Faculty of Health and Life Sciences, Northumbria University at Newcastle, Newcastle Upon Tyne, NE1 8ST, UK.
Inflammation. 2024 Feb;47(1):84-98. doi: 10.1007/s10753-023-01895-2. Epub 2023 Sep 1.
Inhibiting pathological secretion of Interleukin-1β has shown beneficial effects in disease models and in the clinic and thus there is interest in finding inhibitors that can reduce its release from macrophages in response to their activation by foreign pathogens. We used an in vitro human macrophage model to investigate whether ICRF-193, a Topoisomerase II inhibitor could modulate IL1B mRNA expression and IL-1β secretion. These macrophage-like cells readily secrete IL-1β in response to Lipopolysaccharide (LPS). Upon exposure to a non-toxic dose of ICRF-193, IL-1β secretion was diminished by ~ 40%; however, level of transcription of IL1B was unaffected. We show that there was no Topoisomerase 2B (TOP2B) binding to several IL1B gene sites, which may explain why ICRF-193 does not alter IL1B mRNA levels. Hence, we show for the first time that ICRF-193 can reduce IL-1β secretion. Its low cost and the development of water-soluble prodrugs of ICRF-193 warrants its further investigation in the modulation of pathological secretion of this cytokine for the treatment of inflammatory disorders. (165 words).
抑制白细胞介素-1β的病理性分泌已在疾病模型和临床中显示出有益的效果,因此人们有兴趣寻找能够减少其从巨噬细胞中释放的抑制剂,以响应外来病原体对其的激活。我们使用体外人巨噬细胞模型来研究拓扑异构酶 II 抑制剂 ICRF-193 是否可以调节 IL1B mRNA 表达和 IL-1β 分泌。这些类巨噬细胞在响应脂多糖 (LPS) 时很容易分泌 IL-1β。在接触到非毒性剂量的 ICRF-193 后,IL-1β 的分泌减少了约 40%;然而,IL1B 的转录水平不受影响。我们表明,没有拓扑异构酶 2B (TOP2B) 与几个 IL1B 基因位点结合,这可能解释了为什么 ICRF-193 不会改变 IL1B mRNA 水平。因此,我们首次表明 ICRF-193 可以减少 IL-1β 的分泌。它的低成本和水溶性前药的开发使得进一步研究其在调节这种细胞因子的病理性分泌以治疗炎症性疾病方面具有价值。(165 个单词)
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