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表达和分析两种新型大鼠有机阳离子转运体同源物 SLC22A17 和 SLC22A23。

Expression and analysis of two novel rat organic cation transporter homologs, SLC22A17 and SLC22A23.

机构信息

Department of Biomedical Sciences, Texas Tech University Health Sciences Center, School of Pharmacy, Amarillo, TX 79106, USA.

出版信息

Mol Cell Biochem. 2011 Jun;352(1-2):143-54. doi: 10.1007/s11010-011-0748-y. Epub 2011 Feb 27.

Abstract

The organic cation transporter (OCT, SLC22) family is a family of polyspecific transmembrane proteins that are responsible for the uptake or excretion of many cationic drugs, toxins, and endogenous metabolites in a variety of tissues. Many of the OCTs have been previously characterized, but there are a number of orphan genes whose functions remain unknown. In this study, two novel rat SLC22 genes, SLC22A17 (BOCT1) and SLC22A23 (BOCT2), were cloned and characterized. Northern blot analysis showed that BOCT1 and BOCT2 mRNA was expressed in a wide variety of tissues. BOCT1 was strongly expressed in brain, primary neurons and brain endothelial cells, with highest expression in choroid plexus. BOCT2 was also abundantly expressed in brain, as well as in liver. To characterize the products of these genes, BOCT1 cDNA was isolated from a rat blood-brain barrier cDNA library, and BOCT2 cDNA was isolated from rat brain capillary and from cultured neurons using PCR techniques. Plasmids expressing BOCT1 and BOCT2 were transfected into HEK-293 cells, as were control cDNAs for OCT1 and OCTN2. Recombinant cell surface protein was verified by western blot and fluorescence microscopy. Transport activity of BOCT1 and BOCT2 was evaluated using radioisotope uptake assays. The OCT1- and OCTN2-expressing cells transported the canonical substrates, 1-methyl-4-phenyl-pyridinium (MPP(+)) and carnitine, respectively. However, BOCT1 and BOCT2-expressing cells did not show transport activity for these substrates or a number of other SLC22 substrates. These novel family members have a nonconserved amino terminus, relative to other OCTs, that may preclude typical SLC22 transport function.

摘要

有机阳离子转运体(OCT,SLC22)家族是一组多特异性跨膜蛋白,负责在多种组织中摄取或排泄许多阳离子药物、毒素和内源性代谢物。许多 OCT 已经被先前表征,但有许多孤儿基因的功能仍然未知。在这项研究中,克隆并表征了两种新的大鼠 SLC22 基因,SLC22A17(BOCT1)和 SLC22A23(BOCT2)。Northern blot 分析显示,BOCT1 和 BOCT2 mRNA 在广泛的组织中表达。BOCT1 在脑、原代神经元和脑内皮细胞中强烈表达,在脉络丛中表达最高。BOCT2 也在脑中以及肝脏中大量表达。为了表征这些基因的产物,从大鼠血脑屏障 cDNA 文库中分离出 BOCT1 cDNA,从大鼠脑毛细血管和培养的神经元中使用 PCR 技术分离出 BOCT2 cDNA。将表达 BOCT1 和 BOCT2 的质粒转染到 HEK-293 细胞中,同时转染 OCT1 和 OCTN2 的对照 cDNA。通过 Western blot 和荧光显微镜验证重组细胞表面蛋白。使用放射性同位素摄取测定评估 BOCT1 和 BOCT2 的转运活性。表达 OCT1 和 OCTN2 的细胞分别转运典型底物 1-甲基-4-苯基吡啶(MPP(+))和肉碱。然而,BOCT1 和 BOCT2 表达的细胞没有显示对这些底物或许多其他 SLC22 底物的转运活性。这些新的家族成员具有相对于其他 OCT 的非保守氨基末端,这可能排除了典型的 SLC22 转运功能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b437/3097276/9ead712f5735/nihms291260f1.jpg

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