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中间向下片段化用于鉴定和定量 IgG1 分子中特定位置的甲硫氨酸氧化。

Middle-down fragmentation for the identification and quantitation of site-specific methionine oxidation in an IgG1 molecule.

机构信息

Department of Process and Product Development, Amgen, Inc., USA.

出版信息

J Pharm Sci. 2010 Nov;99(11):4469-76. doi: 10.1002/jps.22158.

Abstract

A middle-down LC/MS approach, for the rapid quantitation and characterization of site-specific methionine oxidation in a recombinant monoclonal IgG1 molecule, is described. An IgG1 antibody was digested with endoprotease LysC under limited proteolytic conditions to produce two major components; an antigen binding fragment (Fab) and a crystallizable fraction (Fc). These fractions were then reduced to produce three major species; light chain (LC), Fc/2 which is the C terminal region of the heavy chain (HC) and the N-terminal heavy chain region (Fd). These three fragments were separated by reversed-phase HPLC using a diphenyl column. The diphenyl column resolved site-specific methionine oxidation in all three subunits. Middle-down N-terminal sequencing with a LCT premier mass spectrometer was used to identify the sites of oxidation in the LC. Sites of oxidation in the Fc/2 were identified using middle-down collision-induced dissociation (CID) on a Qtof premier. This method allowed for the rapid quantitation and identification of oxidation on each methionine residue in an IgG1 molecule.

摘要

描述了一种中低分辨率 LC/MS 方法,用于快速定量和鉴定重组单克隆 IgG1 分子中特定位置甲硫氨酸氧化。用内切蛋白酶 LysC 在有限的蛋白水解条件下消化 IgG1 抗体,产生两个主要成分;抗原结合片段 (Fab) 和可结晶片段 (Fc)。然后将这些片段还原生成三种主要物质;轻链 (LC)、Fc/2 是重链 (HC) 的 C 末端区域和 N 末端重链区域 (Fd)。这三个片段通过反相 HPLC 用二苯基柱分离。二苯基柱在所有三个亚基中都能分辨出特定位置的甲硫氨酸氧化。用 LCT premier 质谱仪进行中低分辨率 N 端测序以鉴定 LC 中氧化的位置。用 Qtof premier 上的中低分辨率碰撞诱导解离 (CID) 鉴定 Fc/2 中的氧化位点。该方法允许快速定量和鉴定 IgG1 分子中每个甲硫氨酸残基上的氧化。

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