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利用反复使用和储存后的降解甘油鉴定和描述胰岛素制剂的化学和物理稳定性。

Identification and characterization of chemical and physical stability of insulin formulations utilizing degraded glycerol after repeated use and storage.

机构信息

Institute of Drug Metabolism and Pharmaceutical Analysis, College of Pharmaceutical Sciences, Zhejiang University, Hangzhou 310058, China; Hangzhou Institute of Innovative Medicine, Zhejiang University, Hangzhou 310016, China.

Zhejiang Haisheng Pharmaceutical Inc, Taizhou 318000, China.

出版信息

Eur J Pharm Biopharm. 2022 Aug;177:147-156. doi: 10.1016/j.ejpb.2022.06.011. Epub 2022 Jun 29.

Abstract

Insulin treatment is currently considered to be the main strategy for controlling diabetes. Although the recombinant insulin formulation is relatively mature, we found that a batch of insulin formulation exhibited an unusual degradation rate in the stability experiment. The main purposes of this article are to identify the root cause for this phenomenon and characterize of chemical and physical degradation products. We compared the chemical and physical stability of two batches of insulin formulations prepared separately with simulated repeated use and freshly opened glycerol. The chemical stability of insulin was identified by liquid chromatography coupled with tandem mass spectrometry (LC- MS/MS). Micro-flow imaging (MFI), far-ultraviolet circular dichroism (Far-UV CD) and Thioflavin T (ThT) fluorescent assays were used to reveal protein aggregation and fibrosis. The chemical and physical stability of the insulin formulation with newly opened glycerol was much better than that with degraded glycerol, and both groups of formulations were extremely sensitive to light. The results indicated that the original batch insulin formulation with abnormal stability was indeed caused by the excipient glycerol after long-term storage and repeated usage. More attention should be paid to the quality changes of excipients during repeated usage and storage of excipients for the practical purpose. Moreover, we have discovered a novel degradation pathway for insulin and peptides in general. In addition, LC-MS/MS results suggested that the N-terminus of insulin B-chain was prone to chemical degradation which enlightens that it could be potentially modified to improve the stability of insulin formulations.

摘要

胰岛素治疗目前被认为是控制糖尿病的主要策略。虽然重组胰岛素制剂相对成熟,但我们发现一批胰岛素制剂在稳定性实验中表现出异常的降解速度。本文的主要目的是确定这种现象的根本原因,并对化学和物理降解产物进行特征描述。我们比较了两批分别用模拟重复使用和新开封甘油制备的胰岛素制剂的化学和物理稳定性。通过液相色谱串联质谱(LC-MS/MS)鉴定胰岛素的化学稳定性。采用微流成像(MFI)、远紫外圆二色性(Far-UV CD)和硫黄素 T(ThT)荧光测定法揭示蛋白质聚集和纤维化。新开封甘油的胰岛素制剂的化学和物理稳定性明显优于降解甘油的胰岛素制剂,且两组制剂对光都非常敏感。结果表明,原始批次的胰岛素制剂在长期储存和重复使用后,确实是由于赋形剂甘油引起的异常稳定性。在重复使用和储存赋形剂时,应更加注意赋形剂的质量变化,以达到实际目的。此外,我们发现了胰岛素和一般肽的一种新的降解途径。此外,LC-MS/MS 结果表明胰岛素 B 链的 N 端易发生化学降解,这表明可以对其进行修饰以提高胰岛素制剂的稳定性。

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