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恶性疟原虫FK506结合蛋白35(PfFKBP35)的表达、纯化及分子特征分析

Expression, purification, and molecular characterization of Plasmodium falciparum FK506-binding protein 35 (PfFKBP35).

作者信息

Yoon Hye Rim, Kang Cong Bao, Chia Joel, Tang Kai, Yoon Ho Sup

机构信息

Division of Structural and Computational Biology, School of Biological Sciences, Nanyang Technological University, 60 Nanyang Drive, Singapore 637551, Singapore.

出版信息

Protein Expr Purif. 2007 May;53(1):179-85. doi: 10.1016/j.pep.2006.12.019. Epub 2006 Dec 30.

Abstract

The immunosuppressive drug FK506 binds its targets FK506-binding protein (FKBP) family and modulates cellular processes. Recent studies demonstrated that FK506 shows anti-malaria effects. Newly identified FK506-binding protein 35 from Plasmodium falciparum (PfFKBP35) is assumed to be the molecular target of FK506 in the parasite. Currently, molecular and structural basis of growth inhibition of the parasite by FK506 remains unclear. In this study, to examine characteristics of PfFKBP35 and also understand its molecular mechanism of the inhibition by FK506, we have cloned, expressed, and purified the full-length PfFKBP35 and its FK506-binding domain (FKBD). We demonstrate that the full-length PfFKBP35 and the FKBD were properly folded, and suitable for biochemical and biophysical studies. PfFKBP35 showed a basal activity in inhibiting the phosphatase activity of calcineurin in the absence of FK506, but the presence of FK506 greatly enhanced its calcineurin-inhibitory activity. Our NMR data indicate that the FKBD binds FK506 with a high affinity.

摘要

免疫抑制药物FK506与其靶标FK506结合蛋白(FKBP)家族结合并调节细胞过程。最近的研究表明FK506具有抗疟疾作用。新鉴定出的来自恶性疟原虫的FK506结合蛋白35(PfFKBP35)被认为是寄生虫中FK506的分子靶标。目前,FK506抑制寄生虫生长的分子和结构基础仍不清楚。在本研究中,为了研究PfFKBP35的特性并了解其被FK506抑制的分子机制,我们克隆、表达并纯化了全长PfFKBP35及其FK506结合结构域(FKBD)。我们证明全长PfFKBP35和FKBD正确折叠,适用于生化和生物物理研究。PfFKBP35在没有FK506的情况下显示出抑制钙调神经磷酸酶磷酸酶活性的基础活性,但FK506的存在大大增强了其钙调神经磷酸酶抑制活性。我们的核磁共振数据表明FKBD与FK506具有高亲和力结合。

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