首页> 美国卫生研究院文献>Dose-Response >Exposure to Low to Moderate Doses of Ionizing Radiation Induces A Reduction of Pro-Inflammatory Ly6chigh Monocytes and a U-Curved Response of T Cells in APOE -/- Mice
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Exposure to Low to Moderate Doses of Ionizing Radiation Induces A Reduction of Pro-Inflammatory Ly6chigh Monocytes and a U-Curved Response of T Cells in APOE -/- Mice

机译:暴露于低至中等剂量的电离辐射诱导促炎Ly6chigh单核细胞的减少和Apoe - / - 小鼠中T细胞的U形弯曲反应

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摘要

Low dose ionizing radiation (LDIR) is known to have a protective effect on atherosclerosis in rodent studies, but how it impacts different cells types involved in lesion formation remains incompletely understood. We investigated the immunomodulatory response of different doses and dose-rates of irradiation in ApoE-/- mice. Mice were exposed to external γ rays at very low (1.4 mGy.h-1) or low (50 mGy.h-1) dose-rates, with cumulative doses spanning 50 to 1000 mGy. Flow cytometry of circulating cells revealed a significant decrease in pro-inflammatory Ly6CHi monocytes at all cumulative doses at low dose-rate, but more disparate effects at very low dose-rate with reductions in Ly6CHi cells at doses of 50, 100 and 750 mGy only. In contrast, Ly6CLo monocytes were not affected by LDIR. Similarly, proportions of CD4+ T cell subsets in the spleen did not differ between irradiated mice and non-irradiated controls, whether assessing CD25+FoxP3+ regulatory or CD69+ activated lymphocytes. In the aorta, gene expression of cytokines such as IL-1 and TGF-ß and adhesion molecules such as E-Selectin, ICAM-1, and VCAM-1 were reduced at the intermediate dose of 200 mGy. These results suggest that LDIR may reduce atherosclerotic plaque formation by selectively reducing blood pro-inflammatory monocytes and by impairing adhesion molecule expression and inflammatory processes in the vessel wall. In contrast, splenic T lymphocytes were not affected by LDIR. Furthermore, some responses to irradiation were nonlinear; reductions in aortic gene expression were significant at intermediate doses, but not at either highest or lowest doses. This work furthers our understanding of the impact of LDIR with different dose-rates on immune system response in the context of atherosclerosis.
机译:已知低剂量电离辐射(LDIR)对啮齿动物研究中的动脉粥样硬化具有保护作用,但它如何影响病变形成中所涉及的不同细胞类型仍然不完全理解。我们研究了帕福/小鼠不同剂量和剂量辐射的免疫调节响应。将小鼠暴露于极低(1.4 mgy.h-1)或低(50 mgy.h-1)剂量 - 速率下暴露于外部γ射线,跨越50至1000 mgy的累积剂量。循环细胞的流式细胞术在低剂量速率下促使促炎Ly6CHI单核细胞的显着降低,但在50,100和750 MGY的剂量下,Ly6Chi细胞的降低更低的剂量效果更低。相比之下,Ly6Clo单核细胞不受LDIR的影响。类似地,脾脏中CD4 + T细胞亚群的比例在辐照小鼠和非照射对照之间没有区别,无论是评估CD25 + Foxp3 +调节剂还是CD69 +活化淋巴细胞。在主动脉中,在200 mgy的中间剂量下,减少了细胞因子的细胞因子的基因表达,例如IL-1和TGF-β和粘合分子,例如E-SELICEN,ICAM-1和VCAM-1。这些结果表明,通过选择性地减少血液促炎单核细胞并通过损害血管壁中的粘附分子表达和炎性过程,可以减少动脉粥样硬化斑块的形成。相比之下,脾脏T淋巴细胞不受LDIR的影响。此外,对照射的一些反应是非线性的;在中间剂量下,主动脉基因表达的减少,但不是最高或最低剂量。这项工作传统我们对动脉粥样硬化背景下的免疫系统反应不同剂量率的对LDIR的影响。

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