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鉴定与中国仓鼠卵巢细胞适应抗体分泌相关的细胞特征。

Identification of cellular signatures associated with chinese hamster ovary cell adaptation for secretion of antibodies.

作者信息

Bai Ying, Mercadé Ivan Domenech, Elgendy Ramy, Lambiase Giulia, Peak-Chew Sew, Franco Catarina, Wingett Steven W, Stevens Tim J, Grassi Luigi, Hitchcock Noah, Ferreira Cristina Sayago, Hatton Diane, Miller Elizabeth A, Mistry Rajesh K

机构信息

Cell Biology Division, Medical Research Council Laboratory of Molecular Biology, Cambridge CB2 0QH, UK.

Cell Culture and Fermentation Sciences, BioPharmaceutical Development, AstraZeneca, Cambridge UK.

出版信息

Comput Struct Biotechnol J. 2024 Dec 10;27:17-31. doi: 10.1016/j.csbj.2024.12.006. eCollection 2025.

Abstract

The secretory capacity of Chinese hamster ovary (CHO) cells remains a fundamental bottleneck in the manufacturing of protein-based therapeutics. Unconventional biological drugs with complex structures and processing requirements are particularly problematic. Although engineered vector DNA elements can achieve rapid and high-level therapeutic protein production, a high metabolic and protein folding burden is imposed on the host cell. Cellular adaptations to these conditions include differential gene expression profiles that can in turn influence the productivity and quality control of recombinant proteins. In this study, we used quantitative transcriptomic and proteomic analyses to investigate how biological pathways change with antibody titre. Gene and protein expression profiles of CHO cell pools and clones producing a panel of different monoclonal and bispecific antibodies were analysed during fed-batch production. Antibody-expressing CHO cell pools were heterogeneous, resulting in few discernible genetic signatures. Clonal cell lines derived from these pools, selected for high and low production, yielded a small number of differentially expressed proteins that correlated with productivity and were shared across the biotherapeutics. However, the dominant feature associated with higher protein production was transgene copy number and the resulting mRNA expression level. Moreover, variability between clonal cell lines suggested that the process of cellular adaptation is variable with diverse cellular changes associated with individual adaptation events.

摘要

中国仓鼠卵巢(CHO)细胞的分泌能力仍然是基于蛋白质的治疗药物生产中的一个基本瓶颈。具有复杂结构和加工要求的非传统生物药物尤其成问题。尽管工程化载体DNA元件可以实现快速且高水平的治疗性蛋白质生产,但会给宿主细胞带来高代谢和蛋白质折叠负担。细胞对这些条件的适应包括差异基因表达谱,这反过来又会影响重组蛋白的生产力和质量控制。在本研究中,我们使用定量转录组学和蛋白质组学分析来研究生物途径如何随抗体滴度变化。在补料分批生产过程中,分析了产生一组不同单克隆和双特异性抗体的CHO细胞池和克隆的基因和蛋白质表达谱。表达抗体的CHO细胞池是异质的,导致几乎没有可识别的遗传特征。从这些池中选出的高产和低产克隆细胞系产生了少量与生产力相关且在生物治疗药物中共享的差异表达蛋白质。然而,与更高蛋白质产量相关的主要特征是转基因拷贝数及其产生的mRNA表达水平。此外,克隆细胞系之间的变异性表明细胞适应过程是可变的,与个体适应事件相关的细胞变化多种多样。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/28b2/11697065/5c050777f447/ga1.jpg

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