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体外研究橙皮苷二氢查耳酮通过热诱导鸡卵清溶菌酶展开而发挥抗聚集潜力;溶菌酶淀粉样变性的预防性研究。

An In Vitro elucidation of the antiaggregatory potential of Diosminover thermally induced unfolding of hen egg white lysozyme; A preventive quest for lysozyme amyloidosis.

机构信息

Protein Amyloid Research Laboratory, Interdisciplinary Biotechnology Unit, Aligarh Muslim University, Aligarh, UP 202002, India.

Computational Mechanistic Chemistry and Drug Discovery, Department of Chemistry, Rhodes University, South Africa.

出版信息

Int J Biol Macromol. 2019 May 15;129:1015-1023. doi: 10.1016/j.ijbiomac.2019.02.107. Epub 2019 Feb 19.

Abstract

Protein misfolding diseases are associated with human pathologies. These neurodegenerative diseases remain challenging task for researchers because of their adverse effect on vital organs system. Lysozyme amyloidosis is also associated with multi-organ dysfunction. Hence elucidation of its folding pathway is of great importance, for which hen egg white lysozyme (HEWL) being homological to its human counterpart was taken into consideration. Here in this study we have investigated the effect of diosmin (DSN), a flavonoid over thermally aggregated HEWL. Decrease in ANS, ThT and Rayleigh scattering fluorescence intensity suggests the transition between β to α conformations. Further decrease in absorbance at 360 nm and of congo red with slight blue shift also indicated the disappearance of β sheeted structure under the under the influence of increasing concentration of DSN. These results were also supported by circular dichroism in which gradual appearance α helical structure was observed. Finally visualization under transmission electron microscopy (TEM) authenticated the maximum structural alteration in the previously formed aggregates of HEWL at 250 μM DSN. Molecular docking followed by 100 ns MD simulations help to understand the interaction mechanism of HEWL with DSN. Results suggest DSN could be a useful in the treatment of amyloid related disorders.

摘要

蛋白质错误折叠疾病与人类病理有关。这些神经退行性疾病对研究人员来说仍然是一个具有挑战性的任务,因为它们对重要器官系统有不良影响。溶菌酶淀粉样变性也与多器官功能障碍有关。因此,阐明其折叠途径非常重要,为此考虑了同源的鸡卵清溶菌酶(HEWL)。在这项研究中,我们研究了橙皮苷(DSN)对热聚集 HEWL 的影响。ANS、ThT 和瑞利散射荧光强度的降低表明β到α构象的转变。在增加 DSN 浓度的影响下,360nm 处吸光度的进一步降低以及刚果红的轻微蓝移也表明β片层结构的消失。圆二色性(CD)的结果也支持这一观点,在 CD 中观察到逐渐出现α螺旋结构。最后,在透射电子显微镜(TEM)下的可视化证实了在 250μM DSN 下 HEWL 先前形成的聚集体发生了最大的结构改变。随后进行的 100nsMD 模拟的分子对接有助于了解 HEWL 与 DSN 的相互作用机制。结果表明,DSN 可能是治疗淀粉样相关疾病的有用药物。

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