| Literature DB >> 32992116 |
Jianxiong Xu1, Jinxuan Wang1, Juhui Qiu2, Hua Liu3, Yi Wang1, Yuliang Cui1, Rose Humphry4, Nan Wang4, Colm DurKan4, Yaokai Chen5, Yanqiu Lu5, Qinfeng Ma1, Wei Wu1, Yang Luo1, Lehui Xiao6, Guixue Wang7.
Abstract
The large-scale utilization of nanotechnology depends on public and consumer confidence in the safety of this new technology. Studying the interaction of nanoparticles with immune cells plays a vital role in the safety assessment of nanomedicine. Although some researches have indicated that the immune cells undergo severe interfere after phagocytosis of nanoparticles, the impact on immune system of the whole body are still unclear. Here, we use immune cells labeled transgenic zebrafish to study the mechanisms of nanoparticles on zebrafish immune cells. We demonstrate that gold nanoparticles (Au NPs) phagocytized by immune cells can reduce and retard the sensitivity of immune response, resulting nanoparticle-induced bluntness in immune cell (NIBIC). RNA-seq and functional analysis reveal that NIBIC is mainly induced by the inhibiting expression of chemokine receptor 5 (CCR5). Furthermore, PVP-modified Au NPs can eliminate NIBIC by inhibiting the cell phagocytosis. Our results highlight the potential risk for Au NPs in vivo and further the understanding of the mechanism of the interaction between Au NPs and the immune response. We should consider this factor in future material design and pay more attention to the process of using nanomedicines on immune diseases.Entities:
Keywords: Chemokine receptor; Immune cells; Nanoparticle-induced bluntness in immune cell (NIBIC); Nanoparticles; Trans-endothalial migration
Year: 2020 PMID: 32992116 DOI: 10.1016/j.biomaterials.2020.120392
Source DB: PubMed Journal: Biomaterials ISSN: 0142-9612 Impact factor: 12.479