Nuclear Magnetic Resonance Study of Monoclonal Antibodies Near an Oil-Water Interface.

IF 3.7 3区 医学 Q2 CHEMISTRY, MEDICINAL Journal of pharmaceutical sciences Pub Date : 2025-01-25 DOI:10.1016/j.xphs.2025.01.020
Jamini Bhagu, Lissa C Anderson, Samuel C Grant, Hadi Mohammadigoushki
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Abstract

Monoclonal antibodies (mAb) represent an important class of biologic therapeutics that can treat a variety of diseases including cancer, autoimmune disorders or respiratory conditions (e.g. COVID-19). However, throughout their development, mAb are exposed to air-water or oil-water interfaces that may trigger mAb partial unfolding that can lead to the formation of proteinaceous aggregates. Using a combination of dynamic surface tensiometry and spatially resolved 1D 1H NMR spectroscopy, this study investigates if adsorption of a model IgG2a-κ mAb to the oil-water interface affects its structure. Localized NMR spectroscopy was performed using voxels of 375 µm, incrementally approaching the oil-water interface. Dynamic interfacial tension progressively decreases at the oil-water interface over time, confirming mAb adsorption to the interface. Localized NMR spectroscopy results indicate that, while the number of mAb-related chemical resonances and chemical shift frequencies remain unaffected, spectral line broadening is observed as voxels incrementally approach the oil-water interface. Moreover, the spin-spin (T2) relaxation of the mAb molecule was measured for a voxel centered at the interface and shown to be affected differentially across the mAb resonances, indicating a rotational restriction for mAb molecules due to presence of the interface. Finally, the apparent diffusion coefficient of the mAb for the voxel centered at the interface is lower than the bulk mAb. These results suggest that this specific mAb interacts with and may be in exchange with bulk mAb phase in the vicinity of the interface. As such, these localized NMR techniques offer the potential to probe and quantify alterations of mAb properties near interfacial layers.

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单克隆抗体(mAb)是一类重要的生物疗法,可治疗多种疾病,包括癌症、自身免疫性疾病或呼吸系统疾病(如 COVID-19)。然而,在整个开发过程中,mAb 会暴露在空气-水或油-水界面中,这可能会引发 mAb 的部分折叠,从而形成蛋白质聚集体。本研究结合使用动态表面张力仪和空间分辨一维 1H NMR 光谱法,研究了模型 IgG2a-κ mAb 在油水界面的吸附是否会影响其结构。使用 375 µm 的体素,逐步接近油水界面,进行了局部 NMR 光谱分析。随着时间的推移,油水界面上的动态界面张力逐渐减小,证实了 mAb 在界面上的吸附作用。局部核磁共振光谱结果表明,虽然与 mAb 相关的化学共振数量和化学位移频率未受影响,但随着体素逐渐接近油水界面,可观察到光谱线变宽。此外,还测量了以界面为中心的体素的 mAb 分子自旋-自旋(T2)弛豫,结果表明不同的 mAb 共振会受到不同的影响,这表明由于界面的存在,mAb 分子的旋转受到了限制。最后,以界面为中心的体素的 mAb 表观扩散系数低于体素。这些结果表明,这种特定的 mAb 与界面附近的块状 mAb 相互作用,并可能与块状 mAb 相交换。因此,这些局部核磁共振技术为探测和量化界面层附近 mAb 性质的改变提供了可能。
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来源期刊
CiteScore
7.30
自引率
13.20%
发文量
367
审稿时长
33 days
期刊介绍: The Journal of Pharmaceutical Sciences will publish original research papers, original research notes, invited topical reviews (including Minireviews), and editorial commentary and news. The area of focus shall be concepts in basic pharmaceutical science and such topics as chemical processing of pharmaceuticals, including crystallization, lyophilization, chemical stability of drugs, pharmacokinetics, biopharmaceutics, pharmacodynamics, pro-drug developments, metabolic disposition of bioactive agents, dosage form design, protein-peptide chemistry and biotechnology specifically as these relate to pharmaceutical technology, and targeted drug delivery.
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