Limited mutagenesis of myelokaryocytes following acute external irradiation as a protective mechanism of miliacin in radiation-induced immunosuppression

Y.A. Sarycheva, A. A. Tokareva, A. G. Shechtman, T. Panfilova, Yu. S. Pimenova, R. Mitrofanov, B. Frolov
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Abstract

Antimutagenic effect of the plant triterpenoid miliacin was studied, in order to characterize its protective properties in a model of acute irradiation immunosuppression using outbred male mice. Ionizing irradiation at different doses (0.5; 1.0; 2.0; 4.0 Gy) was used for experimental (miliacin-treated), and control animals that received the miliacin solvent. Miliacin was administered three times intraperitoneally at a single dose of 4.0 mg/kg with 24-hour intervals between injections. The last dose was applied 1 day before irradiation. Myelokaryocytes served as test objects, the analysis of which was carried out 24 hours after irradiation. Miliacin had a certain protective effect by limiting the post-radiation myeloablation, reducing the number of aberrant cells and the total number of aberrations. Protective effect of triterpenoids showed inverse relation to the radiation dose, being most pronounced at the dose of 0.5 Gy. Higher values of chromatid aberrations at radiation doses of 1.0 and 2.0 Gy in animals from the experimental group versus control mice, probably, due to anti-apoptotic effect of the triterpenoid, thus ensuring higher survival rates of mutated cells with severe damage to their genome. The protective effect of miliacin at 24 hours after radiation exposure may indicate its effect on the primary radiochemical stage of radiation injury. It is suggested that the mechanism of protective action of triterpenoid is mediated by its previously shown antioxidant activity, due to its ability to stabilize membranes and normalize expression of genes encoding antioxidant protection enzymes. Thus, the antimutagenic activity of miliacin after irradiation is an important characteristic of its immunoprotective effect during the radiation-induced immunosuppression. With respect to its ability to limit the mutagenic effect, miliacin may be classified as a weak radioprotective antimutagen with a protection efficiency of 20-40% at the dose range of 0.5 to 1.0 Gray.
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急性外照射后髓核细胞的有限突变作为毫米霉素在辐射诱导免疫抑制中的保护机制
研究了植物三萜霉素的抗诱变作用,以鉴定其在远交系雄性小鼠急性辐照免疫抑制模型中的保护作用。不同剂量的电离辐照(0.5;1.0;2.0;4.0 Gy)用于实验动物(用米那霉素处理),而对照动物则接受米那霉素溶剂。米利亚星腹腔注射3次,单次剂量4.0 mg/kg,注射间隔24小时。最后一次剂量在照射前1天施用。髓核细胞作为试验对象,辐照后24小时进行分析。米利沙星具有一定的保护作用,可限制放射后骨髓消融,减少畸变细胞数量和畸变总数目。三萜的保护作用与辐射剂量呈反比关系,在0.5 Gy剂量时效果最为显著。在1.0和2.0 Gy的辐射剂量下,实验组小鼠的染色单体畸变值高于对照组小鼠,这可能是由于三萜的抗凋亡作用,从而确保了基因组严重受损的突变细胞的更高存活率。照射后24小时的保护作用可能表明其对放射损伤初级放射化学阶段的作用。这表明,三萜的保护作用机制是通过其先前显示的抗氧化活性介导的,因为它具有稳定细胞膜和使编码抗氧化保护酶的基因表达正常化的能力。因此,辐射后的抗诱变活性是其在辐射诱导免疫抑制过程中免疫保护作用的重要特征。就其限制诱变效应的能力而言,在0.5 ~ 1.0 Gray剂量范围内,米利沙星可被归类为弱辐射防护抗诱变剂,防护效率为20 ~ 40%。
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