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人单羧酸转运蛋白10对甲状腺激素的有效细胞摄取和外排

Effective cellular uptake and efflux of thyroid hormone by human monocarboxylate transporter 10.

作者信息

Friesema Edith C H, Jansen Jurgen, Jachtenberg Jan-Willem, Visser W Edward, Kester Monique H A, Visser Theo J

机构信息

Department of Internal Medicine, Erasmus University Medical Center, 3015 GE Rotterdam, The Netherlands.

出版信息

Mol Endocrinol. 2008 Jun;22(6):1357-69. doi: 10.1210/me.2007-0112. Epub 2008 Mar 12.

Abstract

Cellular entry of thyroid hormone is mediated by plasma membrane transporters, among others a T-type (aromatic) amino acid transporter. Monocarboxylate transporter 10 (MCT10) has been reported to transport aromatic amino acids but not iodothyronines. Within the MCT family, MCT10 is most homologous to MCT8, which is a very important iodothyronine transporter but does not transport amino acids. In view of this paradox, we decided to reinvestigate the possible transport of thyroid hormone by human (h) MCT10 in comparison with hMCT8. Transfection of COS1 cells with hMCT10 cDNA resulted in 1) the production of an approximately 55 kDa protein located to the plasma membrane as shown by immunoblotting and confocal microscopy, 2) a strong increase in the affinity labeling of intracellular type I deiodinase by N-bromoacetyl-[(125)I]T(3), 3) a marked stimulation of cellular T(4) and, particularly, T(3) uptake, 4) a significant inhibition of T(3) uptake by phenylalanine, tyrosine, and tryptophan of 12.5%, 22.2%, and 51.4%, respectively, and 5) a marked increase in the intracellular deiodination of T(4) and T(3) by different deiodinases. Cotransfection studies using the cytosolic thyroid hormone-binding protein micro-crystallin (CRYM) indicated that hMCT10 facilitates both cellular uptake and efflux of T(4) and T(3). In the absence of CRYM, hMCT10 and hMCT8 increased T(3) uptake after 5 min incubation up to 4.0- and 1.9-fold, and in the presence of CRYM up to 6.9- and 5.8-fold, respectively. hMCT10 was less active toward T(4) than hMCT8. These findings establish that hMCT10 is at least as active a thyroid hormone transporter as hMCT8, and that both transporters facilitate iodothyronine uptake as well as efflux.

摘要

甲状腺激素的细胞摄取由质膜转运蛋白介导,其中包括一种T型(芳香族)氨基酸转运蛋白。据报道,单羧酸转运蛋白10(MCT10)可转运芳香族氨基酸,但不能转运碘甲状腺原氨酸。在MCT家族中,MCT10与MCT8的同源性最高,MCT8是一种非常重要的碘甲状腺原氨酸转运蛋白,但不能转运氨基酸。鉴于这种矛盾情况,我们决定重新研究人(h)MCT10与hMCT8相比,是否可能转运甲状腺激素。用hMCT10 cDNA转染COS1细胞导致:1)免疫印迹和共聚焦显微镜显示产生了一种位于质膜的约55 kDa蛋白质;2)N-溴乙酰基-[(125)I]T3对细胞内I型脱碘酶的亲和标记显著增加;3)细胞对T4,特别是T3的摄取明显受到刺激;4)苯丙氨酸、酪氨酸和色氨酸对T3摄取的显著抑制分别为12.5%、22.2%和51.4%;5)不同脱碘酶对T4和T3的细胞内脱碘作用显著增强。使用胞质甲状腺激素结合蛋白微晶蛋白(CRYM)的共转染研究表明,hMCT10促进T4和T3的细胞摄取和流出。在没有CRYM的情况下,孵育5分钟后,hMCT10和hMCT8使T3摄取分别增加至4.0倍和1.9倍,在有CRYM的情况下分别增加至6.9倍和5.8倍。hMCT10对T4的活性低于hMCT8。这些发现表明,hMCT10作为甲状腺激素转运蛋白的活性至少与hMCT8一样高,并且这两种转运蛋白都促进碘甲状腺原氨酸的摄取和流出。

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