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Increasing Secretion of a Bivalent Anti-T-Cell Immunotoxin by Pichia pastoris

机译:毕赤酵母增加了二价抗T细胞免疫毒素的分泌

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摘要

The bivalent anti-T-cell immunotoxin A-dmDT390-bisFv(G4S) was developed for treatment of T-cell leukemia and autoimmune diseases and for tolerance induction for transplantation. This immunotoxin was produced extracellularly in toxin-sensitive Pichia pastoris JW102 (Mut+) under control of the AOX1 promoter. There were two major barriers to efficient immunotoxin production, the toxicity of the immunotoxin for P. pastoris and the limited capacity of P. pastoris to secrete the immunotoxin. The immunotoxin toxicity resulted in a decrease in the methanol consumption rate, cessation of cell growth, and low immunotoxin productivity after the first 22 h of methanol induction. Continuous cell growth and continuous immunotoxin secretion after the first 22 h of methanol induction were obtained by adding glycerol to the methanol feed by using a 4:1 methanol-glycerol mixed feed as an energy source and by continuously adding a yeast extract solution during methanol induction. The secretory capacity was increased from 22.5 to 37 mg/liter by lowering the induction temperature. A low temperature reduced the methanol consumption rate and protease activity in the supernatant but not cell growth. The effects of adding glycerol and yeast extract to the methanol feed were synergistic. Adding yeast extract primarily enhanced methanol utilization and cell growth, while adding glycerol primarily enhanced immunotoxin production. The synergy was further enhanced by decreasing the induction temperature from 23 to 15°C, which resulted in a robust process with a yield of 37 mg/liter, which was sevenfold greater than the yield previously reported for a toxin-resistant CHO cell expression system. This methodology should be applicable to other toxin-related recombinant proteins in toxin-sensitive P. pastoris.
机译:开发了二价抗T细胞免疫毒素A-dmDT390-bisFv(G4S),用于治疗T细胞白血病和自身免疫性疾病,并诱导移植耐受。这种免疫毒素是在AOX1启动子的控制下在毒素敏感的巴斯德毕赤酵母JW102(Mut +)中在细胞外产生的。有效产生免疫毒素有两个主要障碍,即免疫毒素对巴斯德毕赤酵母的毒性和巴斯德毕赤酵母分泌免疫毒素的能力有限。免疫毒素毒性导致甲醇诱导的最初22小时后,甲醇消耗速率降低,细胞生长停止以及免疫毒素生产率降低。通过使用4:1甲醇-甘油混合饲料作为能源,向甲醇饲料中添加甘油,并在甲醇诱导过程中连续添加酵母提取物溶液,可以在甲醇诱导的最初22小时内获得连续的细胞生长和连续的免疫毒素分泌。 。通过降低诱导温度,分泌能力从22.5增加到37 mg / L。低温降低了上清液中的甲醇消耗速率和蛋白酶活性,但未降低细胞生长。在甲醇进料中添加甘油和酵母提取物的效果是协同的。添加酵母提取物主要增强甲醇利用率和细胞生长,而添加甘油主要增强免疫毒素的产生。通过将诱导温度从23降低到15°C,协同作用得到了进一步增强,这导致了稳健的过程,产量为37 mg / L,比以前报道的抗毒素CHO细胞表达系统的产量高出七倍。该方法应适用于毒素敏感巴斯德毕赤酵母中其他与毒素有关的重组蛋白。

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