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毕赤酵母中β-甘露糖聚糖结构的消除。

Elimination of β-mannose glycan structures in Pichia pastoris.

机构信息

GlycoFi Inc., A wholly-Owned Subsidiary of Merck & Co. Inc., 21 Lafayette street, Suite 200, Lebanon, NH 03766, USA.

出版信息

Glycobiology. 2011 Dec;21(12):1616-26. doi: 10.1093/glycob/cwr108. Epub 2011 Aug 12.

Abstract

The methylotrophic yeast, Pichia pastoris, is an important organism used for the production of therapeutic proteins. However, the presence of fungal-like glycans, such as those containing β-mannose (Man) linkages, can elicit an immune response or bind to Man receptors, thus reducing their efficacy. Recent studies have confirmed that P. pastoris has four genes from the β-mannosyl transferase (BMT) family and that Bmt2p is responsible for the majority of β-Man linkages on glycans. While expressing recombinant human erythropoietin (rhEPO) in a developmental glycoengineered strain devoid of BMT2 gene expression, cross-reactivity was observed with an antibody raised against host cell antigens. Treatment of the rhEPO with protein N-glycosidase F eliminated cross-reactivity, indicating that the antigen was associated with the glycan. Thorough analysis of the glycan profile of rhEPO demonstrated the presence of low amounts of α-1,2-mannosidase resistant high-Man glycoforms. In an attempt to eliminate the α-mannosidase resistant glycoforms, we used a systemic approach to genetically knock-out the remaining members of the BMT family culminating in a quadruple bmt2,4,1,3 knock-out strain. Data presented here conclude that the additive elimination of Bmt2p, Bmt3p and Bmt1p activities are required for total abolition of β-Man-associated glycans and their related antigenicity. Taken together, the elimination of β-Man containing glycoforms represents an important step forward for the Pichia production platform as a suitable system for the production of therapeutic glycoproteins.

摘要

甲醇营养酵母毕赤酵母是一种用于生产治疗性蛋白的重要生物。然而,真菌样聚糖的存在,如含有β-甘露糖(Man)键的聚糖,会引发免疫反应或与 Man 受体结合,从而降低其疗效。最近的研究证实,毕赤酵母有四个来自β-甘露糖基转移酶(BMT)家族的基因,Bmt2p 负责聚糖中大多数β-Man 键的形成。在一个缺乏 Bmt2 基因表达的发育性糖基工程化菌株中表达重组人红细胞生成素(rhEPO)时,观察到与针对宿主细胞抗原的抗体发生交叉反应。用蛋白 N-糖基酶 F 处理 rhEPO 消除了交叉反应,表明抗原与聚糖有关。对 rhEPO 聚糖谱的彻底分析表明,存在低量的α-1,2-甘露糖苷酶抗性高-Man 糖型。为了消除α-甘露糖苷酶抗性糖型,我们采用系统的方法对 BMT 家族的其余成员进行基因敲除,最终得到一个四重 bmt2,4,1,3 敲除菌株。这里呈现的数据表明,需要消除 Bmt2p、Bmt3p 和 Bmt1p 的活性,才能完全消除β-Man 相关聚糖及其相关抗原性。总之,消除含有β-Man 的糖型是毕赤酵母生产平台向前迈进的重要一步,因为它是生产治疗性糖蛋白的合适系统。

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