铅和镉对人滋养细胞线粒体功能和 NLRP3 炎症小体激活的不同影响

IF 4.7 2区医学 Q1 NEUROSCIENCES Journal of Physiology-London Pub Date : 2024-08-28 DOI:10.1113/JP286755

Yifeng Dai, Xijin Xu, Xia Huo, Joost H N Schuitemaker, Marijke M Faas

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引用次数: 0

摘要

重金属会破坏线粒体功能并激活含NOD样受体吡啉3（NLRP3）炎性体。我们研究了铅（Pb）/镉（Cd）在常氧、缺氧和促炎条件下对人滋养层细胞线粒体功能和 NLRP3 炎性体激活的影响。将 JEG-3、BeWo 和 HTR-8/SVneo 细胞暴露于铅或镉 24 小时，同时观察缺氧或促炎症脂多糖（LPS）或聚（I:C）是否存在。然后，我们评估了细胞的活力、凋亡、线粒体 DNA 拷贝数（mtDNAcn）、线粒体膜电位（ΔΨ）、NLRP3 炎症小体蛋白和白细胞介素（IL）-1β 的分泌。尽管我们的数据显示铅、镉、缺氧、多聚（I:C）和 LPS 会降低三种细胞系中的线粒体DNAcn，但这些处理对其他生物标志物的影响在不同细胞系中是不同的。我们发现，缺氧会降低JEG-3细胞的ΔΨ并促进其凋亡，增加BeWo细胞的ΔΨ并阻止其凋亡，而HTR-8/SVneo细胞的ΔΨ和凋亡没有变化。此外，缺氧条件下的铅可降低ΔΨ，促进BeWo细胞的凋亡。将 BeWo 和 HTR-8/SVneo 细胞单独暴露于缺氧、铅或镉条件下会上调 NLRP3 和原天冬酶 1 的表达，但不会激活 NLRP3 炎症体，因为裂解的天冬酶 1 和 IL-1β 没有增加。总之，铅和镉会影响滋养层细胞系的线粒体功能和 NLRP3 蛋白，但影响方式具有细胞系特异性。要点：这项工作的目的是了解铅（Pb）和镉（Cd）在常氧、缺氧和促炎条件下对人滋养层细胞系线粒体功能和 NLRP3 炎性体激活的影响。缺氧会增加 JEG-3 细胞的凋亡，而缺氧会减少 BeWo 细胞的凋亡，缺氧处理不会影响 HTR-8/SVneo 细胞的凋亡。在三种人类胎盘滋养层细胞系中，暴露于铅或镉会减少mtDNAcn。然而，缺氧条件下铅诱导ΔΨ下降并促进BeWo细胞凋亡，但镉在任何条件下都不会诱导三种滋养层细胞系的ΔΨ下降。暴露于缺氧、铅或镉会增加 BeWo 和 HTR-8/SVneo 细胞中的 NLRP3 和促天冬酶 1。我们的研究结果突出表明，铅和镉会影响滋养层细胞系的线粒体功能和NLRP3蛋白，但影响方式因细胞系而异。

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Differential effect of lead and cadmium on mitochondrial function and NLRP3 inflammasome activation in human trophoblast.

Heavy metals disrupt mitochondrial function and activate the NOD-like receptor pyrin-containing 3 (NLRP3) inflammasome. We investigated the effect of lead (Pb)/cadmium (Cd) on mitochondrial function and NLRP3 inflammasome activation in human trophoblast under normoxic, hypoxic and pro-inflammatory conditions. JEG-3, BeWo and HTR-8/SVneo cells were exposed to Pb or Cd for 24 h in the absence or presence of hypoxia or pro-inflammatory lipopolysaccharide (LPS) or poly(I:C). Then, we evaluated cell viability, apoptosis, mitochondrial DNA copy number (mtDNAcn), mitochondrial membrane potential (ΔΨ), NLRP3 inflammasome proteins and interleukin (IL)-1β secretion. Although our data showed that Pb, Cd, hypoxia, poly(I:C) and LPS decreased mtDNAcn in the three cell lines, the effects of these treatments on other biomarkers were different in the different cell lines. We found that hypoxia decreased ΔΨ and promoted apoptosis in JEG-3 cells, increased ΔΨ and prevented apoptosis in BeWo cells, and did not change ΔΨ and apoptosis in HTR-8/SVneo cells. Moreover, Pb under hypoxic conditions reduced ΔΨ and promoted apoptosis of BeWo cells. Exposure of BeWo and HTR-8/SVneo cells to hypoxia, Pb or Cd alone upregulated the expression of NLRP3 and pro-caspase 1 but did not activate the NLRP3 inflammasome since cleaved-caspase 1 and IL-1β were not increased. To conclude, Pb and Cd affected trophoblast mitochondrial function and NLRP3 proteins in trophoblast cell lines, but in a cell line-specific way. KEY POINTS: The objective of this work was an understanding of the effect of lead (Pb) and cadmium (Cd) on mitochondrial function and NLRP3 inflammasome activation in human trophoblast cell lines under normoxic, hypoxic and pro-inflammatory conditions. Apoptosis of JEG-3 cells was increased by hypoxia, while in BeWo cells, apoptosis was decreased by hypoxia, and in HTR-8/SVneo, apoptosis was not affected by hypoxic treatment. Exposure to either Pb or Cd decreased mtDNAcn in three human placental trophoblast cell lines. However, Pb under hypoxia induced a decrease of ΔΨ and promoted apoptosis of BeWo cells, but Cd did not induce a reduction in ΔΨ in the three trophoblast cell lines under any conditions. Exposure to hypoxia, Pb or Cd increased NLRP3 and pro-caspase 1 in BeWo and HTR-8/SVneo cells. Our findings highlight that Pb and Cd affected trophoblast mitochondrial function and NLRP3 proteins in trophoblast cell lines but in a cell line-specific way.

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来源期刊

Journal of Physiology-London 医学-神经科学

CiteScore

9.70

自引率

7.30%

发文量

817

审稿时长

2 months

期刊介绍： The Journal of Physiology publishes full-length original Research Papers and Techniques for Physiology, which are short papers aimed at disseminating new techniques for physiological research. Articles solicited by the Editorial Board include Perspectives, Symposium Reports and Topical Reviews, which highlight areas of special physiological interest. CrossTalk articles are short editorial-style invited articles framing a debate between experts in the field on controversial topics. Letters to the Editor and Journal Club articles are also published. All categories of papers are subjected to peer reivew. The Journal of Physiology welcomes submitted research papers in all areas of physiology. Authors should present original work that illustrates new physiological principles or mechanisms. Papers on work at the molecular level, at the level of the cell membrane, single cells, tissues or organs and on systems physiology are all acceptable. Theoretical papers and papers that use computational models to further our understanding of physiological processes will be considered if based on experimentally derived data and if the hypothesis advanced is directly amenable to experimental testing. While emphasis is on human and mammalian physiology, work on lower vertebrate or invertebrate preparations may be suitable if it furthers the understanding of the functioning of other organisms including mammals.