通过小胶质细胞中线粒体氧化应激诱导石墨烯量子点引发的铁死亡。

Induction of ferroptosis in response to graphene quantum dots through mitochondrial oxidative stress in microglia.

机构信息

Key Laboratory of Environmental Medicine and Engineering, Ministry of Education; School of Public Health, Southeast University, Nanjing, 210009, P. R. China.

School of Medicine, Southeast University, Nanjing, 210009, P. R. China.

出版信息

Part Fibre Toxicol. 2020 Jul 11;17(1):30. doi: 10.1186/s12989-020-00363-1.

DOI:10.1186/s12989-020-00363-1

PMID:32652997

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7353734/

Abstract

BACKGROUND

Graphene quantum dots (GQDs) provide a bright prospect in the biomedical application because they contain low-toxic compounds and promise imaging of deep tissues and tiny vascular structures. However, the biosafety of this novel QDs has not been thoroughly evaluated, especially in the central nervous system (CNS). The microarray analysis provides a hint that nitrogen-doped GQDs (N-GQDs) exposure could cause ferroptosis in microglia, which is a novel form of cell death dependent on iron overload and lipid peroxidation.

RESULTS

The cytosolic iron overload, glutathione (GSH) depletion, excessive reactive oxygen species (ROS) production and lipid peroxidation (LPO) were observed in microglial BV2 cells treated with N-GQDs, which indicated that N-GQDs could damage the iron metabolism and redox balance in microglia. The pre-treatments of a specific ferroptosis inhibitor Ferrostatin-1 (Fer-1) and an iron chelater Deferoxamine mesylate (DFO) not only inhibited cell death, but also alleviated iron overload, LPO and alternations in ferroptosis biomarkers in microglia, which were caused by N-GQDs. When assessing the potential mechanisms of N-GQDs causing ferroptosis in microglia, we found that the iron content, ROS generation and LPO level in mitochondria of BV2 cells all enhanced after N-GQDs exposure. When the antioxidant ability of mitochondria was increased by the pre-treatment of a mitochondria targeted ROS scavenger MitoTEMPO, the ferroptotic biological changes were effectively reversed in BV2 cells treated with N-GQDs, which indicated that the N-GQDs-induced ferroptosis in microglia could be attributed to the mitochondrial oxidative stress. Additionally, amino functionalized GQDs (A-GQDs) elicited milder redox imbalance in mitochondria and resulted in less ferroptotic effects than N-GQDs in microglia, which suggested a slight protection of amino group functionalization in GQDs causing ferroptosis.

CONCLUSION

N-GQDs exposure caused ferroptosis in microglia via inducing mitochondrial oxidative stress, and the ferroptotic effects induced by A-GQDs were milder than N-GQDs when the exposure method is same. This study will not only provide new insights in the GQDs-induced cell damage performed in multiple types of cell death, but also in the influence of chemical modification on the toxicity of GQDs.

摘要

背景

石墨烯量子点（GQDs）由于含有低毒化合物，有望用于生物医学成像，可对深部组织和微小血管结构进行成像，因此在生物医学领域具有广阔的应用前景。然而，这种新型量子点的生物安全性尚未得到充分评估，尤其是在中枢神经系统（CNS）中。微阵列分析提示，氮掺杂石墨烯量子点（N-GQDs）暴露可能导致小胶质细胞发生铁死亡，这是一种依赖于铁过载和脂质过氧化的新型细胞死亡形式。

结果

N-GQDs 处理的小胶质细胞 BV2 中观察到细胞质铁过载、谷胱甘肽（GSH）耗竭、活性氧（ROS）过度产生和脂质过氧化（LPO），表明 N-GQDs 可破坏小胶质细胞中的铁代谢和氧化还原平衡。特定铁死亡抑制剂 Ferrostatin-1（Fer-1）和铁螯合剂甲磺酸去铁胺（DFO）预处理不仅抑制细胞死亡，还可抑制 N-GQDs 引起的小胶质细胞中铁过载、LPO 和铁死亡生物标志物的改变。在评估 N-GQDs 引起小胶质细胞铁死亡的潜在机制时，我们发现 N-GQDs 暴露后 BV2 细胞线粒体中的铁含量、ROS 生成和 LPO 水平均增强。当用线粒体靶向 ROS 清除剂 MitoTEMPO 预处理来增加线粒体的抗氧化能力时，N-GQDs 处理的 BV2 细胞中的铁死亡生物变化得到有效逆转，表明 N-GQDs 诱导的小胶质细胞铁死亡可归因于线粒体氧化应激。此外，与 N-GQDs 相比，氨基功能化 GQDs（A-GQDs）在小胶质细胞中引起的线粒体氧化还原失衡较轻，导致铁死亡的作用较弱，这表明 GQDs 中氨基官能团化在引起铁死亡方面具有轻微的保护作用。