EVALUATION OF THE PRESENCE OF POLYMORPHIC FORMS AND INFLUENCE ON THE DISSOLUTION PROFILE OF TENOXICAM IN ACTIVE PHARMACEUTICAL INGREDIENT AND FORMULATIONS

Aline Taís Fries, N. Olegario, S. Campanharo, V. Pereira, M. Steppe
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Abstract

Polymorphism is a relatively common phenomenon among pharmaceutical compounds, and one of the main aspects to be considered in the production and development of medications. The investigation of polymorphism associated with oxicams, a group belonging to the class of non-steroidal anti-inflammatory drugs (NSAIDs) has increased in recent years and, in the case of tenoxicam, the existence of four polymorphic forms is reported in the literature. The objective of this study was to characterize the presence of different polymorphic forms of tenoxicam in active pharmaceutical ingredient and oral pharmaceutical formulations, as well as to evaluate the influence on in vitro dissolution. The characterization of the three samples of pharmaceutical ingredient of tenoxicam from different suppliers by X-Ray Diffraction (XRD), Infrared (IR) and dissolution profile indicated the presence of a form III crystalline structure, without presenting significant differences between the in vitro dissolution profiles analyzed, and a Dissolution Efficiency (DE%) of 60.30%, 60.70% and 72.34%, respectively. When the four pharmaceutical specialties of tenoxicam were submitted to XRD analysis, they also presented form III crystalline structures. Despite this, the formulations presented different dissolution profiles and a DE% of 75.23%, 83.69%, 78.19% and 90.63%, respectively, without compromising their quality. However, often polymorphism affects physico-chemical properties of drugs, showing the importance of studying this phenomenon, by correlating the presence of crystalline structures to alterations in the quality of active ingredients and pharmaceutical products.
评价多形性形式的存在及其对替诺昔康在活性药物成分和制剂中的溶出谱的影响
多态性是药物化合物中比较普遍的现象,也是药物生产和开发中需要考虑的主要方面之一。奥昔康属于非甾体类抗炎药(NSAIDs),近年来对其多态性的研究有所增加,在替诺昔康的案例中,文献报道了四种多态性形式的存在。本研究的目的是表征活性药物成分和口服药物制剂中不同形态的替诺昔康的存在,并评估其对体外溶出度的影响。通过x射线衍射(XRD)、红外(IR)和溶出度谱对三种不同供应商的替诺昔康原药样品进行表征,发现其存在III型晶体结构,体外溶出度谱分析差异不显著,溶出效率(DE%)分别为60.30%、60.70%和72.34%。当对替诺昔康的四个药系进行XRD分析时,它们也呈现出III型晶体结构。尽管如此,在不影响其质量的情况下,各配方的溶出度分布不同,DE%分别为75.23%、83.69%、78.19%和90.63%。然而,晶型常常影响药物的物理化学性质,通过将晶体结构的存在与有效成分和药品质量的变化联系起来,表明研究这种现象的重要性。
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