善NPC1细胞中蛋白质表达失调水平方面的差异。结果证明了在用作治疗剂之前预先筛选不同的环糊精制剂的重要性。质谱分析,药理活性测量和蛋白质组学分析相结合,为治疗应用中的环糊精表征提供了有效的分析程序。

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