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单羧酸根阴离子底物选择性和抑制剂敏感性在钠碘同向转运体(NIS)中的种间差异。

Inter-species variation in monovalent anion substrate selectivity and inhibitor sensitivity in the sodium iodide symporter (NIS).

机构信息

Department of Molecular Medicine, Mayo Clinic, Rochester, Minnesota, United States of America.

Mayo Clinic Graduate School of Biomedical Sciences, Mayo Clinic, Rochester, Minnesota, United States of America.

出版信息

PLoS One. 2020 Feb 21;15(2):e0229085. doi: 10.1371/journal.pone.0229085. eCollection 2020.

DOI:10.1371/journal.pone.0229085
PMID:32084174
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7034854/
Abstract

The sodium iodide symporter (NIS) transports iodide, which is necessary for thyroid hormone production. NIS also transports other monovalent anions such as tetrafluoroborate (BF4-), pertechnetate (TcO4-), and thiocyanate (SCN-), and is competitively inhibited by perchlorate (ClO4-). However, the mechanisms of substrate selectivity and inhibitor sensitivity are poorly understood. Here, a comparative approach was taken to determine whether naturally evolved NIS proteins exhibit variability in their substrate transport properties. The NIS proteins of thirteen animal species were initially assessed, and three species from environments with differing iodide availability, freshwater species Danio rerio (zebrafish), saltwater species Balaenoptera acutorostrata scammoni (minke whale), and non-aquatic mammalian species Homo sapiens (human) were studied in detail. NIS genes from each of these species were lentivirally transduced into HeLa cells, which were then characterized using radioisotope uptake assays, 125I- competitive substrate uptake assays, and kinetic assays. Homology models of human, minke whale and zebrafish NIS were used to evaluate sequence-dependent impact on the organization of Na+ and I- binding pockets. Whereas each of the three proteins that were analyzed in detail concentrated iodide to a similar degree, their sensitivity to perchlorate inhibition varied significantly: minke whale NIS was the least impacted by perchlorate inhibition (IC50 = 4.599 μM), zebrafish NIS was highly sensitive (IC50 = 0.081 μM), and human NIS showed intermediate sensitivity (IC50 = 1.566 μM). Further studies with fifteen additional substrates and inhibitors revealed similar patterns of iodide uptake inhibition, though the degree of 125I- uptake inhibition varied with each compound. Kinetic analysis revealed whale NIS had the lowest Km-I and the highest Vmax-I. Conversely, zebrafish NIS had the highest Km and lowest Vmax. Again, human NIS was intermediate. Molecular modeling revealed a high degree of conservation in the putative ion binding pockets of NIS proteins from different species, which suggests the residues responsible for the observed differences in substrate selectivity lie elsewhere in the protein. Ongoing studies are focusing on residues in the extracellular loops of NIS as determinants of anion specificity. These data demonstrate significant transport differences between the NIS proteins of different species, which may be influenced by the unique physiological needs of each organism. Our results also identify naturally-existing NIS proteins with significant variability in substrate transport kinetics and inhibitor sensitivity, which suggest that the affinity and selectivity of NIS for certain substrates can be altered for biotechnological and clinical applications. Further examination of interspecies differences may improve understanding of the substrate transport mechanism.

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f64c/7034854/b537571d58b6/pone.0229085.g008.jpg
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https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f64c/7034854/b537571d58b6/pone.0229085.g008.jpg
摘要

钠碘转运体 (NIS) 转运碘,这是甲状腺激素产生所必需的。NIS 还转运其他单价阴离子,如四氟化硼 (BF4-)、高锝酸盐 (TcO4-) 和硫氰酸盐 (SCN-),并被高氯酸盐 (ClO4-) 竞争性抑制。然而,底物选择性和抑制剂敏感性的机制还不太清楚。在这里,采用比较方法来确定天然进化的 NIS 蛋白是否在其底物转运特性上表现出可变性。最初评估了 13 种动物物种的 NIS 蛋白,并且来自碘可用性不同的环境的三种物种,淡水物种 Danio rerio(斑马鱼),盐水物种 Balaenoptera acutorostrata scammoni(小须鲸)和非水生哺乳动物物种 Homo sapiens(人类)进行了详细研究。来自这些物种的 NIS 基因通过慢病毒转导被转入 HeLa 细胞,然后使用放射性同位素摄取测定、125I-竞争性底物摄取测定和动力学测定进行表征。使用人、小须鲸和斑马鱼 NIS 的同源模型来评估序列依赖性对 Na+和 I-结合口袋组织的影响。尽管分析的三种蛋白质都将碘浓缩到相似的程度,但它们对高氯酸盐抑制的敏感性差异很大:小须鲸 NIS 受高氯酸盐抑制的影响最小(IC50=4.599 μM),斑马鱼 NIS 非常敏感(IC50=0.081 μM),而人 NIS 表现出中等敏感性(IC50=1.566 μM)。对另外 15 种底物和抑制剂的进一步研究揭示了类似的碘摄取抑制模式,尽管每种化合物的 125I-摄取抑制程度不同。动力学分析表明鲸 NIS 具有最低的 Km-I 和最高的 Vmax-I。相反,斑马鱼 NIS 具有最高的 Km 和最低的 Vmax。同样,人 NIS 处于中间位置。分子建模显示不同物种的 NIS 蛋白中存在高度保守的假定离子结合口袋,这表明导致观察到的底物选择性差异的残基位于蛋白质的其他部位。正在进行的研究集中在 NIS 的细胞外环中的残基上,作为阴离子特异性的决定因素。这些数据表明不同物种的 NIS 蛋白之间存在显著的转运差异,这可能受到每个生物体独特的生理需求的影响。我们的结果还表明,天然存在的 NIS 蛋白在底物转运动力学和抑制剂敏感性方面存在显著差异,这表明 NIS 对某些底物的亲和力和选择性可以改变,以用于生物技术和临床应用。进一步研究种间差异可能有助于更好地理解底物转运机制。

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