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马杜拉霉素,一种新型的糖基化调节剂,用于哺乳动物补料分批和恒态灌注工艺。

Maduramycin, a novel glycosylation modulator for mammalian fed-batch and steady-state perfusion processes.

机构信息

Institute for Pharma Technology, School of Life Sciences, University of Applied Sciences and Arts Northwestern Switzerland, Muttenz, Switzerland; Research Division Biochemical Engineering, Institute of Chemical Environmental and Bioscience Engineering, Vienna University of Technology, Vienna, Austria.

Global Drug Substance Development, Merck Serono SA (an affiliate of Merck KGaA, Darmstadt, Germany), Corsier-sur-Vevey, Switzerland.

出版信息

J Biotechnol. 2024 Mar 10;383:73-85. doi: 10.1016/j.jbiotec.2024.02.003. Epub 2024 Feb 9.

DOI:10.1016/j.jbiotec.2024.02.003
PMID:38340899
Abstract

Controlling high-mannose (HM) content of therapeutic proteins during process intensification, reformulation for subcutaneous delivery, antibody-drug conjugate or biosimilar manufacturing represents an ongoing challenge. Even though a range of glycosylation levers to increase HM content exist, modulators specially increasing M5 glycans are still scarce. Several compounds of the polyether ionophore family were screened for their ability to selectively increase M5 glycans of mAb products and compared to the well-known α-mannosidase I inhibitor kifunensine known to increase mainly M8-M9 glycans. Maduramycin, amongst other promising polyether ionophores, showed the desired effect on different cell lines. For fed-batch processes, a double bolus addition modulator feed strategy was developed maximizing the effect on glycosylation by minimizing impact on culture performance. Further, a continuous feeding strategy for steady-state perfusion processes was successfully developed, enabling consistent product quality at elevated HM glycan levels. With kifunensine and maduramycin showing inverse effects on the relative HM distribution, a combined usage of these modulators was further evaluated to fine-tune a desired HM glycan pattern. The discovered HM modulators expand the current HM modulating toolbox for biotherapeutics. Their application not only for fed-batch processes, but also steady-state perfusion processes, make them a universal tool with regards to fully continuous manufacturing processes.

摘要

在工艺强化、皮下给药制剂、抗体药物偶联物或生物类似药生产过程中,控制治疗性蛋白的高甘露糖(HM)含量是一个持续存在的挑战。尽管存在一系列增加 HM 含量的糖基化手段,但专门增加 M5 聚糖的调节剂仍然稀缺。筛选了一系列聚醚离子载体化合物,以评估它们选择性增加单抗产品中 M5 聚糖的能力,并与众所周知的主要增加 M8-M9 聚糖的α-甘露糖苷酶 I 抑制剂 Kifunensine 进行比较。Maduramycin 等其他有前途的聚醚离子载体在不同的细胞系中表现出了所需的效果。对于分批补料工艺,开发了双补料调节剂补料策略,通过最小化对培养性能的影响,最大限度地提高糖基化效果。此外,还成功开发了用于稳态灌注工艺的连续进料策略,在提高 HM 聚糖水平的同时,保持一致的产品质量。由于 Kifunensine 和 Maduramycin 对相对 HM 分布有相反的影响,因此进一步评估了联合使用这些调节剂来微调所需的 HM 聚糖模式。所发现的 HM 调节剂扩展了生物治疗剂当前的 HM 调节工具包。它们不仅可用于分批补料工艺,还可用于稳态灌注工艺,使其成为全连续制造工艺的通用工具。

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