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首页> 外文期刊>Journal of Molecular Liquids >Investigation of aggregation behavior of ibuprofen sodium drug under the influence of gelatin protein and salt
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Investigation of aggregation behavior of ibuprofen sodium drug under the influence of gelatin protein and salt

机译:明胶蛋白和盐影响下布洛芬钠药物的聚集行为研究

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The interaction of amphiphilic drug ibuprofen sodium salt (IBS) and gelatin (GT) protein have evaluated in the current system by means of conductometric, tensiometric and fluorometric techniques in aqueous as well as in aqueous electrolytes solutions at 298.15 K. IBS is utilized as an analgesic, an antipyretic and anti-inflammatory drug. Akin to surfactants and polymers interaction drug also interacts through gelatin. For that reason, in the present study, we have evaluated the drug IBS and gelatin (GT) interaction by means of conductimetry, tensiometry as fluorometry in aqueous along with in occurrence of additive (sodium chloride (NaCI)) at 298.15 K. From the graphs of specific conductivity against IBS concentration in case of conductivity and from the plots of surface tension (gamma) vs. log IBS concentration, two break point was achieved in the occurrence of GT in absence and the presence of additives. The achieved primary cut-off point is entitled critical aggregation concentration (cc) that obtained lower than the characteristic critical micelle concentration (cmc) and the attained a subsequent cutoff point means the second one is entitled polymer saturation point (pp) i.e. resembling cmc. The interaction amongst IBS and GT occurs as a result of the well formation of the surface active complex by drug and GT as revealed via lessening of gamma of gelatin solution through the addition of IBS in all different media. NaCI increases the interaction of IBS-GT mixtures. The achieved cc value of drug and gelatin mixtures reduce via raising the GT concentration (%w/v), while their pp value enhances viewing the clear interaction amid IBS and GT. Free energies of aggregation (Delta G(agg)) along with micellization (Delta G(mic)) were also assessed and discussed. Fluorescence spectroscopy was employed to evaluate the aggregation numbers (N-agg) of IBS and IBS-GT mixtures in the absence and occurrence of additive. (C) 2019 Elsevier B.V. All rights reserved.
机译:通过在298.15k的水性电解质和电解质溶液中的电导率,张力和荧光技术在当前系统中评估了两亲药物中布洛芬钠盐(IBS)和明胶(GT)蛋白的相互作用。镇痛剂,一种解热和抗炎药。类似于表面活性剂和聚合物相互作用药物也通过明胶相互作用。因此,在本研究中,我们已经通过电导率,张力测定,作为水性的荧光法以及在298.15k的发生(氯化钠(NaClime))中,评估了药物IBS和明胶(GT)相互作用。在电导率和表面张力(γ)的图中,在导电性和表面张力(γ)的曲线图中,在不存在和添加剂存在的情况下实现了两次断裂点的特定电导率的图。所实现的初级截止点是题为基于特征临界胶束浓度(CMC)的关键聚集浓度(CC),并且达到后续的截止点是指第二一个是具有高分子饱和点(PP)I.E.类似CMC的截止点。 IBS和GT之间的相互作用是由于药物和GT的良好形成,通过在所有不同培养基中加入IBS来通过减少明胶溶液的γ揭示。 NaCI增加了IBS-GT混合物的相互作用。所获得的药物和明胶混合物的CC值通过提高GT浓度(%w / v)而降低,而其PP值增强了在IBS和GT中的透明相互作用。还评估并讨论了聚集的自由能量(Delta G(Agg))以及胶束化(Delta G(MIC))。使用荧光光谱法在不存在和发生的情况下评估IBS和IBS-GT混合物的聚集数(N-AGG)。 (c)2019 Elsevier B.v.保留所有权利。

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