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Production of anti TNF-α antibodies in eukaryotic cells using different combinations of vectors carrying heavy and light chains

机译:使用携带重链和轻链的载体的不同组合在真核细胞中产生抗TNF-α抗体

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Tumor necrosis factor-α (TNF-α) plays a key role in rheumatoid arthritis and some other autoimmune diseases. Therapy with anti-TNF-α recombinant antibodies (Ab) appears to be highly effective. Production of new hyper-producing eukaryotic cell lines can decrease the treatment cost, which currently is very high. However, due to the complexity of protein transcription, translation, processing, and secretion in mammalian cells, the stages at which antibody expression is affected are still poorly determined. The aim of this work was to compare the productivity of two cell lines developed in CHO DG44 cells, deficient in dihydrofolate reductase, transfected with vectors carrying either heavy (H) or light (L) chains of chimeric antibody under different combinations of selective elements. Both H and L chains were cloned either in pOptiVEC or pcDNA3.3 vectors and different combinations were used to produce HL and LH cell lines. We have shown that Ab production has been low and comparable between HL and LH cells until selection on methotrexate (MTX) when LH but not HL cells have responded with 3.5 times increased productivity. Flow cytometry analysis has demonstrated that intracellular concentration of full size Abs in LH cells was 5.6 times higher than in HL ones due to higher amount of H chain synthesis. No differences in viability between HL and LH cells have been found. We have concluded that the expression of H chain in the pOptiVEC vector, which is responsible for MTX resistance, has led to the suppression of H chain synthesis and limitation in full Ab assembly.
机译:肿瘤坏死因子-α(TNF-α)在类风湿关节炎和其他一些自身免疫性疾病中起关键作用。抗TNF-α重组抗体(Ab)的治疗似乎非常有效。生产新的高产真核细胞系可以降低治疗成本,目前这是非常高的。但是,由于哺乳动物细胞中蛋白质转录,翻译,加工和分泌的复杂性,影响抗体表达的阶段仍然很难确定。这项工作的目的是比较用二价叶酸还原酶缺陷的CHO DG44细胞中开发的两种细胞系的生产力,这些细胞用在不同选择元件组合下携带嵌合抗体重链(H)或轻链(L)的载体转染。 H链和L链均克隆到pOptiVEC或pcDNA3.3载体中,并使用不同的组合产生HL和LH细胞系。我们已经表明,直到LH而不是HL细胞以3.5倍的生产率响应时,在甲氨蝶呤(MTX)上进行选择之前,直到HL和LH细胞之间的Ab产量都较低,并且相当。流式细胞仪分析表明,由于H链合成量较高,LH细胞中全尺寸Abs的细胞内浓度比HL高5.6倍。 HL和LH细胞之间的生存力没有发现差异。我们已经得出结论,负责MTX抗性的pOptiVEC载体中H链的表达已导致H链合成的抑制和完全Ab装配中的限制。

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