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首页> 外文期刊>International Journal of Radiation Biology: Covering the Physical, Chemical, Biological, and Medical Effects of Ionizing and Non-ionizing Radiations >Early changes in L-arginine-nitric oxide metabolic pathways in response to the whole-body gamma irradiation of rats.
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Early changes in L-arginine-nitric oxide metabolic pathways in response to the whole-body gamma irradiation of rats.

机译:L-精氨酸一氧化氮代谢途径的早期变化对大鼠全身γ射线的响应。

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摘要

PURPOSE: Nitric oxide (NO), a reactive radical, is formed in higher amounts from L-arginine by inducible NO synthase (iNOS) during early response to ionizing radiation presumably as a part of signal transduction pathways. This study investigated the changes in L-arginine-NO metabolic pathways within a 24-hour period after whole-body gamma irradiation of rats with the range of low to supra-lethal doses. MATERIALS AND METHODS: Young adult female Wistar rats received either 0-50 Gy whole-body irradiation or an intraperitoneal injection of bacterial lipopolysaccharide (LPS, 10 mg/kg). Exhaled NO was monitored using chemiluminiscence, nitrite + nitrate (NO(x)) and L-arginine were assayed by high-performance liquid chromatography, and expression of iNOS was determined using Western blot. RESULTS: Irradiation resulted in a dose-dependent increase of plasma NO(x) to maximum levels which were 4-fold higher compared to controls (p < 0.001). The NO(x) levels increased less in the bronchoalveolar lavage fluid (BAL) (1.7-fold, p < 0.001) and liver homogenate (2.5-fold, p < 0.05), respectively, and were dose-independent. Exhaled NO, lung NO(x), plasma and BAL L-arginine, and the expression of iNOS in lung and liver tissues of irradiated rats and controls were similar. LPS caused a considerable increase (p < 0.001) in exhaled NO (61-fold), NO(x) levels (plasma 34-fold, BAL 6-fold, lung 5-fold, liver 4-fold), and in iNOS expression, respectively. CONCLUSION: In contrast to the LPS treatment of rats, the radiation-induced changes in L-arginine-NO metabolic pathways are modest, particularly in the airways and lungs. Noninvasive measurement of exhaled NO within a 24-h period following the exposure of rats to ionizing radiation has no value for biodosimetry.
机译:目的:一氧化氮(NO)是一种反应性自由基,在对电离辐射的早期响应过程中,由诱导型一氧化氮合酶(iNOS)从L-精氨酸中形成的量较高,大概是信号转导途径的一部分。这项研究调查了在全身伽马射线辐照低至超致死剂量范围的大鼠后24小时内L-精氨酸-NO代谢途径的变化。材料和方法:成年雌性Wistar大鼠接受0-50 Gy全身照射或腹膜内注射细菌性脂多糖(LPS,10 mg / kg)。使用化学发光法监测呼出的NO,通过高效液相色谱法测定亚硝酸盐+硝酸盐(NO(x))和L-精氨酸,并使用Western blot检测iNOS的表达。结果:辐照导致血浆NO(x)剂量依赖性增加至最大水平,与对照组相比增加了4倍(p <0.001)。支气管肺泡灌洗液(BAL)中NO(x)的增加较少(1.7倍,p <0.001)和肝匀浆(2.5倍,p <0.05),并且与剂量无关。呼出的NO,肺NO(x),血浆和BAL L-精氨酸以及iNOS在辐照大鼠和对照组的肺和肝组织中的表达相似。 LPS导致呼出的NO(61倍),NO(x)水平(血浆34倍,BAL 6倍,肺5倍,肝脏4倍)和iNOS表达显着增加(p <0.001) , 分别。结论:与LPS治疗的大鼠相反,L-精氨酸-NO代谢途径的辐射诱导变化是适度的,尤其是在气道和肺中。在大鼠暴露于电离辐射后的24小时内,无创测量呼出的NO对生物剂量测定没有价值。

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