Development of the composition and technology of a combined gel for the treatment of osteoarthritis with a pharmacological rationale for the content of components

Q3 Pharmacology, Toxicology and Pharmaceutics
U. V. Nogaeva, Julia M. Kotsur, E. Flisyuk, D. Ivkin, E. D. Semivelichenko, I. A. Titovich, I. Narkevich, V. G. Antonov
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引用次数: 1

Abstract

Introduction. Osteoarthritis (OA) is the most common joint disease that affects more than 10 % of the world's population. More than 600 000 people are diagnosed for the first time each year, but these data do not reflect the true prevalence of the disease, since not all patients seek help from hospitals [1, 2].Aim. Pharmaceutical development of the composition and technology of a gel based on meloxicam, a purine derivative and an immunomodulating component for the treatment of OA with pharmacological substantiation of the content of active substances.Materials and methods. A combination of three active pharmaceutical substances was studied: a non-steroidal anti-inflammatory drug – meloxicam, a purine derivative and an original immunomodulator M. Sodium alginate, natrozole and xanthan gum were considered as gelling agents. Were identified two technological modes of obtaining a gel base. The concentrations of active substances were selected based on the results of preclinical studies. OA was modeled by the combined administration of 0.1 ml of a mixture of Freund's complete adjuvant with a 10 % talc suspension in isotonic sodium chloride solution in a ratio of 1 : 10 into the hock (tarsus) joint cavity. The criteria for choosing the optimal composition of the gel were the size of the damaged joint, exercise tolerance and the histological picture in comparison with intact and control animals. For quantitative data, sample mean values (M) and standard deviations (SD) were calculated. The results corresponded to the laws of normal distribution, statistical processing was carried out using one-way analysis of variance (One-Way ANOVA) using the GraphPad Prism 8.0.2 software, USA at the level of statistical significance of differences p < 0,05 и p < 0,001.Results and discussion. The composition was developed and the technology of the topical dosage form based on sodium alginate was proposed. Preclinical data indicate that the highest efficacy is achieved when using a formulation containing 3 % purine derivative, 5 % immunomodulator M and 0.5 % meloxicam. The developed composition for the effectiveness of suppressing the symptoms of OA showed results that exceeded the reference drug.Conclusion. An original combined agent for the treatment of OA has been developed. Due to the selected component composition, with greater efficiency, it was possible to reduce the dosage of meloxicam to 0.5 %, and the use of sodium alginate as a gelling agent contributed to the prolongation of the action of the gel and the subsequent reduction in the number of applications.
一种用于治疗骨关节炎的联合凝胶的组合物和技术的发展,其成分的药理学原理
介绍骨关节炎(OA)是最常见的关节疾病,影响着世界上超过10%的人口。每年有超过60万人首次被确诊,但这些数据并不能反映该疾病的真实患病率,因为并非所有患者都会向医院寻求帮助[1,2]。目的:开发基于美洛昔康的凝胶的成分和技术,嘌呤衍生物和免疫调节成分,用于通过药理学证实活性物质含量来治疗OA。材料和方法。研究了三种活性药物的组合:非甾体抗炎药美洛昔康、嘌呤衍生物和原始免疫调节剂M。褐藻酸钠、钠唑和黄原胶被认为是胶凝剂。确定了获得凝胶基质的两种技术模式。活性物质的浓度是根据临床前研究的结果选择的。OA通过将0.1ml弗氏完全佐剂与10%滑石悬浮液在等渗氯化钠溶液中的混合物以1∶10的比例联合施用到飞节(跗骨)关节腔内来建模。选择凝胶最佳成分的标准是受损关节的大小、运动耐受性以及与完整动物和对照动物相比的组织学图像。对于定量数据,计算样本平均值(M)和标准偏差(SD)。结果符合正态分布规律,使用GraphPad Prism 8.0.2软件进行单向方差分析(单向方差分析)进行统计处理,在统计学显著性水平上的差异p<0.05иp<0001。结果和讨论。研制了该制剂,并提出了以海藻酸钠为基础的局部剂型的工艺。临床前数据表明,当使用含有3%嘌呤衍生物、5%免疫调节剂M和0.5%美洛昔康的制剂时,可获得最高疗效。所开发的有效抑制OA症状的组合物显示出超过参考药物的结果。结论已经开发出一种用于治疗OA的原始联合制剂。由于所选择的组分组成,以更高的效率,可以将美洛昔康的剂量减少到0.5%,并且使用藻酸钠作为胶凝剂有助于延长凝胶的作用并随后减少应用次数。
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来源期刊
Drug Development and Registration
Drug Development and Registration Pharmacology, Toxicology and Pharmaceutics-Pharmaceutical Science
CiteScore
1.20
自引率
0.00%
发文量
61
审稿时长
8 weeks
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