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最佳蛋白质合成在防止培养的B细胞杂交瘤凋亡死亡中的关键作用。

Essential role of optimal protein synthesis in preventing the apoptotic death of cultured B cell hybridomas.

作者信息

Perreault J, Lemieux R

机构信息

Canadian Red Cross, Blood Services, Terminus, Québec.

出版信息

Cytotechnology. 1993;13(2):99-105. doi: 10.1007/BF00749936.

Abstract

The monoclonal antibody productivity of cell culture systems is strongly dependent on the maintenance of hybridoma cell viability. We report that partial (< 50%) and transient (3 h) inhibition of protein synthesis by cycloheximide or deprivation of an essential amino acid induces apoptosis (programmed cell death) in B cell hybridomas. This unusual mechanism of apoptosis induction is likely to play a significant role in limiting cell viability in batch and perfusion cultures of hybridomas and emphasizes the importance of constantly maintaining a near optimal rate of macromolecular synthesis by optimization of all culture parameters. Inhibition of apoptosis in hybridomas by cell engineering and other technologies should permit, in the near future, a significant increase in the antibody productivity of existing cell culture systems.

摘要

细胞培养系统的单克隆抗体产量在很大程度上取决于杂交瘤细胞活力的维持。我们报告,用放线菌酮部分(<50%)和短暂(3小时)抑制蛋白质合成或剥夺必需氨基酸会诱导B细胞杂交瘤细胞发生凋亡(程序性细胞死亡)。这种不寻常的凋亡诱导机制可能在限制杂交瘤分批培养和灌注培养中的细胞活力方面发挥重要作用,并强调了通过优化所有培养参数不断维持接近最佳大分子合成速率的重要性。通过细胞工程和其他技术抑制杂交瘤细胞凋亡,在不久的将来应该能够显著提高现有细胞培养系统的抗体产量。

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