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Comparative structural modeling and docking studies of uricase: Possible implication in enzyme supplementation therapy for hyperuricemic disorders

机译:尿酸酶的比较结构建模和对接研究:对高尿酸血症疾病的酶补充治疗的可能含义

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摘要

Uricase (EC 1.7.3.3, UC) catalyzes the oxidation of uric acid (UA) to more soluble allantoin thereby lowering plasma UA levels. In humans, when concentration of UA exceeds >7. mg/dl, it leads to hyperuricemia, gout, nephrolithiasis and urolithiasis. A new remedy to cure such metabolic diseases is the enzyme supplementation therapy by UC but with high degree of antigenic independence. Therefore screening of new uricase sources to expand its usefulness and reduced antigenecity is needed. Present study employed cheminformatics approach to construct models of reported UC from different sources viz. . Bacillus megaterium, . Streptomyces bingchenggensis BCW-1, . Paenibacillus sp, . Solibacter usitatus Ellin6076, . Truepera radiovictrix DSM 17093 and . Ktedonobacter racemifer DSM 4496 in order to study their structure-function relationship for enzyme mass production and modification for improved characteristics. BioMed CAChe version 6.1 was further used to study enzyme-substrate interactions of models with uric acid using docking approach. Results indicated that models for UC of . Streptomyces bingchenggensis BCW-1 accounted for better regio-specificity towards UA, supporting the interested metabolism and thus may further be implicated in enzyme supplementation therapy for hyperuricemic associated disorders.
机译:尿酸酶(EC 1.7.3.3,UC)催化尿酸(UA)氧化为更易溶解的尿囊素,从而降低血浆UA水平。在人类中,UA的浓度超过> 7。 mg / dl会导致高尿酸血症,痛风,肾结石和尿石症。治疗此类代谢性疾病的新方法是通过UC进行的酶补充疗法,但具有高度的抗原独立性。因此,需要筛选新的尿酸酶来源以扩大其用途并降低抗原性。本研究采用化学信息学方法从不同来源构建报道的UC模型。 。巨大芽孢杆菌。炳城链霉菌BCW-1,。芽孢杆菌属。乌杆菌(Solibacter usitatus)Ellin6076 ,。 Truepera radiovictrix DSM 17093和。为了研究它们的结构与功能的关系,研究了竞争激烈的竞争细菌DSM 4496,以进行酶的大量生产和修饰以改善特性。 BioMed CAChe版本6.1还用于通过对接方法研究模型与尿酸的酶-底物相互作用。结果表明,UC的UC模型。 bingchenggensis BCW-1链霉菌对UA具有更好的区域特异性,支持感兴趣的代谢,因此可能进一步参与高尿酸血症相关疾病的酶补充治疗。

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