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华支睾吸虫多药耐药相关蛋白7的分子与结构特征

Molecular and structural characteristics of multidrug resistance-associated protein 7 in Chinese liver fluke Clonorchis sinensis.

作者信息

Dai Fuhong, Yoo Won Gi, Lee Ji-Yun, Lu Yanyan, Pak Jhang Ho, Sohn Woon-Mok, Hong Sung-Jong

机构信息

Department of Medical Environmental Biology, Chung-Ang University College of Medicine, Seoul, 06974, South Korea.

Department of Convergence Medicine University of Ulsan College of Medicine and Asan Institute for Life Sciences, Asan Medical Center, Seoul, 05505, South Korea.

出版信息

Parasitol Res. 2017 Mar;116(3):953-962. doi: 10.1007/s00436-016-5371-0. Epub 2017 Jan 5.

DOI:10.1007/s00436-016-5371-0
PMID:28058535
Abstract

Multidrug resistance-associated protein 7 (MRP7, ABCC10) is a C subfamily member of the ATP-binding cassette (ABC) superfamily. MRP7 is a lipophilic anion transporter that pumps endogenous and xenobiotic substrates from the cytoplasm to the extracellular milieu. Here, we cloned and characterized CsMRP7 as a novel ABC transporter from the Chinese liver fluke, Clonorchis sinensis. Full-length cDNA of CsMRP7 was 5174 nt, encoded 1636 amino acids (aa), and harbored a 147-bp 5'-untranslated region (5'-UTR) and 116-bp 3'-UTR. Phylogenetic analysis confirmed that CsMRP7 was closer to the ABCC subfamily than the ABCB subfamily. Tertiary structures of the N-terminal region (1-322 aa) and core region (323-1621 aa) of CsMRP7 were generated by homology modeling using glucagon receptor (PDB ID: 5ee7_A) and P-glycoprotein (PDB ID: 4f4c_A) as templates, respectively. CsMRP7 nucleotide-binding domain 2 (NBD2) was conserved more than NBD1, which was the sites of ATP binding and hydrolysis. Like typical long MRPs, CsMRP7 has an additional membrane-spanning domain 0 (MSD0) and cytoplasmic loop, along with a common structural fold consisting of MSD1-NBD1-MSD2-NBD2 as a single polypeptide assembly. MSD0, MSD1, and MSD2 consisted of TM1-7, TM8-13, and TM14-19, respectively. The CsMRP7 transcript was more abundant in the metacercariae than in the adult worms. Truncated NBD1 (39 kDa) and NBD2 (44 kDa) were produced in bacteria and mouse immune sera were raised. CsMRP7 was localized in the apical side of the intestinal epithelium, sperm in the testes and seminal receptacle, receptacle membrane, and mesenchymal tissue around intestine in the adult worm. These results provide molecular information and insights into structural and functional characteristics of CsMRP7 and homologs of flukes.

摘要

多药耐药相关蛋白7(MRP7,ABCC10)是ATP结合盒(ABC)超家族C亚家族成员。MRP7是一种亲脂性阴离子转运蛋白,可将内源性和外源性底物从细胞质泵送到细胞外环境。在此,我们克隆并鉴定了来自中华肝吸虫的新型ABC转运蛋白CsMRP7。CsMRP7的全长cDNA为5174 nt,编码1636个氨基酸(aa),并含有一个147 bp的5'非翻译区(5'-UTR)和116 bp的3'-UTR。系统发育分析证实,CsMRP7与ABCC亚家族的亲缘关系比ABCB亚家族更近。CsMRP7的N端区域(1-322 aa)和核心区域(323-1621 aa)的三级结构分别以胰高血糖素受体(PDB ID:5ee7_A)和P-糖蛋白(PDB ID:4f4c_A)为模板通过同源建模生成。CsMRP7核苷酸结合结构域2(NBD2)比NBD1保守性更强,NBD1是ATP结合和水解的位点。与典型的长MRP一样,CsMRP7具有一个额外的跨膜结构域0(MSD0)和细胞质环,以及由MSD1-NBD1-MSD2-NBD2组成的单一多肽组装体的常见结构折叠。MSD0、MSD1和MSD2分别由TM1-7、TM8-13和TM14-19组成。CsMRP7转录本在尾蚴中的丰度高于成虫。在细菌中产生了截短的NBD1(39 kDa)和NBD2(44 kDa),并制备了小鼠免疫血清。CsMRP7定位于成虫肠道上皮的顶端、睾丸和受精囊中的精子、受精囊膜以及肠道周围的间充质组织。这些结果为CsMRP7和吸虫同源物的结构和功能特征提供了分子信息和见解。

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