Pre-irradiation effects of ectoine on radiation-induced cardiotoxicity in female Swiss albino mice model

Sameh F. Nakhla, Basma Albehery, Sana Shawky, Salwa Lotfi, M. Kotb, E. El-Bassiouni, Eman El-Abd
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Abstract

Ectoine is a compatible solute that acts as a natural protectant. In the mice model, a single post-irradiation ectoine dose showed protective effects by modulating both inflammatory and oxidative stress pathways. The effect of ectoine has never been tested on mice cardiac tissue, thus the current study aimed to explore the pre-irradiation effect(s) of ectoine on radiation-induced cardiotoxicity. Forty female Swiss albino mice (17.6-23.1 g); controls (injected intraperitoneally for ten days with 0.2 mL saline), ectoine groups injected with 20 mg/kg of ectoine for ten days), irradiated groups (injected intraperitoneally for ten days with 0.2 mL saline then received six Gy whole body x-irradiation single dose), ectoine irradiated groups (injected with ectoine for ten days then irradiated). Animals were sacrificed on days seven, and 14 (five animals each). Hearts were examined for histological changes and immune-stained for Bax. Ectoine concentration in hearts was measured by HPLC. Serum cardiac troponin T, Total antioxidant capacity, and apoptosis-inducing factor were evaluated by mice with ready-to-use ELISA kits. Heart histological changes were documented in 40% of the 7- & 14-days post-irradiation. Ectoine concentrations (0.63 x 10 -4 mg/mg of heart weight) were higher in ectoine groups than ectoine irradiated groups (0.011 x 10 -4 mg/mg) 14-days post-treatment. Serum troponin T significantly differed between the 14 days groups ( p = 0.032). Apoptosis inducible factor significantly increased in ectoine irradiated group (at 14 days) than those of control ( p = 0.014), irradiated ( p = 0.020), and ectoine ( p = 0.033) groups. Bax showed strong to moderate immunostaining in ectoine and irradiated groups. In conclusion, Ectoine has pre-irradiation partial protective effects on heart cytotoxicity.
外托碱对瑞士雌性白化小鼠模型辐射致心脏毒性的辐照前作用
依托碱是一种相容的溶质,作为天然保护剂。在小鼠模型中,单次辐照后异托因剂量通过调节炎症和氧化应激途径显示出保护作用。依托碱对小鼠心脏组织的影响尚未进行过实验,因此本研究旨在探讨依托碱对辐射引起的心脏毒性的辐照前作用。40只瑞士白化雌性小鼠(17.6-23.1 g);对照组(0.2 mL生理盐水腹腔注射10天)、异托碱组(20 mg/kg异托碱腹腔注射10天)、照射组(0.2 mL生理盐水腹腔注射10天,然后接受6 Gy全身x射线单剂量照射)、异托碱照射组(异托碱注射10天,然后照射)。动物在第7天和第14天献祭(每天5只)。检查心脏组织学变化和Bax免疫染色。采用高效液相色谱法测定心脏内异托因浓度。小鼠血清肌钙蛋白T、总抗氧化能力和凋亡诱导因子用即用型ELISA试剂盒进行测定。在照射后7天和14天,有40%的患者发生了心脏组织学变化。治疗14天后,依托碱组的依托碱浓度(0.63 × 10 -4 mg/mg心脏重量)高于依托碱照射组(0.011 × 10 -4 mg/mg)。14 d组间血清肌钙蛋白T差异有统计学意义(p = 0.032)。凋亡诱导因子在外托碱照射组(14 d)显著高于对照组(p = 0.014)、照射组(p = 0.020)和外托碱组(p = 0.033)。体外托碱组和辐照组Bax显示强至中度免疫染色。综上所述,依托碱对心脏细胞毒性具有局部保护作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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