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SLC10 家族转运体对甲状腺激素转运的研究。

Study of the transport of thyroid hormone by transporters of the SLC10 family.

机构信息

Department of Internal Medicine, Erasmus University Medical Center, Dr Molewaterplein 50, 3015 GE Rotterdam, The Netherlands.

出版信息

Mol Cell Endocrinol. 2010 Feb 5;315(1-2):138-45. doi: 10.1016/j.mce.2009.08.003. Epub 2009 Aug 12.

Abstract

Transport of (sulfated) iodothyronines across the plasma membrane is required for their intracellular metabolism. Rat Na(+)/taurocholate cotransporting polypeptide (Ntcp; Slc10a1) has been identified as an important transporter protein. We demonstrate that among the 7 members of the solute carrier family SLC10, only human SLC10A1 mediates sodium-dependent transport of the iodothyronine T4 and iodothyronine sulfates T3S and T4S. In contrast to SLC10A2-7, cells co-expressing SLC10A1 and the deiodinase D1 demonstrate a dramatic increase in T3S and T4S metabolism. The SLC10A1 substrates taurocholate, DHEAS and E3S inhibit T3S and T4S transport. Furthermore, co-transfection of SLC10A1 with CRYM, a well-known intracellular iodothyronine-binding protein, results in an enhanced intracellular accumulation of T3S and T4S, indicating that CRYM binds iodothyronine sulfates. The present findings indicate that the liver-specific transporter SLC10A1 transports (sulfated) iodothyronines, thereby increasing their intracellular availability. Therefore, SLC10A1 may fulfill a critical step in providing liver D1 with iodothyronine sulfates for rapid degradation.

摘要

(硫酸化)甲状腺素穿过质膜的转运对于其细胞内代谢是必需的。大鼠 Na(+)/牛磺胆酸钠共转运蛋白(Ntcp;Slc10a1)已被鉴定为一种重要的转运蛋白。我们证明,在溶质载体家族 SLC10 的 7 个成员中,只有人 SLC10A1 介导甲状腺素 T4 和甲状腺素硫酸盐 T3S 和 T4S 的钠依赖性转运。与 SLC10A2-7 不同,共表达 SLC10A1 和脱碘酶 D1 的细胞显示 T3S 和 T4S 代谢的显著增加。SLC10A1 的底物牛磺胆酸钠、DHEAS 和 E3S 抑制 T3S 和 T4S 转运。此外,SLC10A1 与 CRYM(一种已知的细胞内甲状腺素结合蛋白)共转染导致 T3S 和 T4S 的细胞内积累增加,表明 CRYM 结合甲状腺素硫酸盐。本研究结果表明,肝脏特异性转运蛋白 SLC10A1 转运(硫酸化)甲状腺素,从而增加其细胞内可用性。因此,SLC10A1 可能在为肝脏 D1 提供甲状腺素硫酸盐以供快速降解方面发挥关键作用。

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