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上转换纳米粒子(NaYF:Yb, Er)在斑马鱼早期生活阶段的体内毒性:发育毒性、肠道微生物组破坏和促炎作用。

In vivo toxicity of upconversion nanoparticles (NaYF:Yb, Er) in zebrafish during early life stages: Developmental toxicity, gut-microbiome disruption, and proinflammatory effects.

机构信息

School of Environmental and Chemical Engineering, Shanghai University, Shanghai 200444, China.

School of Environmental and Chemical Engineering, Shanghai University, Shanghai 200444, China.

出版信息

Ecotoxicol Environ Saf. 2024 Oct 1;284:116905. doi: 10.1016/j.ecoenv.2024.116905. Epub 2024 Aug 27.

Abstract

Lanthanide-doped upconversion nanoparticles (Ln-UCNPs) have been considered promising materials for various fields, such as biomedical and industrial applications. However, data and reports regarding its toxicity and environmental risks are scarce. Under these circumstances, data must be obtained to fully understand potential toxicity and adverse outcome pathways. In the present study, the toxicity of uncoated Ln-UCNP cores (NaYF:Yb, Er) was systematically assessed in zebrafish embryos during early developmental stages. Ln-UCNPs were found to have multiple toxic effects, such as effects on survival rates, delayed hatching times, shorter body lengths, altered heart rates and blood circulation (significantly reduced), and neurobehavioral impairments in response to photoperiod stimulation. Bioimaging showed that Ln-UCNPs were distributed on the chorion, eyes, and skin at 72 hpf. However, it accumulates in the pharynx, esophagus, and intestine after oral administration. Ln-UCNPs disrupt the diversity and abundance of host-associated microorganisms (gut microbiota) leading to an increase in the prevalence of harmful bacteria in zebrafish. Transcriptomic and Ingenuity Pathway Analysis (IPA) predicted Interleukin-8 (IL-8) signaling, neuroinflammation, cardiac hypertrophy signaling pathways, immune and inflammation-related response interferon-gamma (ifnγ), and miR-155 as key mediators in regulatory effects. Based on this, a causal network was built showing the strong links between the induced gene expression of differentially expressed genes (DEGs), such as nitric oxide synthase 2 (nos2) and tumor necrosis factor (tnf) upon Ln-UCNPs treatment, and with the downstream adverse outcomes, in particular, the promotion of apoptosis, liver damage, and inflammatory response. Finally, RT-qPCR analysis confirmed the up-regulated expression of nos2 and tnf in the exposed larvae, consistent with the observation of an increased number of fluorescence-labelled neutrophils and macrophages in lyz: DsRed transgenic zebrafish until 120 hpf exposure, which together demonstrated the proinflammatory effects of Ln-UCNPs on organisms. In conclusion, we illustrated the developmental toxicity, disruption of gut-microbiome, and proinflammatory effects of Ln-UCNP cores on zebrafish, and the causal network from IPA analysis may help further elucidate the adverse outcome pathway of Ln-UCNPs.

摘要

镧系掺杂上转换纳米粒子(Ln-UCNPs)在生物医学和工业应用等各个领域都被认为是很有前途的材料。然而,关于其毒性和环境风险的数据和报告却很少。在这种情况下,必须获取数据来充分了解潜在的毒性和不良后果途径。在本研究中,我们系统评估了未涂层的镧系掺杂上转换纳米粒子核心(NaYF:Yb,Er)在斑马鱼胚胎早期发育阶段的毒性。研究发现,Ln-UCNPs 具有多种毒性作用,例如对存活率、孵化时间延迟、体长缩短、心率和血液循环改变(显著降低)以及对光周期刺激的神经行为损伤。生物成像显示,72 hpf 时 Ln-UCNPs 分布在卵壳、眼睛和皮肤上。然而,口服给药后,它们会在咽部、食管和肠道中积累。Ln-UCNPs 破坏了宿主相关微生物(肠道微生物群)的多样性和丰度,导致斑马鱼中有害细菌的流行率增加。转录组学和 Ingenuity 通路分析(IPA)预测,白细胞介素 8(IL-8)信号、神经炎症、心脏肥大信号通路、免疫和炎症相关反应干扰素-γ(ifnγ)和 miR-155 作为关键调节因子。在此基础上,构建了一个因果网络,显示了差异表达基因(DEGs)诱导基因表达与下游不良结果之间的强联系,如一氧化氮合酶 2(nos2)和肿瘤坏死因子(tnf)在 Ln-UCNPs 处理后,特别是促进细胞凋亡、肝损伤和炎症反应。最后,RT-qPCR 分析证实了暴露幼虫中 nos2 和 tnf 的上调表达,与 lyz:DsRed 转基因斑马鱼中荧光标记的中性粒细胞和巨噬细胞数量增加的观察结果一致,直到 120 hpf 暴露,这共同证明了 Ln-UCNPs 对生物体的促炎作用。总之,我们说明了 Ln-UCNP 核心对斑马鱼的发育毒性、肠道微生物组的破坏和促炎作用,以及 IPA 分析的因果网络可能有助于进一步阐明 Ln-UCNPs 的不良后果途径。

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