Exploring metabolic effects of dipeptide feed media on CHO cell cultures by in silico model-guided flux analysis.

IF 3.9 3区 生物学 Q2 BIOTECHNOLOGY & APPLIED MICROBIOLOGY
Applied Microbiology and Biotechnology Pub Date : 2024-12-01 Epub Date: 2024-01-16 DOI:10.1007/s00253-023-12997-0
Seo-Young Park, Jinsung Song, Dong-Hyuk Choi, Uiseon Park, Hyeran Cho, Bee Hak Hong, Yaron R Silberberg, Dong-Yup Lee
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引用次数: 0

Abstract

There is a growing interest in perfusion or continuous processes to achieve higher productivity of biopharmaceuticals in mammalian cell culture, specifically Chinese hamster ovary (CHO) cells, towards advanced biomanufacturing. These intensified bioprocesses highly require concentrated feed media in order to counteract their dilution effects. However, designing such condensed media formulation poses several challenges, particularly regarding the stability and solubility of specific amino acids. To address the difficulty and complexity in relevant media development, the biopharmaceutical industry has recently suggested forming dipeptides by combining one from problematic amino acids with selected pairs to compensate for limitations. In this study, we combined one of the lead amino acids, L-tyrosine, which is known for its poor solubility in water due to its aromatic ring and hydroxyl group, with glycine as the partner, thus forming glycyl-L-tyrosine (GY) dipeptide. Subsequently, we investigated the utilization of GY dipeptide during fed-batch cultures of IgG-producing CHO cells, by changing its concentrations (0.125 × , 0.25 × , 0.5 × , 1.0 × , and 2.0 ×). Multivariate statistical analysis of culture profiles was then conducted to identify and correlate the most significant nutrients with the production, followed by in silico model-guided analysis to systematically evaluate their effects on the culture performance, and elucidate metabolic states and cellular behaviors. As such, it allowed us to explain how the cells can more efficiently utilize GY dipeptide with respect to the balance of cofactor regeneration and energy distribution for the required biomass and protein synthesis. For example, our analysis results uncovered specific amino acids (Asn and Gln) and the 0.5 × GY dipeptide in the feed medium synergistically alleviated the metabolic bottleneck, resulting in enhanced IgG titer and productivity. In the validation experiments, we tested and observed that lower levels of Asn and Gln led to decreased secretion of toxic metabolites, enhanced longevity, and elevated specific cell growth and titer. KEY POINTS: • Explored the optimal Tyr dipeptide for the enhanced CHO cell culture performance • Systematically analyzed effects of dipeptide media by model-guided approach • Uncovered synergistic metabolic utilization of amino acids with dipeptide.

Abstract Image

通过硅学模型引导的通量分析,探索二肽饲料培养基对 CHO 细胞培养的代谢影响。
为了提高哺乳动物细胞培养(特别是中国仓鼠卵巢(CHO)细胞)中生物制药的生产率,人们对灌流或连续工艺越来越感兴趣,以实现先进的生物制造。这些强化的生物工艺非常需要浓缩的饲用培养基,以抵消其稀释效应。然而,设计这种浓缩培养基配方面临着一些挑战,特别是特定氨基酸的稳定性和溶解性。为了解决相关培养基开发中的困难和复杂性,生物制药行业最近建议将问题氨基酸中的一种与所选的一对组合成二肽,以弥补其局限性。众所周知,L-酪氨酸因其芳香环和羟基而在水中溶解性较差,在本研究中,我们将其与甘氨酸结合,形成了甘氨酰-L-酪氨酸(GY)二肽。随后,我们通过改变 GY 二肽的浓度(0.125 ×、0.25 ×、0.5 ×、1.0 × 和 2.0 ×),研究了在喂养批次培养产生 IgG 的 CHO 细胞过程中 GY 二肽的利用情况。然后对培养曲线进行多变量统计分析,以确定最重要的营养成分并将其与产量联系起来,接着进行硅学模型指导分析,以系统评估这些营养成分对培养性能的影响,并阐明代谢状态和细胞行为。这样,我们就能解释细胞如何能更有效地利用 GY 二肽,平衡辅助因子再生和能量分配,以合成所需的生物量和蛋白质。例如,我们的分析结果发现,特定氨基酸(Asn 和 Gln)和饲用培养基中的 0.5 × GY 二肽能协同缓解代谢瓶颈,从而提高 IgG 滴度和生产率。在验证实验中,我们测试并观察到较低水平的 Asn 和 Gln 可减少有毒代谢物的分泌、延长寿命并提高特定细胞的生长和滴度。要点- 探索提高 CHO 细胞培养性能的最佳 Tyr 二肽 - 通过模型指导方法系统分析二肽培养基的影响 - 发现二肽对氨基酸的协同代谢利用。
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来源期刊
Applied Microbiology and Biotechnology
Applied Microbiology and Biotechnology 工程技术-生物工程与应用微生物
CiteScore
10.00
自引率
4.00%
发文量
535
审稿时长
2 months
期刊介绍: Applied Microbiology and Biotechnology focusses on prokaryotic or eukaryotic cells, relevant enzymes and proteins; applied genetics and molecular biotechnology; genomics and proteomics; applied microbial and cell physiology; environmental biotechnology; process and products and more. The journal welcomes full-length papers and mini-reviews of new and emerging products, processes and technologies.
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