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固定化“仿生”配体的亲和色谱法。一种免疫球蛋白G结合配体的合成、固定化及色谱评估。

Affinity chromatography on immobilized "biomimetic" ligands. Synthesis, immobilization and chromatographic assessment of an immunoglobulin G-binding ligand.

作者信息

Teng S F, Sproule K, Husain A, Lowe C R

机构信息

Institute of Biotechnology, University of Cambridge, UK.

出版信息

J Chromatogr B Biomed Sci Appl. 2000 Mar 31;740(1):1-15.

Abstract

A synthetic bifunctional ligand (22/8) comprising a triazine scaffold substituted with 3-aminophenol (22) and 4-amino-1-naphthol (8) has been designed, synthesised, characterised and immobilized on agarose beads to create a robust, highly selective affinity adsorbent for human immunoglobulin G (IgG). Scatchard analysis of the binding isotherm for IgG on immobilized 22/8 (90 micromol 22/8/g moist weight gel) indicated an affinity constant (Ka) of 1.4 x 10(5) M(-1) and a theoretical maximum capacity of 151.9 mg IgG/g moist weight gel. The adsorbent shows similar selectivity to immobilized protein A and binds IgG from a number of species. An apparent capacity of 51.9 mg human IgG/g moist weight gel was observed under the experimental conditions selected for adsorption. Human IgG was eluted with glycine-HCl buffer with a recovery of 67-69% and a purity of 97.3-99.2%, depending on the pH value of the buffer used for elution. Preparative chromatography of IgG from human plasma showed that under the specified conditions, 94.4% of plasma IgG was adsorbed and 60% subsequently eluted with a purity of 92.5%. The immobilized ligand was able to withstand incubation in 1 M NaOH for 7 days without loss of binding capacity for IgG.

摘要

一种合成双功能配体(22/8)已被设计、合成、表征并固定在琼脂糖珠上,该配体由被3-氨基苯酚(22)和4-氨基-1-萘酚(8)取代的三嗪支架组成,用于制备一种坚固、高选择性的人免疫球蛋白G(IgG)亲和吸附剂。对固定化22/8(90微摩尔22/8/克湿重凝胶)上IgG的结合等温线进行Scatchard分析,结果表明亲和常数(Ka)为1.4×10⁵ M⁻¹,理论最大容量为151.9毫克IgG/克湿重凝胶。该吸附剂对固定化蛋白A表现出相似的选择性,并能结合多种物种的IgG。在选定的吸附实验条件下,观察到人IgG的表观容量为51.9毫克/克湿重凝胶。用甘氨酸-HCl缓冲液洗脱人IgG,回收率为67-69%,纯度为97.3-99.2%,具体取决于用于洗脱的缓冲液的pH值。从人血浆中制备色谱法分离IgG的结果表明,在特定条件下,94.4%的血浆IgG被吸附,随后60%被洗脱,纯度为92.5%。固定化配体能够在1 M NaOH中孵育7天而不丧失对IgG的结合能力。

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