Hernandez Christopher, Gawlik Natalia, Goss Monika, Zhou Haoyan, Jeganathan Selva, Gilbert Danielle, Exner Agata A
Department of Biomedical Engineering, Case Western Reserve University, 11100 Euclid Ave, Cleveland, OH 44106, USA.
Department of Biomedical Engineering, Case Western Reserve University, 11100 Euclid Ave, Cleveland, OH 44106, USA; Department of Radiology, Case Western Reserve University, 11100 Euclid Ave, Cleveland, OH 44106, USA.
J Control Release. 2016 Dec 10;243:225-231. doi: 10.1016/j.jconrel.2016.10.009. Epub 2016 Oct 11.
In situ forming implants (ISFIs) have shown promise as a sustained, local drug delivery system for therapeutics in a variety of applications. However, development of ISFIs has been hindered by poor correlation between in vitro study results and in vivo performance. In contrast to oral dosage forms, there is currently no clear consensus on a standard for in vitro drug dissolution studies for parenteral formulations. Recent studies have suggested that the disparity between in vivo and in vitro behavior of phase-inverting ISFIs may be, in part, due to differences in injection site stiffness. Accordingly, this study aimed to create acrylamide-based hydrogel phantoms of varying porosity and stiffness, which we hypothesized would better predict in vivo performance. Implant microstructure and shape were found to be dependent on the stiffness of the phantoms, while drug release was found to be dependent on both phantom porosity and stiffness. Specifically, SEM analysis revealed that implant porosity and interconnectivity decreased with increasing phantom stiffness and better mimicked the microstructure seen in vivo. Burst release of drug increased from 31% to 43% when in standard acrylamide phantoms vs macroporous phantoms (10kPa), improving the correlation to the burst release seen in vivo. Implants in 30kPa macroporous phantoms had the best correlation with in vivo burst release, significantly improving (p<0.05) the burst release relative to in vivo from 64%, using a standard PBS dissolution method, to 92%. These findings confirm that implant behavior is affected by injection site stiffness. Importantly, with appropriate optimization and validation, hydrogel phantoms such as the one investigated here could be used to improve the in vitro-in vivo correlation of in situ forming implant formulations and potentially augment their advancement to clinical use.
原位成型植入物(ISFIs)已显示出有望成为一种用于多种治疗应用的持续局部给药系统。然而,体外研究结果与体内性能之间的相关性较差,这阻碍了ISFIs的发展。与口服剂型不同,目前对于肠胃外制剂的体外药物溶出度研究标准尚无明确共识。最近的研究表明,相转变ISFIs体内和体外行为之间的差异可能部分归因于注射部位硬度的不同。因此,本研究旨在创建具有不同孔隙率和硬度的基于丙烯酰胺的水凝胶模型,我们假设这些模型能更好地预测体内性能。研究发现植入物的微观结构和形状取决于模型的硬度,而药物释放则取决于模型的孔隙率和硬度。具体而言,扫描电子显微镜(SEM)分析显示,随着模型硬度的增加,植入物的孔隙率和连通性降低,并且更好地模拟了体内观察到的微观结构。当使用标准丙烯酰胺模型与大孔模型(10kPa)时,药物的突释从31%增加到43%,改善了与体内突释的相关性。在30kPa大孔模型中的植入物与体内突释具有最佳相关性,相对于体内,使用标准磷酸盐缓冲盐水(PBS)溶出方法时,突释从64%显著提高(p<0.05)至92%。这些发现证实植入物行为受注射部位硬度影响。重要的是,通过适当的优化和验证,本文所研究的这类水凝胶模型可用于改善原位成型植入制剂的体外-体内相关性,并有可能推动其向临床应用发展。