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一种新型氧化亲和素的生化和生物学特性及其组织结合性能的增强。

Biochemical and biological characterization of a new oxidized avidin with enhanced tissue binding properties.

机构信息

Research and Development Department, Tecnogen SpA, Piana di Monte Verna, 81013 Caserta, Italy.

出版信息

J Biol Chem. 2010 Mar 19;285(12):9090-9. doi: 10.1074/jbc.M109.080457. Epub 2010 Jan 25.

Abstract

Chicken avidin and bacterial streptavidin are widely employed in vitro for their capacity to bind biotin, but their pharmacokinetics and immunological properties are not always optimal, thereby limiting their use in medical treatments. Here we investigate the biochemical and biological properties of a new modified avidin, obtained by ligand-assisted sodium periodate oxidation of avidin. This method allows protection of biotin-binding sites of avidin from inactivation caused by the oxidation step and delay of avidin clearance from injected tissue by generation of aldehyde groups from avidin carbohydrate moieties. Oxidized avidin shows spectroscopic properties similar to that of native avidin, indicating that tryptophan residues are spared from oxidation damage. In strict agreement with these results, circular dichroism and isothermal titration calorimetry analyses confirm that the ligand-assisted oxidation preserves the avidin protein structure and its biotin binding capacity. In vitro cell binding and in vivo tissue residence experiments demonstrate that aldehyde groups provide oxidized avidin the property to bind cellular and interstitial protein amino groups through Schiff's base formation, resulting in a tissue half-life of 2 weeks, compared with 2 h of native avidin. In addition, the efficient uptake of the intravenously injected (111)In-BiotinDOTA (ST2210) in the site previously treated with modified avidin underlines that tissue-bound oxidized avidin retains its biotin binding capacity in vivo. The results presented here indicate that oxidized avidin could be employed to create a stable artificial receptor in diseased tissues for the targeting of biotinylated therapeutics.

摘要

鸡亲和素和细菌链霉亲和素因其结合生物素的能力而被广泛应用于体外,但它们的药代动力学和免疫特性并不总是最佳的,从而限制了它们在医疗中的应用。在这里,我们研究了一种新的修饰亲和素的生化和生物学特性,该亲和素是通过亲和素的配体辅助的高碘酸钠氧化获得的。这种方法可以保护亲和素的生物素结合位点免受氧化步骤引起的失活,并通过亲和素碳水化合物部分的醛基生成延迟亲和素从注射组织中的清除。氧化亲和素表现出与天然亲和素相似的光谱特性,表明色氨酸残基免受氧化损伤。与这些结果完全一致,圆二色性和等温热滴定分析证实,配体辅助的氧化保留了亲和素蛋白结构及其生物素结合能力。体外细胞结合和体内组织驻留实验表明,醛基通过席夫碱形成赋予氧化亲和素结合细胞和间质蛋白氨基的能力,导致组织半衰期为 2 周,而天然亲和素为 2 小时。此外,静脉注射的 (111)In-BiotinDOTA(ST2210)在先前用修饰亲和素处理的部位的有效摄取突出表明,组织结合的氧化亲和素在体内保留其生物素结合能力。这里呈现的结果表明,氧化亲和素可用于在患病组织中创建稳定的人工受体,以靶向生物素化治疗剂。

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