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通过 LC 和 LC-MS 分析三种促红细胞生成素 α 产品表明糖基化关键质量属性(包括唾液酸含量)存在差异。

Analysis of Three Epoetin Alpha Products by LC and LC-MS Indicates Differences in Glycosylation Critical Quality Attributes, Including Sialic Acid Content.

机构信息

Reading School of Pharmacy, University of Reading , Reading, Berkshire RG6 6AP, United Kingdom.

Ludger, Ltd. , Culham Science Centre, Abingdon, Oxfordshire OX14 3EB, United Kingdom.

出版信息

Anal Chem. 2017 Jun 20;89(12):6455-6462. doi: 10.1021/acs.analchem.7b00353. Epub 2017 Jun 9.

Abstract

Erythropoietin (EPO) is one of the main therapeutics used to treat anemic patients, greatly improving their quality of life. In this study, biosimilars Binocrit and a development product, called here CIGB-EPO, were compared to the originator product, Eprex. All three are epoetin alpha products, reputed to have similar glycosylation profiles. The quality, safety, and efficacy of this biotherapeutic depend on the following glycosylation critical quality attributes (GCQAs): sialylation, N-glycolyl-neuraminic acid (Neu5Gc) content, branching, N-acetyl-lactosamine (LacNAc) extensions, and O-acetylation pattern. Reverse-phase ultra-high-pressure liquid chromatography (RP-UHPLC) analysis of acid-released, 1,2-diamino-4,5-methylenedioxybenzene (DMB) labeled sialic acid derivatives and hydrophilic interaction liquid chromatography (HILIC) in combination with mass spectrometry (HILIC-UHPLC-MS) of procainamide (PROC) labeled N-glycans were the analytical tools used. An automated method for enzymatic release and PROC labeling was applied for the first time to the erythropoiesis stimulating agent (ESA) products, which facilitated novel, in-depth characterization, and allowed identification of precise structural features including the location of O-acetyl groups on sialic acid (SA) moieties. Samples were digested by a sialate-O-acetylesterase (NanS) to confirm the presence of O-acetyl groups. It was found that Eprex contained the greatest relative abundance of O-acetylated derivatives, Binocrit expressed the least Neu5Gc, and CIGB-EPO showed the greatest variety of high-mannose-phosphate structures. The sialylation and LacNAc extension patterns of the three ESAs were similar, with a maximum of four N-acetyl-neuraminic acid (Neu5Ac) moieties detected per glycan. Such differences in SA derivatization, particularly O-acetylation, could have consequences for the quality and safety of a biotherapeutic, as well as its efficacy.

摘要

促红细胞生成素(EPO)是治疗贫血患者的主要治疗方法之一,可显著提高患者的生活质量。在这项研究中,将生物仿制药 Binocrit 和一种开发产品(此处称为 CIGB-EPO)与原研产品 Eprex 进行了比较。所有这三种产品都是促红细胞生成素 α 产品,据称其糖基化谱相似。这种生物治疗药物的质量、安全性和疗效取决于以下糖基化关键质量属性(GCQAs):唾液酸化、N-糖基化神经氨酸(Neu5Gc)含量、分支、N-乙酰乳糖胺(LacNAc)延伸和 O-乙酰化模式。用于分析的方法是反相超高压液相色谱(RP-UHPLC)分析酸释放的 1,2-二氨基-4,5-亚甲基二氧基苯(DMB)标记的唾液酸衍生物和亲水相互作用液相色谱(HILIC)与丙酰氨基酚(PROC)标记的 N-聚糖的结合(HILIC-UHPLC-MS)。首次将一种用于酶释放和 PROC 标记的自动化方法应用于促红细胞生成刺激剂(ESA)产品,这促进了对 ESA 产品的新的深入表征,并能够确定包括唾液酸(SA)部分上 O-乙酰基位置在内的精确结构特征。通过唾液酸-O-乙酰酯酶(NanS)对样品进行消化,以确认 O-乙酰基的存在。结果发现,Eprex 含有最多的相对丰度的 O-乙酰化衍生物,Binocrit 表达的 Neu5Gc 最少,而 CIGB-EPO 则显示出最多的高甘露糖磷酸结构变化。三种 ESA 的唾液酸化和 LacNAc 延伸模式相似,每个聚糖最多检测到四个 N-乙酰神经氨酸(Neu5Ac)部分。这种 SA 衍生化,特别是 O-乙酰化的差异,可能会对生物治疗药物的质量和安全性以及其疗效产生影响。

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