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首页> 外文期刊>RSC Advances >Assessment of the interacting mechanism between Candida rugosa lipases and hydroxyapatite and identification of the hydroxyapatite-binding sequence through proteomics and molecular modelling
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Assessment of the interacting mechanism between Candida rugosa lipases and hydroxyapatite and identification of the hydroxyapatite-binding sequence through proteomics and molecular modelling

机译:评估念珠菌脂肪酶与羟基磷灰石和羟基磷灰石结合序列蛋白质组学的鉴定的评估

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摘要

Hydroxyapatite (HAP), a calcium-phosphate bioactive ceramic, is actively employed in medical and separation sciences. Although different classes of biomacromolecules interact with this material, interactions with proteins are the most important, since they directly affect the biocompatibility of the carrier and it's industrial application. In the presented work, we thoroughly investigate and elucidate the interaction mechanism between Candida rugosa lipase (CRL) upon it's immobilization on HAP, since this immobilized enzyme showed advanced catalytic properties in previous studies. Applying elution and protein modification strategies we concluded that Ca-chelation of HAP's C-site and CRL's -COOH groups is the most probable interacting mechanism. A proteomics approach revealed that this chelation is conserved throughout all CRL isoforms, while results of molecular modelling led us to propose the involvement of a specific region of the protein surface and side chains in interactions with HAP.
机译:羟基磷灰石(HAP),磷酸钙的生物活性陶瓷,正在积极在医疗和科学分离使用。虽然不同类型的生物大分子用这种材料相互作用的,与蛋白质的相互作用是最重要的,因为它们直接影响到运营商的生物相容性和它的工业应用。在所提出的工作中,我们深入调查,并在其上的固定在HAP阐明皱褶假丝酵母脂肪酶(CRL)之间的相互作用机制,因为这种固定化酶显示出在以往的研究先进的催化性能。应用洗脱和蛋白质修饰策略,我们得出的结论是HAP的C-网站和CRL的-COOH基团的钙,螯合是最有可能的互动机制。蛋白质组学方法发现,该螯合在所有CRL亚型保守的,而分子模拟的结果使我们提出的蛋白质表面和侧链的特定区域的与HAP相互作用的参与。

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