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Producing recombinant therapeutic glycoproteins with enhanced sialylation using CHO-gmt4 glycosylation mutant cells

机译:使用CHO-gmt4糖基化突变细胞生产具有增强唾液酸化作用的重组治疗性糖蛋白

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摘要

Recombinant glycoprotein drugs require proper glycosylation for optimal therapeutic efficacy. Glycoprotein therapeutics are rapidly removed from circulation and have reduced efficacy if they are poorly sialylated. Ricinus communis agglutinin-I (RCA-I) was found highly toxic to wild-type CHO-K1 cells and all the mutants that survived RCA-I treatment contained a dysfunctional N-acetylglucosaminyltransferase I (GnT I) gene. These mutants are named CHO-gmt4 cells. Interestingly, upon restoration of GnT I, the sialylation of a model glycoprotein, erythropoietin, produced in CHO-gmt4 cells was shown to be superior to that produced in wild-type CHO-K1 cells. This addendum summarizes the applicability of this cell line, from transient to stable expression of the recombinant protein, and from a lab scale to an industrial scale perfusion bioreactor. In addition, CHO-gmt4 cells can be used to produce glycoproteins with mannose-terminated N-glycans. Recombinant glucocerebrosidase produced by CHO-gmt4 cells will not require glycan remodeling and may be directly used to treat patients with Gaucher disease. CHO-gmt4 cells can also be used to produce other glycoprotein therapeutics which target cells expressing mannose receptors.
机译:重组糖蛋白药物需要适当的糖基化才能获得最佳治疗效果。糖蛋白治疗剂从唾液中迅速清除,如果唾液酸化程度较差,则疗效会降低。发现蓖麻蓖​​麻凝集素-I(RCA-I)对野生型CHO-K1细胞具有高毒性,并且所有在RCA-I处理中幸存的突变体均含有功能异常的N-乙酰氨基葡萄糖氨基转移酶I(GnT I)基因。这些突变体被称为CHO-gmt4细胞。有趣的是,在恢复GnT I后,在CHO-gmt4细胞中产生的模型糖蛋白促红细胞生成素的唾液酸化作用优于在野生型CHO-K1细胞中产生的唾液酸化作用。该附录总结了该细胞系的适用性,从瞬时表达到稳定表达的重组蛋白,从实验室规模到工业规模的灌注生物反应器。此外,CHO-gmt4细胞可用于产生带有甘露糖末端的N-聚糖的糖蛋白。 CHO-gmt4细胞产生的重组葡糖脑苷脂酶不需要聚糖重塑,可以直接用于治疗高雪氏病患者。 CHO-gmt4细胞也可用于产生其他糖蛋白治疗药物,这些药物靶向表达甘露糖受体的细胞。

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