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抗疟药耐药蛋白恶性疟原虫氯喹耐药转运蛋白可结合氯喹。

The antimalarial drug resistance protein Plasmodium falciparum chloroquine resistance transporter binds chloroquine.

作者信息

Zhang Hanbang, Paguio Michelle, Roepe Paul D

机构信息

Department of Chemistry, Lombardi Cancer Center, Georgetown University Medical Center, 3900 Reservoir Road, Washington, DC 20057, USA.

出版信息

Biochemistry. 2004 Jul 6;43(26):8290-6. doi: 10.1021/bi049137i.

Abstract

Recently, mutations in the novel polytopic integral membrane protein PfCRT were shown to cause chloroquine resistance (CQR) in the malarial parasite Plasmodium falciparum. PfCRT is not a member of the well-known family of ABC proteins that have previously been associated with other drug resistance phenomena. Thus, the mechanism(s) whereby mutant PfCRT molecules confer antimalarial drug resistance is (are) unknown. Previously, we succeeded in overexpressing PfCRT to high levels in Pichia pastoris yeast by synthesizing a codon-optimized version of the pfcrt gene. Using purified membranes and inside-out plasma membrane vesicles (ISOV) isolated from strains harboring either wild-type or CQR-associated mutant PfCRT, we now show that under deenergized conditions the PfCRT protein specifically binds the antimalarial drug chloroquine (CQ) with a K(D) near 400 nM but does not measurably bind the related drug quinine (QN) at physiologically relevant concentrations. Transport studies using ISOV show that QN is passively accumulated as expected on the basis of previous measurement of the ISOV DeltapH for the different strains. However, passive accumulation of CQ is lower than expected for ISOV harboring mutant PfCRT, despite higher DeltapH for these ISOV.

摘要

最近,新型多聚体整合膜蛋白PfCRT中的突变被证明会导致恶性疟原虫对氯喹产生耐药性(CQR)。PfCRT并非先前与其他耐药现象相关的著名ABC蛋白家族的成员。因此,突变型PfCRT分子赋予抗疟药物耐药性的机制尚不清楚。此前,我们通过合成密码子优化的pfcrt基因,成功在巴斯德毕赤酵母中高水平过表达PfCRT。利用从携带野生型或与CQR相关的突变型PfCRT的菌株中分离出的纯化膜和外翻质膜囊泡(ISOV),我们现在表明,在去能条件下,PfCRT蛋白以接近400 nM的解离常数(K(D))特异性结合抗疟药物氯喹(CQ),但在生理相关浓度下不会明显结合相关药物奎宁(QN)。使用ISOV进行的转运研究表明,根据先前对不同菌株ISOV的ΔpH测量结果,奎宁如预期那样被动积累。然而,尽管这些ISOV的ΔpH较高,但携带突变型PfCRT的ISOV中氯喹的被动积累低于预期。

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