Wang Hongpeng, Roof Mike, Burgher Kyle, Pham Chiem, Samuels Eric R, He Yan, Jian Huahua, Wang Tao
Analytical Research and Development, AbbVie, 2525 Dupont Drive, Irvine, CA 92612, USA.
Analytical Research and Development, AbbVie, 2525 Dupont Drive, Irvine, CA 92612, USA.
J Pharm Sci. 2025 Jan;114(1):245-255. doi: 10.1016/j.xphs.2024.08.028. Epub 2024 Aug 31.
Erosion of biodegradable polymeric excipients, such as polylactic acid (PLA) and polylactic-co-glycolic acid (PLGA), is generally characterized by microbalance for the remaining mass of PLA and/or PLGA and Gel Permeation Chromatography (GPC) for molecular weight (MW) decrease. For polymer erosion studies of intravitreal sustained release brimonidine implants, however, both microbalance and GPC present several challenges. Mass loss measurement by microbalance does not have specificity for excipient polymers and drug substances. Accuracy of the remaining mass by weighing could also be low due to sample mass loss through retrieval-drying steps, especially at later drug release (DR) time points. When measuring the decrease of polymer MW by GPC, trace amounts of polymeric degradants (oligomers and/or monomers) trapped inside the implants during DR tests may not be measurable due to sensitivity limitations of the GPC detector and column MW range. Previous efforts to measure remained PLGA weight of dexamethasone micro-implants using qNMR with external calibration have been performed, however, these measurements do not account for chemical structure changes (i.e. LA to GA ratio changes from time zero) of PLGA implants during drug release tests. Here, a qNMR method with an internal standard was developed to monitor the following changes in micro-implants during drug release tests: 1. The remaining overall PLA/PLGA mass. 2. The remaining lactic acid (LA), glycolic acid (GA) unit and PLGA's lauryl ester end group percentages. 3. The trace content of PLA/PLGA oligomers as degradants retained in the implants. Unlike microbalance analysis, qNMR has both specificity for drug substance, excipient polymer, and accuracy due to minimal implant loss during sample preparation. Compared to the overall PLA/PLGA remaining mass generally monitored in erosion studies, the percentage of remaining LA, GA, and the ester end group provide more information about the microstructure change (such as hydrophobicity) of PLA/PLGA. Additionally, the qNMR method can complement GPC methods by measuring the change of remaining PLA and PLGA oligomer concentrations in brimonidine implants, with tenfold less sample and no MW cutoff. The qNMR method can be used as a sensitive tool for both polymer excipient characterization and kinetics studies of brimonidine implant erosion.
可生物降解聚合物辅料(如聚乳酸(PLA)和聚乳酸 - 乙醇酸共聚物(PLGA))的侵蚀通常通过微量天平测量PLA和/或PLGA的剩余质量以及凝胶渗透色谱法(GPC)测量分子量(MW)的降低来表征。然而,对于玻璃体内持续释放溴莫尼定植入物的聚合物侵蚀研究,微量天平和GPC都存在一些挑战。通过微量天平测量质量损失对辅料聚合物和药物没有特异性。由于在取回 - 干燥步骤中样品质量损失,尤其是在药物释放(DR)后期时间点,通过称重测量剩余质量的准确性也可能较低。当通过GPC测量聚合物MW的降低时,由于GPC检测器和柱MW范围的灵敏度限制,在DR测试期间植入物内捕获的痕量聚合物降解产物(低聚物和/或单体)可能无法测量。以前曾尝试使用具有外部校准的定量核磁共振(qNMR)测量地塞米松微植入物中剩余的PLGA重量,然而,这些测量没有考虑药物释放测试期间PLGA植入物的化学结构变化(即从零时起LA与GA比例的变化)。在此,开发了一种带有内标物的qNMR方法,以监测药物释放测试期间微植入物的以下变化:1. 剩余的总PLA/PLGA质量。2. 剩余的乳酸(LA)、乙醇酸(GA)单元和PLGA的月桂酸酯端基百分比。3. 保留在植入物中的作为降解产物的PLA/PLGA低聚物的痕量含量。与微量天平分析不同,qNMR对药物、辅料聚合物具有特异性,并且由于样品制备过程中植入物损失最小而具有准确性。与侵蚀研究中通常监测的总PLA/PLGA剩余质量相比,剩余LA、GA和酯端基的百分比提供了更多关于PLA/PLGA微观结构变化(如疏水性)的信息。此外,qNMR方法可以通过测量溴莫尼定植入物中剩余PLA和PLGA低聚物浓度的变化来补充GPC方法,所需样品量减少十倍且没有MW截止值。qNMR方法可作为聚合物辅料表征和溴莫尼定植入物侵蚀动力学研究的灵敏工具。
