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人源PER.C6(®)细胞产生的重组人抗-D-IgG1抗体的效应子特性和糖基化模式

Effector properties and glycosylation patterns of recombinant human anti-D-IgG1 antibodies produced by human PER.C6(®) cells.

作者信息

Olovnikova N I, Grigorieva O V, Petrov A V

机构信息

Hematology Research Center, Ministry of Health and Social Development of the Russian Federation, Russia.

出版信息

Bull Exp Biol Med. 2012 Dec;154(2):245-9. doi: 10.1007/s10517-012-1923-1.

Abstract

Creation of effective monoclonal anti-D immunoglobulin for prevention of hemolytic disease of the newborn remains an unsolved problem because there is still no producer cell strain providing stable production and adequate glycosylation of antibodies. Recombinant anti-D have been obtained on the basis of human PER.C6(®) cells and characterized. Anti-D antibodies expressed in PER.C6(®) exhibited lower hemolytic activity in antibody-dependent cytotoxicity (ADCC) reaction mediated by low-affinity Fcγ receptors in comparison with identical antibodies of lymphoblastoid origin. Monoclonal antibodies produced by PER.C6(®) are completely fucosylated and desialylated, i.e. are characterized by abnormal glycosylation. Addition of kifunensine (α-mannosidase I inhibitor) to the medium led to production of antibodies with high hemolytic activity. Reduced activity of monoclonal antibodies in PER.C6(®) cells and the effect of kifunensine (causing synthesis of defucosylated glycans) suggest that the absence of fucose is the key factor responsible for Fc affinity for low-affinity receptors.

摘要

由于仍然没有能够稳定生产并使抗体进行充分糖基化的生产细胞系,因此制备用于预防新生儿溶血病的有效单克隆抗-D免疫球蛋白仍是一个未解决的问题。基于人PER.C6(®)细胞已获得重组抗-D并对其进行了表征。与源自淋巴母细胞样的相同抗体相比,在PER.C6(®)中表达的抗-D抗体在由低亲和力Fcγ受体介导的抗体依赖性细胞毒性(ADCC)反应中表现出较低的溶血活性。由PER.C6(®)产生的单克隆抗体完全岩藻糖基化且去唾液酸化,即具有异常糖基化的特征。向培养基中添加基弗那辛(α-甘露糖苷酶I抑制剂)导致产生具有高溶血活性的抗体。PER.C6(®)细胞中单克隆抗体活性的降低以及基弗那辛的作用(导致去岩藻糖基化聚糖的合成)表明,岩藻糖的缺失是导致Fc对低亲和力受体亲和力的关键因素。

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