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Heavy-metal modulation of the human intercellular adhesion molecule (ICAM-1) gene expression

机译:重金属对人类细胞间粘附分子(ICAM-1)基因表达的调节

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The intercellular adhesion molecule 1 (ICAM-1) can be induced on many different cell types by a set of various modulators (IL1β, TNF, LPS, IFN-γ), which are released during the inflammatory process. We have investigated the possibility that other factors, related to the stress and biophysical perturbations of the inflammatory response, may also modulate ICAM-1. Here, we report that heavy metals, in particular zinc, can enhance the expression of the ICAM-1 gene on cells actively involved at different levels during inflammation. Kinetic studies of ICAM-1 gene expression shows a maximum level of induction 4 h after treatment with metals, followed by a rapid decrease to basal levels within 12 h. The effect on enhanced gene expression is mostly due to a rapid increase of the transcriptional rate as shown by nuclear run-on experiments. In B lymphoblastoid cells, but not in fibroblasts, the increase in RNA expression seems significantly greater that the subsequent increase in protein expression, suggesting that a further point of post-transcriptional regulation of ICAM-1 occurs and may be linked to the cellular specificity.
机译:细胞间粘附分子1(ICAM-1)可以通过在炎症过程中释放的各种调节剂(IL1β,TNF,LPS,IFN-γ)在许多不同的细胞类型上诱导。我们调查了与压力和炎症反应的生物物理扰动有关的其他因素也可能调节ICAM-1的可能性。在这里,我们报道了重金属,特别是锌,可以增强炎症过程中活跃参与不同水平细胞上ICAM-1基因的表达。对ICAM-1基因表达的动力学研究表明,用金属处理后4 h诱导水平最高,随后在12 h内迅速降至基础水平。对基因表达增强的影响主要是由于核运行实验所显示的转录速率的快速增加。在B淋巴母细胞中,而不在成纤维细胞中,RNA表达的增加似乎明显大于随后的蛋白质表达的增加,这提示了ICAM-1的转录后调控的进一步发生,并且可能与细胞特异性有关。

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