产品设计参数对宫内系统体外释放的影响。

ty10086 提交于 周三, 08/25/2021 - 17:26
文章英文标题
Impact of product design parameters on in vitro release from intrauterine systems.
正文
聚二甲基硅氧烷( PDMS )基左炔诺孕酮宫内节育系统( LNG-IUSs )含有大量强效LNG,因此了解产品设计参数对体外和体内性能的影响,确保安全性和有效性,避免因剂量倾倒而产生严重副作用具有重要意义。LNG-IUS是一种复杂的药物-装置组合产品,其配方设计,除了配方和加工参数外,还需要考虑装置配置和尺寸等额外因素。本研究制备了10种定性( Q1 )和定量( Q2 )等效的LNG-IUS,其外膜的来源(供应商)和尺寸(即厚度)、药物粒径、药物储藏的尺寸(即内径)以及整个IUS的构型不同。建立了一种实时的LNG-IUS体外释放试验方法。此外,为了减少与配方设计相关联的时间,还开发了一种利用水酒精介质的加速释放试验方法。LNG - IUSs外膜的厚度和来源对体外药物释放有很大影响。结果表明,外膜越厚,药物释放速度越慢。对不同来源的外膜的理化性质进行了表征,以了解它们对LNG-IUS体外释药的影响。组成和机械强度可能在药物释放的差异中起作用。以较大药物粒径制备的LNG-IUS制剂,其日释放速率稍慢。组成等效的LNG-IUSs的药物释放速率与相应药物库的表面积线性相关。影响药物释放率的另一个因素是整个IUS的配置。结果表明,外膜的放置意义重大,即药库末端是否复盖。需要注意的是,在大约900天的试验期内,实时释放呈现零级释放动力学。本研究全面了解了产品设计参数对LNG-IUSs体外释药的影响。此外,开发的实时和加速释放试验方法对采用不同产品设计参数制备的组成等效的LNG-IUS显示了良好的区分能力。
文章内容(英文)
Polydimethylsiloxane (PDMS)-based levonorgestrel intrauterine systems (LNG-IUSs) contain a large amount of potent LNG, and therefore it is important to understand the impact of product design parameters on the in vitro and in vivo performance to ensure safety and efficacy, as well as to avoid serious side effects resulting from dose dumping. LNG-IUS is a complex drug-device combination product, and its formulation design, requires consideration of additional factors such as device configuration and dimensions, in addition to formulation and processing parameters. In this study, ten qualitatively (Q1) and quantitatively (Q2) equivalent LNG-IUSs were manufactured with differences in source (supplier) and dimensions (i.e., thickness) of the outer membrane, drug particle size, dimensions of the drug reservoir (i.e., inner diameter), as well as configuration of the entire IUS. A real-time in vitro release testing method was developed for the LNG-IUSs. In addition, an accelerated release testing method was developed using hydro-alcoholic media in order to reduce the time associated with formulation design. Source variations and thickness of their outer membranes had a great impact on the in vitro drug release from the LNG-IUSs. It was demonstrated that the thicker the outer membrane, the slower the drug release rate. The physicochemical properties of the outer membranes obtained from different sources were characterized to understand their impact on the in vitro drug release of the LNG-IUSs. The composition and mechanical strength may play a role in differences in drug release. The LNG-IUS formulation prepared with the larger drug particle size showed a slightly slower daily release rate. The drug release rates from the compositionally equivalent LNG-IUSs linearly correlated to the surface area of the corresponding drug reservoirs. Another factor that affected the drug release rate was the configuration of the entire IUS. It was shown that the placement of the outer membrane was significant, i.e. whether the ends of the drug reservoir were covered or not. It is important to note that real-time release showed zero-order release kinetics over the test period of approximately 900 days. The current study provides a comprehensive understanding of the impact of product design parameters on the in vitro drug release of LNG-IUSs. In addition, the developed real-time and accelerated release testing methods showed good discriminatory ability for compositionally equivalent LNG-IUSs prepared using different product design parameters.
来源出处
Journal|[J]International Journal of PharmaceuticsVolume 578, 2020. PP 119135-119135
DOI
https://doi.org/10.1016/J.IJPHARM.2020.119135

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