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辐射引起的慢性氧化肾损伤可以用氨磷汀来减轻。

Radiation-induced chronic oxidative renal damage can be reduced by amifostine.

机构信息

Department of Radiation Oncology, Trakya University Faculty of Medicine, 22030 Edirne, Turkey.

出版信息

Med Oncol. 2012 Jun;29(2):768-75. doi: 10.1007/s12032-011-9870-7. Epub 2011 Feb 24.

Abstract

In the current study, amifostine is evaluated for its radioprotective role in serum and kidney tissue by oxidative (malondialdehyde-MDA, advanced oxidation protein product-AOPP) and antioxidative markers (catalase, glutathione-GSH, free-thiols-F-SH). Thirty Wistar albino 3-4 months old, female rats, were randomly divided into Group I (n = 10): Control, Group II (n = 10): Irradiation-alone, Group III (n = 10): Amifostine before irradiation. In Group II and III, right kidneys of the rats were irradiated with a single dose of 6 Gy using a 60Co treatment unit. Rats in Group III received 200 mg/kg amifostine intraperitoneally, 30 min prior to irradiation. Following sacrification at 24th week, blood and kidney tissue samples were collected. Statistical analysis was done by One-way ANOVA, Post hoc Bonferroni, Dunnett T3, and Mann-Whitney U tests. Administration of amifostine significantly decreased the serum AOPP and MDA levels when compared to the irradiation-only group (P = 0.004, P = 0.006; respectively). Also amifostine significantly increased serum catalase activities and GSH levels, when given 30 min prior to irradiation (P = 00.02, P = 0.000; respectively). In the kidney tissue, administration of amifostine significantly decreased AOPP and MDA levels (P = 0.002, P = 0.016; respectively). Tissue GSH activity was increased following amifostine administration (P = 0.001). There was no statistically significant result on histopathological evaluation. Amifostine may reduce radiation-induced nephropathy by inhibiting chronic oxidative stress. Biomarkers of oxidative stress in serum and kidney tissue may be used for evaluation of the radiation-induced nephropathy.

摘要

在当前的研究中,评估了氨磷汀在血清和肾脏组织中的放射防护作用,通过氧化(丙二醛-MDA、晚期氧化蛋白产物-AOPP)和抗氧化标记物(过氧化氢酶、谷胱甘肽-GSH、游离巯基-F-SH)。将 30 只 3-4 个月大的 Wistar 白化雌性大鼠随机分为 3 组:第 I 组(n = 10):对照组,第 II 组(n = 10):单独照射组,第 III 组(n = 10):照射前氨磷汀组。在第 II 组和第 III 组中,使用 60Co 治疗装置对大鼠右肾进行单次 6 Gy 照射。第 III 组大鼠在照射前 30 分钟给予 200 mg/kg 氨磷汀腹腔内注射。在第 24 周处死时,收集血液和肾脏组织样本。采用单因素方差分析、事后 Bonferroni、Dunnett T3 和 Mann-Whitney U 检验进行统计学分析。与单独照射组相比,氨磷汀的给药显著降低了血清 AOPP 和 MDA 水平(P = 0.004,P = 0.006)。此外,氨磷汀在照射前 30 分钟给予时,还显著增加了血清过氧化氢酶活性和 GSH 水平(P = 00.02,P = 0.000)。在肾脏组织中,氨磷汀的给药显著降低了 AOPP 和 MDA 水平(P = 0.002,P = 0.016)。组织 GSH 活性增加(P = 0.001)。组织学评估没有统计学意义。氨磷汀通过抑制慢性氧化应激可能减轻放射性肾病。血清和肾脏组织中氧化应激的生物标志物可用于评估放射性肾病。

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