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高糖环境中胰岛素或白细胞介素-6存在下培养的 C2C12 细胞中锌转运体表达的锌调节作用。

Modulation of Zinc Transporter Expressions by Additional Zinc in C2C12 Cells Cultured in a High Glucose Environment and in the Presence of Insulin or Interleukin-6.

机构信息

Department of Nutrition, Faculty of Medicine, University of Chile, Avenida Independencia 1027, Independencia, Santiago, Chile.

Micronutrient Laboratory, Institute of Nutrition and Food Technology, University of Chile, Macul 5540, Macul, Santiago, Chile.

出版信息

Biol Trace Elem Res. 2023 Jul;201(7):3428-3437. doi: 10.1007/s12011-022-03443-9. Epub 2022 Oct 13.

DOI:10.1007/s12011-022-03443-9
PMID:36227447
Abstract

Zn status has been related to various chronic diseases presenting oxidative stress and inflammation, such as type 2 diabetes. Zn supplementation has been suggested to be a potential coadjuvant in the management of this condition. Zn transporters constitute a key component in the maintenance of Zn homeostasis. Our aim was to evaluate the modulatory effect of additional Zn (10 or 100 µM; as a ZnSO*7H0) on the mRNA relative expression of selected Zn transporters (ZnT1, ZnT5, ZnT7, ZIP6, ZIP7, ZIP10, ZIP14), in myoblast (C2C12) cells cultured in normal (10 mM) and high glucose (30 mM), and in the absence or presence of insulin (1 nM), and interleukin-6 (IL-6; 5 nM) for 24 h. The main findings of our study were that in high glucose conditions in absence of insulin or IL-6, additional Zn increased ZnT1 and ZIP6, and decreased ZnT5 and ZIP7 expressions. However, this situation is modified by insulin, where incremental Zn induced increased expressions of ZnT1, ZnT5, and all the ZIP transporters studied. In high glucose conditions and in the presence of IL-6, additional Zn caused increased expressions of ZnT7, ZIP7, and ZIP14, compared with results in the absence of IL-6. This study provides preliminary evidence for the differential expression of selected Zn transporters in C2C12 cells subjected to high glucose and incremental Zn, suggesting that important changes in intracellular Zn distribution take place in response to inflammatory and high-insulin environments. Further study is necessary to understand the implications of these findings.

摘要

锌的状态与各种表现出氧化应激和炎症的慢性疾病有关,如 2 型糖尿病。有人建议补充锌作为这种情况的潜在辅助治疗。锌转运蛋白是维持锌体内平衡的关键组成部分。我们的目的是评估额外的锌(10 或 100 μM;作为 ZnSO*7H0)对选定的锌转运体(ZnT1、ZnT5、ZnT7、ZIP6、ZIP7、ZIP10、ZIP14)的 mRNA 相对表达的调节作用,在正常(10 mM)和高葡萄糖(30 mM)培养的肌母细胞(C2C12)中,以及在没有或存在胰岛素(1 nM)和白细胞介素-6(IL-6;5 nM)的情况下培养 24 小时。我们研究的主要发现是,在没有胰岛素或 IL-6 的高葡萄糖条件下,额外的锌增加了 ZnT1 和 ZIP6 的表达,降低了 ZnT5 和 ZIP7 的表达。然而,这种情况被胰岛素所改变,其中增量锌诱导了 ZnT1、ZnT5 和所有研究的 ZIP 转运体的表达增加。在高葡萄糖条件下和存在 IL-6 的情况下,与不存在 IL-6 的情况相比,额外的锌导致 ZnT7、ZIP7 和 ZIP14 的表达增加。本研究为 C2C12 细胞在高葡萄糖和增量锌作用下选择的锌转运体的差异表达提供了初步证据,表明在炎症和高胰岛素环境下,细胞内锌分布发生了重要变化。需要进一步研究以了解这些发现的意义。

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本文引用的文献

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Adv Nutr. 2021 Feb 1;12(1):141-160. doi: 10.1093/advances/nmaa087.
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The zinc transporter Zip14 (SLC39a14) affects Beta-cell Function: Proteomics, Gene expression, and Insulin secretion studies in INS-1E cells.锌转运蛋白 Zip14(SLC39a14)影响β细胞功能:INS-1E 细胞的蛋白质组学、基因表达和胰岛素分泌研究。
Sci Rep. 2019 Jun 13;9(1):8589. doi: 10.1038/s41598-019-44954-1.
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Zinc supplementation improves glycemic control for diabetes prevention and management: a systematic review and meta-analysis of randomized controlled trials.
锌补充剂可改善血糖控制,有助于预防和治疗糖尿病:一项随机对照试验的系统评价和荟萃分析。
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Zinc Transporter Proteins.锌转运蛋白。
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Hepatic ZIP14-mediated Zinc Transport Contributes to Endosomal Insulin Receptor Trafficking and Glucose Metabolism.肝脏中ZIP14介导的锌转运有助于内体胰岛素受体运输和葡萄糖代谢。
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