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蛋白质的冷冻储存:甘露醇的使用产生均匀的冷冻浓缩物。

Frozen storage of proteins: Use of mannitol to generate a homogenous freeze-concentrate.

机构信息

Department of Pharmaceutics, College of Pharmacy, 308 Harvard St. SE, University of Minnesota, Minneapolis, MN 55455, USA.

Drug Product Development, BioTherapeutics Development & Supply, Janssen Research & Development, Malvern, PA 19355, USA.

出版信息

Int J Pharm. 2023 Jan 5;630:121995. doi: 10.1016/j.ijpharm.2022.121995. Epub 2022 Jul 6.

Abstract

Therapeutic proteins may be subjected to several freeze-thaw cycles throughout manufacturing and storage. The protein solution composition and the freezing conditions may lead to incomplete ice crystallization in the frozen state. This can also result in freeze-concentrate heterogeneity characterized by multiple glass transition temperatures and protein destabilization. The overall objective was to investigate the potential advantages of including a crystallizing excipient (mannitol) along with a sugar (sucrose or trehalose) for frozen storage. This study showed that the addition of mannitol, a readily crystallizing excipient, facilitated ice crystallization. Inclusion of an isothermal hold during cooling (annealing) maximized the mannitol crystallization and resulted in a homogenous freeze-concentrate of a constant composition characterized by a single glass transition temperature. The role of freezing rate and annealing on both mannitol and ice crystallization were discerned using high intensity synchrotron radiation. The addition of sucrose or trehalose, at an appropriate concentration, stabilized the protein. The mannitol to sugar ratio (3:1 or 1:1, 5 % w/v) was optimized to selectively cause maximal crystallization of mannitol while retaining the sugar amorphous. Human serum albumin (1 mg/mL) in these optimized and annealed compositions did not show any meaningful aggregation, even after multiple freeze-thaw cycles. Thus, in addition to a sugar as a stabilizer, the use of a crystallizing excipient coupled with an annealing step can provide an avenue for frozen storage of proteins.

摘要

治疗性蛋白在生产和储存过程中可能会经历多次冻融循环。蛋白溶液的组成和冷冻条件可能导致在冷冻状态下不完全形成冰晶。这也会导致冷冻浓缩物不均匀,表现为多个玻璃化转变温度和蛋白不稳定。总体目标是研究在冷冻储存中加入结晶赋形剂(甘露醇)和糖(蔗糖或海藻糖)的潜在优势。本研究表明,添加甘露醇作为易结晶的赋形剂有助于冰晶的形成。在冷却过程中(退火)加入等温保持期可最大限度地促进甘露醇结晶,并形成具有单一玻璃化转变温度的同质冷冻浓缩物,其组成恒定。使用高强度同步辐射来区分冷冻速率和退火对甘露醇和冰结晶的作用。以适当浓度添加蔗糖或海藻糖可稳定蛋白。甘露醇与糖的比例(3:1 或 1:1,5%w/v)进行优化,以选择性地引起甘露醇的最大结晶,同时保持糖的无定形状态。在这些优化和退火的组合物中,人血清白蛋白(1mg/mL)即使经过多次冻融循环也没有发生任何有意义的聚集。因此,除了使用糖作为稳定剂之外,使用结晶赋形剂结合退火步骤可以为蛋白的冷冻储存提供一种途径。

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