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氨基酸向中国仓鼠卵巢细胞内的转运调控。

Control of amino acid transport into Chinese hamster ovary cells.

机构信息

Department of Chemical and Biological Engineering, University of Sheffield, Sheffield, UK.

MedImmune Ltd, Granta Park, Cambridge, UK.

出版信息

Biotechnol Bioeng. 2018 Dec;115(12):2908-2929. doi: 10.1002/bit.26794. Epub 2018 Oct 5.

DOI:10.1002/bit.26794
PMID:29987891
Abstract

Amino acid transporters (AATs) represent a key interface between the cell and its environment, critical for all cellular processes: Energy generation, redox control, and synthesis of cell and product biomass. However, very little is known about the activity of different functional classes of AATs in Chinese hamster ovary (CHO) cells, how they support cell growth and productivity, and the potential for engineering their activity and/or the composition of amino acids in growth media to improve CHO cell performance in vitro. In this study, we have comparatively characterized AAT expression in untransfected and monoclonal antibody (MAb)-producing CHO cells using transcriptome analysis by RNA-seq, and mechanistically dissected AAT function using a variety of transporter-specific chemical inhibitors, comparing their effect on cell proliferation, recombinant protein production, and amino acid transport. Of a possible 56 mammalian plasma membrane AATs, 16 AAT messenger RNAs (mRNAs) were relatively abundant across all CHO cell populations. Of these, a subset of nine AAT mRNAs were more abundant in CHO cells engineered to produce a recombinant MAb. Together, upregulated AATs provide additional supply of specific amino acids overrepresented in MAb biomass compared to CHO host cell biomass, enable transport of synthetic substrates for glutathione synthesis, facilitate transport of essential amino acids to maintain active protein synthesis, and provide amino acid substrates for coordinated antiport systems to maintain supplies of proteinogenic and essential amino acids.

摘要

氨基酸转运蛋白(AATs)代表细胞与其环境之间的关键界面,对所有细胞过程都至关重要:能量产生、氧化还原控制以及细胞和产物生物质的合成。然而,对于中国仓鼠卵巢(CHO)细胞中不同功能类别的 AAT 的活性、它们如何支持细胞生长和生产力,以及工程改造它们的活性和/或生长培养基中氨基酸组成以提高 CHO 细胞在体外性能的潜力,我们知之甚少。在这项研究中,我们使用 RNA-seq 进行转录组分析,比较了未转染和单克隆抗体(MAb)产生的 CHO 细胞中的 AAT 表达,并使用各种转运体特异性化学抑制剂从机制上剖析了 AAT 功能,比较了它们对细胞增殖、重组蛋白生产和氨基酸转运的影响。在可能的 56 种哺乳动物质膜 AAT 中,有 16 种 AAT 信使 RNA(mRNA)在所有 CHO 细胞群体中相对丰富。在这些基因中,有一组 9 种 AAT mRNA 在工程改造以生产重组 MAb 的 CHO 细胞中更为丰富。总的来说,上调的 AAT 提供了与 CHO 宿主细胞生物质相比在 MAb 生物质中过量的特定氨基酸的额外供应,能够转运用于合成谷胱甘肽的合成底物,促进必需氨基酸的转运以维持活跃的蛋白质合成,并为协调的反向转运系统提供氨基酸底物,以维持蛋白质和必需氨基酸的供应。

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