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Preparation Optimization and Evaluation of Chitosan-Based Avanafil Nanocomplex Utilizing Antioxidants for Enhanced Neuroprotective Effect on PC12 Cells

机译:利用抗氧化剂对PC12细胞进行抗氧化剂的制备优化和评价抗氧化剂增强神经保护作用

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摘要

(1) Introduction: in recent decades, interdisciplinary research on the utilization of natural products as “active moiety carriers” was focused on due to their superior safety profile, biodegradability, biocompatibility and the ability for sustained or controlled release activity. The nano-based neuroprotective strategy is explored as an imperative treatment for diabetic neuropathy (DN). Avanafil (AV), that selectively inhibits the degradation of cGMP-specific phosphodiesterase, thereby increasing the levels of cGMP, makes a decisive mediator for cytoprotection. (2) Methods: AVnanocomplex formulations were prepared by a modified anti-solvent precipitation method and the method was optimized by Box–Behnken design. An optimized formulation was characterized and evaluated for various in vitro parameters; (3) results:based on the desirability approach, the formulation containing 2.176 g of chitosan, 7.984 g of zein and 90% v/v ethanol concentration can fulfill the prerequisites of optimum formulation (OB-AV-NC).OB-AV-NC was characterized and evaluated for various parameters. The neuroprotective mechanism of AV was evaluated by pretreatment of PC12 cells with plain AV, avanafil nanocomplex (NC) without antioxidants (AV-NC) and with antioxidants (α-Lipoic acid LP; Ellagic Acid EA), AV-LP-EA-Nanocomplex has also shown considerable attenuation in intracellular reactive oxygen species (ROS) and lipid peroxidation with a significant increase in the PC 12 viability under HG conditions in comparison to pure AV; (4) conclusion: the nanocomplex of AV prepared to utilize natural polymers and antioxidants aided for high solubility of AV and exhibited desired neuroprotective activity.This can be one of the promisingstrategy to translate the AV nanocomplex with safety and efficacy in treating DN.
机译:(1)介绍:近几十年来,天然产物为“活动部分运营商”的利用跨学科研究的重点是由于其卓越的安全性,可降解性,生物相容性和缓释或控释活性的能力。所述基于纳米神经保护策略是探索作为当务之急治疗糖尿病性神经病变(DN)。 Avanafil(AV),选择性抑制cGMP特异性磷酸二酯酶降解,从而增加cGMP的水平,使得用于细胞保护的决定性介体。 (2)方法:通过修饰的抗溶剂沉淀法制备AVnanocomplex制剂和方法是由箱式Behnken法设计优化。优化的配方进行了表征和体外评价参数的各种; (3)结果:基于所述可取的方法,将含有2.176克壳聚糖,7.984克玉米蛋白和90%v / v乙醇浓度的制剂可实现最佳制剂的先决条件(OB-AV-NC).OB-AV- NC进行表征并评估各种参数。 ,AV-LP-EA-纳米复合; AV的神经保护机制是由PC12细胞用普通AV,avanafil纳米复合物(NC)的预处理而不抗氧化剂(AV-NC)和抗氧化剂(鞣花酸EAα硫辛酸LP)评价也显示出在细胞内活性氧簇(ROS)和具有相比于纯AV在HG的条件下,PC 12活力显著增加脂质过氧化相当大的衰减; (4)结论:AV的纳米复合物制备利用天然聚合物和辅助用于AV的高溶解度的抗氧化剂和表现出神经保护所需activity.This可以是promisingstrategy在治疗DN平移与安全性和有效性的AV纳米复合物中的一个。

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