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糖基化纳米颗粒伴侣比分子糖抑制蛋白质聚集和降低淀粉样毒性的效果好 10-100 倍。

Sugar-Terminated Nanoparticle Chaperones Are 10-10 Times Better Than Molecular Sugars in Inhibiting Protein Aggregation and Reducing Amyloidogenic Cytotoxicity.

机构信息

Centre for Advanced Materials, Indian Association for the Cultivation of Science , Kolkata-700032, India.

Cellular and Molecular Neuroscience Laboratory, National Brain Research Centre , Manesar, Gurgaon-122051, India.

出版信息

ACS Appl Mater Interfaces. 2017 Mar 29;9(12):10554-10566. doi: 10.1021/acsami.7b01886. Epub 2017 Mar 17.

DOI:10.1021/acsami.7b01886
PMID:28272865
Abstract

Sugar-based osmolyte molecules are known to stabilize proteins under stress, but usually they have poor chaperone performance in inhibiting protein aggregation. Here, we show that the nanoparticle form of sugars molecule can enhance their chaperone performance typically by 10-10 times, compared to molecular sugar. Sugar-based plate-like nanoparticles of 20-40 nm hydrodynamic size have been synthesized by simple heating of acidic aqueous solution of glucose/sucrose/maltose/trehalose. These nanoparticles have excitation-dependent green/yellow/orange emission and surface chemistry identical to the respective sugar molecule. Fibrillation of lysozyme/insulin/amyloid beta in extracellular space, aggregation of mutant huntingtin protein inside model neuronal cell, and cytotoxic effect of fibrils are investigated in the presence of these sugar nanoparticles. We found that sugar nanoparticles are 10-10 times efficient than respective sugar molecules in inhibiting protein fibrillation and preventing cytotoxicity arising of fibrils. We propose that better performance of the nanoparticle form is linked to its stronger binding with fibril structure and enhanced cell uptake. This result suggests that nanoparticle form of osmolyte can be an attractive option in prevention and curing of protein aggregation-derived diseases.

摘要

糖基渗透调节剂分子在应激条件下可稳定蛋白质,但通常在抑制蛋白质聚集方面的分子伴侣性能较差。在这里,我们表明,与分子糖相比,糖分子的纳米颗粒形式可使它们的分子伴侣性能典型增强 10-10 倍。通过简单地加热葡萄糖/蔗糖/麦芽糖/海藻糖的酸性水溶液,合成了 20-40nm 水动力尺寸的基于糖的片状纳米颗粒。这些纳米颗粒具有依赖于激发的绿色/黄色/橙色发射,并且表面化学与各自的糖分子相同。在存在这些糖纳米颗粒的情况下,研究了溶菌酶/胰岛素/β淀粉样蛋白在细胞外空间中的纤维化、突变 huntingtin 蛋白在模型神经元细胞内的聚集以及纤维的细胞毒性作用。我们发现,纳米颗粒形式的糖比各自的糖分子在抑制蛋白质纤维化和防止纤维毒性方面的效率高 10-10 倍。我们提出,纳米颗粒形式的更好性能与其与纤维结构的更强结合以及增强的细胞摄取有关。这一结果表明,渗透调节剂的纳米颗粒形式可能是预防和治疗蛋白质聚集相关疾病的一种有吸引力的选择。

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