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使用动态核极化(DNP)魔角旋转核磁共振(MAS NMR)研究冷冻条件下的蛋白质治疗药物:帕博利珠单抗的研究。

Investigation of Protein Therapeutics in Frozen Conditions Using DNP MAS NMR: A Study on Pembrolizumab.

作者信息

Banks Daniel, Kempf James G, Du Yong, Reichert Paul, Narasimhan Chakravarthy, Fang Rui, Kwon Soonbum, Ling Jing, Lay-Fortenbery Ashley, Zhang Yongqian, Ni Qing Zhe, Cote Aaron, Su Yongchao

机构信息

Bruker Biospin Corporation, Billerica, Massachusetts 01821, United States.

Analytical Research and Development, Merck & Co., Inc., Rahway, New Jersey 07065, United States.

出版信息

Mol Pharm. 2024 Dec 2;21(12):6363-6375. doi: 10.1021/acs.molpharmaceut.4c00929. Epub 2024 Nov 18.

DOI:10.1021/acs.molpharmaceut.4c00929
PMID:39555969
Abstract

The success of modern biopharmaceutical products depends on enhancing the stability of protein therapeutics. Freezing and thawing, which are common thermal stresses encountered throughout the lifecycle of drug substances, spanning protein production, formulation design, manufacturing, storage, and shipping, can impact this stability. Understanding the physicochemical and molecular behaviors of components in biological drug products at temperatures relevant to manufacturing and shipping is essential for assessing stability risks and determining appropriate storage conditions. This study focuses on the stability of high-concentration monoclonal antibody (mAb) pembrolizumab, the drug substance of Keytruda (Merck & Co., Inc., Rahway, NJ, United States), and its excipients in a frozen solution. By leveraging dynamic nuclear polarization (DNP), we achieve more than 100-fold signal enhancements in solid-state NMR (ssNMR), enabling efficient low-temperature (LT) analysis of pembrolizumab without isotopic enrichment. Through both ex situ and in situ ssNMR experiments conducted across a temperature range of 297 to 77 K, we provide insights into the stability of crystalline pembrolizumab under frozen conditions. Importantly, utilizing LT magic-angle spinning (MAS) probes allows us to study molecular dynamics in pembrolizumab from room temperature down to liquid nitrogen temperatures (<100 K). Our results demonstrate that valuable insights into protein conformation and dynamics, crystallinity, and the phase transformations of excipients during the freezing of the formulation matrix can be readily obtained for biological drug products. This study underscores the potential of LT-MAS ssNMR and DNP techniques for analyzing protein therapeutics and vaccines in frozen solutions.

摘要

现代生物制药产品的成功取决于提高蛋白质治疗药物的稳定性。冻融是在药物生命周期中常见的热应力,贯穿蛋白质生产、制剂设计、制造、储存和运输等环节,会影响这种稳定性。了解生物药品中各成分在与制造和运输相关温度下的物理化学和分子行为,对于评估稳定性风险和确定合适的储存条件至关重要。本研究聚焦于高浓度单克隆抗体帕博利珠单抗(可瑞达的原料药,美国默克公司,新泽西州拉威市)及其辅料在冷冻溶液中的稳定性。通过利用动态核极化(DNP)技术,我们在固态核磁共振(ssNMR)中实现了超过100倍的信号增强,从而能够在无需同位素富集的情况下对帕博利珠单抗进行高效低温(LT)分析。通过在297至77 K温度范围内进行的非原位和原位ssNMR实验,我们深入了解了冷冻条件下结晶帕博利珠单抗的稳定性。重要的是,利用低温魔角旋转(MAS)探头使我们能够研究帕博利珠单抗从室温到液氮温度(<100 K)的分子动力学。我们的结果表明,对于生物药品,可以很容易地获得有关蛋白质构象和动力学、结晶度以及制剂基质冷冻过程中辅料相变的宝贵见解。本研究强调了低温MAS ssNMR和DNP技术在分析冷冻溶液中的蛋白质治疗药物和疫苗方面的潜力。

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