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首页> 外文期刊>RSC Advances >Engineering O-glycosylation in modified N-linked oligosaccharide (Man(12)GlcNAc(2)similar to Man(16)GlcNAc(2)) Pichia pastoris strains
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Engineering O-glycosylation in modified N-linked oligosaccharide (Man(12)GlcNAc(2)similar to Man(16)GlcNAc(2)) Pichia pastoris strains

机译:改性N-连接的寡糖(Man(12)Glcnac(2)与人(16)Glcnac(2)类似的人(12))的工程o-糖基化(2))Pichia Pastoris菌株

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摘要

Yeast have been engineered for the production of therapeutic glycoproteins with humanized N-linked oligosaccharides. Both N- and O-linked oligosaccharides engineered yeast have been attractive prospects, since yeast-specific O-mannosylated proteins were reported to induce an aberrant immune response and alter pharmacokinetics in vivo. In the present study, we genetically manipulated O-glycosylation by disrupting O-mannosyltransferase PMT1 and PMT5 in a low-mannose type N-linked oligosaccharide (Man(12)GlcNAc(2)similar to Man(16)GlcNAc(2)) engineered Pichia pastoris strain to produce therapeutic glycoproteins. The O-mannosyltransferase PMT1 mutant produces anti-Her-2 antibodies with reduced O-linked oligosaccharides and protein degradation, but this strain exhibited growth defects. However, the deletion of O-mannosyltransferase PMT5 individually has a minimal effect on O-glycosylation, degradation of the anti-Her-2 antibody, and strain growth. Thus, by disrupting O-mannosyltransferase PMT1 in an N-glycosylation engineered Pichia pastoris strain, we generated an effective glycoengineered Pichia pastoris strain to effectively produce therapeutic glycoproteins with both engineered N-and O-linked oligosaccharides.
机译:酵母已经设计用于生产治疗性糖蛋白与人源化的N-连接的低聚糖。由于据报道酵母特异性O-甘露糖基化蛋白据报道酵母特异性的O-甘露糖基化蛋白,因此促使酵母特异性的O-甘露糖基蛋白和体内改变药代动力学,因此均有吸引力的前景。在本研究中,通过在低甘露糖型N-连接的低聚糖(MAN(12)GLCNAC(2)中破坏O-甘露那糖基转移酶PMT1和PMT5,遗传地操纵O-糖基化学化(16)GLCNAC(2)的MAN(12)GLCNAC(2)) Pichia Pastoris菌株产生治疗糖蛋白。 O-甘露糖基转移酶PMT1突变体产生抗HER-2抗体,其具有降低的O型寡糖和蛋白质降解,但这种应变表现出生长缺陷。然而,O-甘露糖基转移酶PMT5的缺失单独对O-糖基化,抗HER-2抗体的降解和菌株生长的最小影响。因此,通过在N-糖基化学化的Pichia牧场菌中破坏O-甘露糖基转移酶PMT1,我们产生了有效的甘油化肽牧场菌菌株,以有效地产生具有工程化的N-和O连接的低聚糖的治疗糖蛋白。

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  • 来源
    《RSC Advances 》 |2019年第15期| 共7页
  • 作者单位

    Beijing Inst Biotechnol Beijing 100071 Peoples R China;

    Beijing Inst Biotechnol Beijing 100071 Peoples R China;

    Beijing Inst Biotechnol Beijing 100071 Peoples R China;

    Beijing Inst Biotechnol Beijing 100071 Peoples R China;

    Huanghuai Univ Sch Biol &

    Food Engn Zhumadian 463000 Peoples R China;

    Huanghuai Univ Sch Biol &

    Food Engn Zhumadian 463000 Peoples R China;

    Beijing Inst Biotechnol Beijing 100071 Peoples R China;

    Beijing Inst Biotechnol Beijing 100071 Peoples R China;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 化学 ;
  • 关键词

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