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An afucosylated anti-CD20 monoclonal antibody with greater antibody-dependent cellular cytotoxicity and B-cell depletion and lower complement-dependent cytotoxicity than rituximab

机译:一种岩藻糖基化抗CD20单克隆抗体,与利妥昔单抗相比,具有更高的抗体依赖性细胞毒性和B细胞耗竭性以及更低的补体依赖性细胞毒性

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摘要

The objective of this study was to characterize the in vitro and in vivo activity of a novel afucosylated rituximab (BLX-300) expressed in a Lemna aquatic plant-based system free of zoonotic pathogens. The glycosylation of BLX-300 was shown to be homogeneous, composed of a single major N-glycan species without detectable fucose or xylose. Target cell binding and induction of apoptosis were similar for BLX-300 and rituximab. Antibody-dependent cellular cytotoxicity (ADCC) was increased by BLX-300 versus rituximab in phenylalanine/phenylalanine (F/F), phenylalanine/valine (F/V) and valine/valine (V/V) genotype donors, as indicated by respective log reductions of 0.82, 1.07 and 0.92 in EC 50. BLX-300 also showed greater B-cell depletion than rituximab in whole blood from donors of F/F, F/V and V/V genotype in vitro and cynomolgus monkeys in vivo. Temporal changes in circulating levels of BLX-300 and rituximab were similar in cynomolgus monkeys. Complement-dependent cytotoxicity (CDC) was attenuated by BLX-300 relative to rituximab, as judged by a log increase of 0.51 in EC 50. The higher ADCC and B-cell depletion suggest a potential improvement in effectiveness and potency, while lower CDC may mitigate infusion toxicity.
机译:这项研究的目的是表征在无人畜共患病病原体的以Lemna水生植物为基础的系统中表达的新型岩藻糖基化利妥昔单抗(BLX-300)的体外和体内活性。已显示BLX-300的糖基化是均质的,由单个主要N-聚糖组成,没有可检测到的岩藻糖或木糖。 BLX-300和利妥昔单抗的靶细胞结合和凋亡诱导相似。 BLX-300与利妥昔单抗相比,苯丙氨酸/苯丙氨酸(F / F),苯丙氨酸/缬氨酸(F / V)和缬氨酸/缬氨酸(V / V)基因型供体的抗体依赖性细胞毒性(ADCC)增加EC 50的对数减少了0.82、1.07和0.92。在体外F / F,F / V和V / V基因型供体和食蟹猕猴的全血中,BLX-300还显示出比利妥昔单抗更大的B细胞耗竭。食蟹猴BLX-300和利妥昔单抗循环水平的时间变化相似。相对于利妥昔单抗,BLX-300减弱了补体依赖性细胞毒性(CDC),这是通过EC 50的对数增加0.51来判断的。较高的ADCC和B细胞耗竭量表明其有效性和效力有潜在的改善,而较低的CDC可能减轻输液毒性。

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