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PEG-chitosan and glycol-chitosan for improvement of biopharmaceutical properties of recombinant L-asparaginase from Erwinia carotovora

机译:PEG-壳聚糖和乙二醇-壳聚糖用于改善胡萝卜软腐欧文氏菌重组L-天冬酰胺酶的生物制药性能

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摘要

Conjugation with the new branched copolymers, PEG-chitosan and glycol-chitosan, is suggested to improve the therapeutic properties of L-asparaginase from Erwinia carotovora (EwA). The structure and composition of such conjugates were optimized for maximal catalytic efficiency (k cat/K M) under physiological conditions, yielding improvement by a factor of 3-6 compared to the native enzyme. This effect is attributed mainly to the shift of pH activity profile towards lower pH values due to the polycationic nature of the copolymer. The thermostability of EwA conjugates was also considerably improved. Chito-PEGylation, similarly to PEGylation, can be expected to improve pharmacokinetic properties and to reduce immunogenicity of this medically relevant enzyme. It is worth mentioning that a new versatile approach based on IR spectroscopy has been developed to determine PEG-chitosan copolymer composition as well as composition of copolymer-enzyme conjugates. The proposed analytic method is "reagent-free" and allows fast and reliable determination of parameters of interest from the single IR spectrum in contrast to laborious and unreliable methods based on polymer free amino group titration with TNBS and OPA.
机译:建议与新的支链共聚物PEG-壳聚糖和乙二醇-壳聚糖结合使用,以改善来自胡萝卜欧文氏菌(EwA)的L-天冬酰胺酶的治疗性能。对此类缀合物的结构和组成进行了优化,以在生理条件下实现最大催化效率(k cat / K M),与天然酶相比,可提高3-6倍。这种影响主要归因于由于共聚物的聚阳离子性质,pH活性曲线向较低的pH值转移。 EwA缀合物的热稳定性也得到了显着改善。与聚乙二醇化相似,壳聚乙二醇化可望改善药代动力学性质并降低该医学上相关酶的免疫原性。值得一提的是,已经开发出一种新的基于IR光谱的通用方法来确定PEG-壳聚糖共聚物的组成以及共聚物-酶结合物的组成。与基于TNBS和OPA的无聚合物氨基滴定的费力且不可靠的方法相比,所提出的分析方法是“无试剂”的,并且可以从单个IR光谱中快速,可靠地确定目标参数。

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