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  • 文献标题:   Graphene quantum dots in alveolar macrophage: uptake-exocytosis, accumulation in nuclei, nuclear responses and DNA cleavage
  • 文献类型:   Article
  • 作  者:   XU LN, DAI YH, WANG ZY, ZHAO J, LI F, WHITE JC, XING BS
  • 作者关键词:   aminated graphene quantum dot, macrophage, endocytosi, nuclear accumulation, dna cleavage, molecular docking
  • 出版物名称:   PARTICLE FIBRE TOXICOLOGY
  • ISSN:   1743-8977
  • 通讯作者地址:   Ocean Univ China
  • 被引频次:   4
  • DOI:   10.1186/s12989-018-0279-8
  • 出版年:   2018

▎ 摘  要

BackgroundGiven the tremendous potential for graphene quantum dots (QDs) in biomedical applications, a thorough understanding of the interaction of these materials with macrophages is essential because macrophages are one of the most important barriers against exogenous particles. Although the cytotoxicity and cellular uptake of graphene QDs were reported in previous studies, the interaction between nuclei and the internalized graphene QDs is not well understood. We thus systematically studied the nuclear uptake and related nuclear response associated with aminated graphene QDs (AG-QDs) exposure.ResultsAG-QDs showed modest 24-h inhibition to rat alveolar macrophages (NR8383), with a minimum inhibitory concentration (MIC) of 200g/mL. Early apoptosis was significantly increased by AG-QDs (100 and 200g/mL) exposure and played a major role in cell death. The internalization of AG-QDs was mainly via energy-dependent endocytosis, phagocytosis and caveolae-mediated endocytosis. After a 48-h clearance period, more than half of the internalized AG-QDs remained in the cellular cytoplasm and nucleus. Moreover, AG-QDs were effectively accumulated in nucleus and were likely regulated by two nuclear pore complexes genes (Kap2 and Nup98). AG-QDs were shown to alter the morphology, area, viability and nuclear components of exposed cells. Significant cleavage and cross-linking of DNA chains after AG-QDs exposure were confirmed by atomic force microscopy investigation. Molecular docking simulations showed that H-bonding and - stacking were the dominant forces mediating the interactions between AG-QDs and DNA, and were the important mechanisms resulting in DNA chain cleavage. In addition, the generation of reactive oxygen species (ROS) (e.g., center dot OH), and the up-regulation of caspase genes also contributed to DNA cleavage.ConclusionsAG-QDs were internalized by macrophages and accumulated in nuclei, which further resulted in nuclear damage and DNA cleavage. It is demonstrated that oxidative damage, direct contact via H-bonding and - stacking, and the up-regulation of caspase genes are the primary mechanisms for the observed DNA cleavage by AG-QDs.