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Zn 转运蛋白 ZnT10 的外排功能、组织特异性表达和细胞内运输表明其在成人 Zn 稳态中的作用。

Efflux function, tissue-specific expression and intracellular trafficking of the Zn transporter ZnT10 indicate roles in adult Zn homeostasis.

机构信息

Human Nutrition Research Centre, Newcastle University, Newcastle upon Tyne, NE2 4BW, UK.

出版信息

Metallomics. 2012 Aug;4(8):771-9. doi: 10.1039/c2mt20088k. Epub 2012 Jun 18.

DOI:10.1039/c2mt20088k
PMID:22706290
Abstract

Zn is essential to the structure and function of numerous proteins and enzymes so requires tight homeostatic control at both the systemic and cellular level. Two families of Zn transporters - ZIP (SLC39) and ZnT (SLC30) - contribute to Zn homeostasis. There are at least 10 members of the human ZnT family, and the expression profile and regulation of each varies depending on tissue type. Little is known about the role and expression pattern of ZnT10; however in silico data predict restricted expression to foetal tissue. We show a differential expression profile for ZnT10 in adult human tissue by RT-qPCR and detect highest levels of expression in small intestine, liver and brain tissues. We present data revealing the functional activity of ZnT10 to be in the efflux direction. Using a plasmid construct to express ZnT10 with an N-terminal FLAG-epitope tag, we reveal subcellular localisation in a neuroblastoma cell line (SH-SY5Y) to be at the Golgi apparatus under standard conditions of culture, with trafficking to the plasma membrane observed at higher extracellular Zn concentrations. We demonstrate down-regulation by Zn of ZnT10 mRNA levels in cultured intestinal and neuroblastoma cell lines and demonstrate reduced transcription from the ZnT10 promoter at an elevated extracellular Zn concentration. These features of ZnT10 localisation, regulation and function, together with the discovery that ZnT10 is expressed a high levels in brain tissue, indicate that ZnT10 has a role in regulating Zn homeostasis in the brain so may have relevance to the development of neurodegenerative disease.

摘要

锌对于许多蛋白质和酶的结构和功能至关重要,因此需要在全身和细胞水平上进行严格的动态平衡控制。两种锌转运体家族 - ZIP(SLC39)和 ZnT(SLC30) - 有助于维持锌的动态平衡。人类 ZnT 家族至少有 10 个成员,每个成员的表达谱和调节都取决于组织类型。关于 ZnT10 的作用和表达模式知之甚少;然而,计算机数据预测其表达仅限于胎儿组织。我们通过 RT-qPCR 显示了 ZnT10 在成人组织中的差异表达谱,并在小肠、肝脏和脑组织中检测到最高水平的表达。我们提供的数据揭示了 ZnT10 的功能活性是在流出方向。使用表达带有 N 端 FLAG 表位标签的 ZnT10 的质粒构建体,我们在神经母细胞瘤细胞系(SH-SY5Y)中揭示了亚细胞定位在高尔基体,在标准培养条件下,在较高的细胞外锌浓度下观察到向质膜的运输。我们证明 Zn 在培养的肠和神经母细胞瘤细胞系中下调 ZnT10 mRNA 水平,并证明在升高的细胞外 Zn 浓度下 ZnT10 启动子的转录减少。ZnT10 的这些定位、调节和功能特征,以及发现 ZnT10 在脑组织中高表达,表明 ZnT10 在调节大脑中的锌动态平衡中发挥作用,因此可能与神经退行性疾病的发展有关。

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