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使用自下而上和自上而下相结合的氢-氘交换质谱法对抗体生物类似药进行高阶结构比较分析。

Comparative higher-order structure analysis of antibody biosimilars using combined bottom-up and top-down hydrogen-deuterium exchange mass spectrometry.

作者信息

Pan Jingxi, Zhang Suping, Borchers Christoph H

机构信息

University of Victoria-Genome British Columbia Proteomics Centre, Vancouver Island Technology Park, #3101-4464 Markham St., Victoria, BC V8Z 7X8, Canada.

MRM Proteomics Inc., Victoria, BC, Canada.

出版信息

Biochim Biophys Acta. 2016 Dec;1864(12):1801-1808. doi: 10.1016/j.bbapap.2016.08.013. Epub 2016 Aug 25.

DOI:10.1016/j.bbapap.2016.08.013
PMID:27569733
Abstract

Hydrogen/deuterium exchange (HDX) coupled with mass spectrometry (MS) is a powerful technique for higher-order structural characterization of antibodies. Although the peptide-based bottom-up HDX approach and the protein-based top-down HDX approach have complementary advantages, the work done so far on biosimilars has involved only one or the other approach. Herein we have characterized the structures of two bevacizumab (BEV) biosimilars and compared them to the reference BEV using both methods. A sequence coverage of 87% was obtained for the heavy chain and 74% for the light chain in the bottom-up approach. The deuterium incorporation behavior of the peptic peptides from the three BEVs were compared side by side and showed no differences at various HDX time points. Top-down experiments were carried out using subzero temperature LC-MS, and the deuterium incorporation of the intact light chain and heavy chain were obtained. Top-down ETD was also performed to obtain amino acid-level HDX information that covered 100% of the light chain, but only 50% coverage is possible for the heavy chain. Consistent with the intact subunit level data, no differences were observed in the amino acid level HDX data. All these results indicate that there are no differences between the three BEV samples with respect to their high-order structures. The peptide level information from the bottom-up approach, and the residue level and intact subunit level information from the top-down approach were complementary and covered the entire antibody.

摘要

氢/氘交换(HDX)与质谱(MS)联用是一种用于抗体高阶结构表征的强大技术。尽管基于肽段的自下而上HDX方法和基于蛋白质的自上而下HDX方法具有互补优势,但迄今为止在生物类似药方面所做的工作仅涉及其中一种方法。在此,我们使用这两种方法对两种贝伐单抗(BEV)生物类似药的结构进行了表征,并将它们与参比BEV进行了比较。在自下而上的方法中,重链的序列覆盖率为87%,轻链为74%。对三种BEV的胃蛋白酶消化肽段的氘掺入行为进行了并排比较,发现在不同的HDX时间点没有差异。使用低温液相色谱-质谱进行自上而下的实验,获得了完整轻链和重链的氘掺入情况。还进行了自上而下的电子转移解离(ETD)以获得覆盖轻链100%的氨基酸水平HDX信息,但重链只能覆盖50%。与完整亚基水平数据一致,在氨基酸水平HDX数据中未观察到差异。所有这些结果表明,三种BEV样品在高阶结构方面没有差异。自下而上方法的肽段水平信息,以及自上而下方法的残基水平和完整亚基水平信息是互补的,覆盖了整个抗体。

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