Development of a live cell assay for the zinc transporter ZnT8

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS ACS Applied Bio Materials Pub Date : 2024-06-05 DOI:10.1016/j.slasd.2024.100166
Lucia Azzollini , Dolores Del Prete , Gernot Wolf , Christoph Klimek , Mattia Saggioro , Fernanda Ricci , Eirini Christodoulaki , Tabea Wiedmer , Alvaro Ingles-Prieto , Giulio Superti-Furga , Lia Scarabottolo
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Abstract

Zinc is an essential trace element that is involved in many biological processes and in cellular homeostasis. In pancreatic β-cells, zinc is crucial for the synthesis, processing, and secretion of insulin, which plays a key role in glucose homeostasis and which deficiency is the cause of diabetes. The accumulation of zinc in pancreatic cells is regulated by the solute carrier transporter SLC30A8 (or Zinc Transporter 8, ZnT8), which transports zinc from cytoplasm in intracellular vesicles. Allelic variants of SLC30A8 gene have been linked to diabetes. Given the physiological intracellular localization of SLC30A8 in pancreatic β-cells and the ubiquitous endogenous expression of other Zinc transporters in different cell lines that could be used as cellular model for SLC30A8 recombinant over-expression, it is challenging to develop a functional assay to measure SLC30A8 activity. To achieve this goal, we have firstly generated a HEK293 cell line stably overexpressing SLC30A8, where the over-expression favors the partial localization of SLC30A8 on the plasma membrane. Then, we used the combination of this cell model, commercial FluoZin-3 cell permeant zinc dye and live cell imaging approach to follow zinc flux across SLC30A8 over-expressed on plasma membrane, thus developing a novel functional imaging- based assay specific for SLC30A8. Our novel approach can be further explored and optimized, paving the way for future small molecule medium-throughput screening.

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开发锌转运体 ZnT8 的活细胞检测方法。
锌是一种重要的微量元素,参与许多生物过程和细胞平衡。在胰腺β细胞中,锌对胰岛素的合成、加工和分泌至关重要,而胰岛素在葡萄糖稳态中起着关键作用,缺锌会导致糖尿病。锌在胰腺细胞中的积累受溶质载体转运体 SLC30A8(或锌转运体 8,ZnT8)的调控,该转运体通过细胞内囊泡从细胞质中转运锌。SLC30A8 基因的等位基因变异与糖尿病有关。鉴于 SLC30A8 在胰腺 β 细胞中的生理胞内定位,以及其他锌转运体在不同细胞系中的普遍内源性表达,这些细胞系可用作 SLC30A8 重组过表达的细胞模型,因此开发一种功能测定法来测量 SLC30A8 的活性具有挑战性。为了实现这一目标,我们首先生成了稳定过表达 SLC30A8 的 HEK293 细胞系,过表达有利于 SLC30A8 在质膜上的部分定位。然后,我们利用这种细胞模型、商品化的 FluoZin-3 细胞渗透锌染料和活细胞成像方法,跟踪锌在过表达的 SLC30A8 质膜上的通量,从而开发出一种新型的基于功能成像的 SLC30A8 特异性检测方法。我们的新方法可以进一步探索和优化,为未来的小分子中通量筛选铺平道路。
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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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