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冷冻制剂玻璃小瓶破裂的机制研究。I. 可结晶辅料甘露醇引起的小瓶破裂

Mechanistic studies of glass vial breakage for frozen formulations. I. Vial breakage caused by crystallizable excipient mannitol.

作者信息

Jiang Ge, Akers Mike, Jain Manish, Guo Jeremy, Distler Adrian, Swift Rob, Wadhwa Manpreet-Vick S, Jameel Feroz, Patro Sugu, Freund Erwin

机构信息

Drug Product and Device Development, Amgen Inc., USA.

出版信息

PDA J Pharm Sci Technol. 2007 Nov-Dec;61(6):441-51.

Abstract

The process of freeze-thaw not only subjects bioproducts to potentially destabilizing stress, but also imposes challenges to retain container integrity. Shipment and storage of frozen products in glass vials and thawing of the vials prior to use at clinics is a common situation. Vial integrity failure during freeze-thaw results in product loss and safety issues. Formulations of biomolecules often include crystallizable excipients, which can cause glass vial breakage during freeze-thaw operations. In this study, mannitol formulations served as models for mechanistic investigation of root causes for vial breakage. Several parameters and their impacts on vial breakage were investigated, including mannitol concentration (5% and 15%), different freeze-thaw conditions (fast, slow, and staging), fill configurations (varying fill volume/vial size ratio), and vial tray materials (plastic, stainless steel, corrugated cardboard, aluminum, and polyurethane foam). The results in this study were subjected to a statistical proportion test. The data showed that large fill volumes strongly correlated with higher percentage of vial cracks. Furthermore, the 15% mannitol was found to cause more breakage than 5% mannitol, especially with fast temperature gradient. Significantly more thawing vial breakage occurred in the fast compared to slow freeze-thaw with all types of vial trays. The freezing breakage was substantially lower than the thawing breakage using the fast temperature gradient, and the trend was reversed with the slow temperature gradient. An intermediate hold at -30 degrees C prior to further decrease in temperature proved to be a practical approach to minimize mannitol-induced vial breakage. Thermal mechanical analysis (TMA) and strain gage techniques were employed to gain mechanistic insights, and it was found that the primary causes for mannitol-induced vial breakage were partial crystallization during freezing and "secondary" crystallization of non-crystallized fraction during thawing. The strain on the vial's axial direction was significantly higher than the hoop direction, typically resulting in bottom lens of the vial coming off. Without a -30 degrees C hold, rapid volume expansions due to initial crystallization and secondary crystallization of mannitol were observed in TMA profiles, and these expansions were more apparent in 15% mannitol compared to 5% mannitol. With the introduction of a -30 degrees C hold step, abrupt expansions diminished in TMA profiles, suggesting that most of the mannitol crystallization occurred concurrently with ice solidification during the -30 degrees C holding step and, thus, secondary crystallization during thawing was minimal and the sudden expansion event was eliminated. Therefore, vial breakage during both freezing and thawing was reduced.

摘要

冻融过程不仅会使生物制品面临潜在的稳定性破坏压力,还对保持容器完整性提出了挑战。在玻璃小瓶中运输和储存冷冻产品,并在临床使用前对小瓶进行解冻是常见的情况。冻融过程中小瓶完整性的破坏会导致产品损失和安全问题。生物分子制剂通常包含可结晶的辅料,这可能会在冻融操作过程中导致玻璃小瓶破裂。在本研究中,甘露醇制剂用作小瓶破裂根本原因的机理研究模型。研究了几个参数及其对小瓶破裂的影响,包括甘露醇浓度(5%和15%)、不同的冻融条件(快速、慢速和分段)、灌装配置(不同的灌装体积/小瓶尺寸比)以及小瓶托盘材料(塑料、不锈钢、瓦楞纸板、铝和聚氨酯泡沫)。本研究的结果进行了统计比例检验。数据表明,大灌装体积与更高比例的小瓶裂纹密切相关。此外,发现15%的甘露醇比5%的甘露醇导致更多的破裂,特别是在快速温度梯度下。与所有类型的小瓶托盘的慢速冻融相比,快速冻融过程中解冻小瓶的破裂明显更多。使用快速温度梯度时,冷冻破裂明显低于解冻破裂,而使用慢速温度梯度时趋势相反。在进一步降低温度之前在-30℃进行中间保持被证明是一种将甘露醇引起的小瓶破裂降至最低的实用方法。采用热机械分析(TMA)和应变片技术来获得机理见解,发现甘露醇引起小瓶破裂的主要原因是冷冻过程中的部分结晶以及解冻过程中非结晶部分的“二次”结晶。小瓶轴向的应变明显高于环向,通常导致小瓶底部透镜脱落。在没有-30℃保持的情况下,在TMA曲线中观察到由于甘露醇的初始结晶和二次结晶导致的快速体积膨胀,并且与5%的甘露醇相比,这些膨胀在15%的甘露醇中更明显。随着引入-30℃保持步骤,TMA曲线中的突然膨胀减小,这表明大部分甘露醇结晶在-30℃保持步骤期间与冰凝固同时发生,因此解冻过程中的二次结晶最小化并且消除了突然膨胀事件。因此,冷冻和解冻过程中的小瓶破裂都减少了。

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