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首页> 外文期刊>Archives of Toxicology >Comparative effect of benzanthrone and 3-bromobenzanthrone on hepatic xenobiotic metabolism and anti-oxidative defense system in guinea pigs.
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Comparative effect of benzanthrone and 3-bromobenzanthrone on hepatic xenobiotic metabolism and anti-oxidative defense system in guinea pigs.

机译:苯并蒽醌和3-溴苯并蒽醌对豚鼠肝脏异种生物代谢和抗氧化防御系统的比较作用。

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摘要

Benzanthrone (BA) and 3-bromobenzanthrone (3-BBA) are important dye intermediates used in the manufacture of various vat and disperse dyes. BA has been implicated as a cause of hepatic malfunctions and dermal lesions in workers. However, not much information on halogenated BAs, especially 3-BBA, is available. Experiments were designed to undertake a comparative safety assessment of both BA and 3-BBA, given orally at a dose of 50 mg/kg body weight for 10 days to guinea pigs. There was a significant decrease (25%) in body weight with 3-BBA, whereas BA treatment did not cause any change. Serum glutamate oxaloacetate transaminase and glutamate pyruvate transminase were found to be significantly ( P<0.05) increased in 3-BBA- as well as in BA-treated animals. 3-BBA and BA led to substantial depletion of ascorbic acid in both liver and adrenal glands. However, depletion of ascorbic acid was more pronounced with 3-BBA (19.2-28.3%) than with BA (13.5-16.6%). 3-BBA and BA treatments caused 80% and 24% depletion of hepatic free sulfydryl content, while lipid peroxidation showed a significant enhancement of 73% and 47%, respectively. BA and 3-BBA caused decreases in cytochrome P-450 content and phase I enzymes particularly ethoxyresorufin- O-deethylase and aryl hydrocarbon hydroxylase, whereas phase II enzymes (quinone reductase and glutathione- S-transferase) were substantially increased. Activities of bio-antioxidant enzymes, viz., glutathione peroxidase, glutathione reductase, superoxide dismutase and catalase, were significantly increased by 153, 104, 20 and 67% in the 3-BBA-treated group, whereas the degree of increase in these parameters was relatively less in BA-treated group. The data indicate that both BA and 3-BBA can disturb membrane integrity by decreasing endogenous glutathione and ascorbic acid levels with a concomitant increase in lipid peroxidative damage. This may in turn lead to impairment of hepatic P-450-dependent monooxygenase, while the changes in antioxidant enzymes reveal oxidative stress. 3-BBA treatment caused dilation of portal triad with thickening of arterial wall, hyperplasia of Kupffer cells and influx of inflammatory cells between hepatic cords, which could be due to formation of Br(*) radical or due to formation of semiquinone type of intermediate following oxidation. The results may be interpreted to mean that industrial workers exposed to 3-BBA are at higher risk than those exposed to BA, and necessary precautions should be taken to safeguard their exposure risks.
机译:苯并蒽酮(BA)和3-溴苯并蒽酮(3-BBA)是重要的染料中间体,可用于制造各种还原染料和分散染料。 BA被认为是工人肝功能衰竭和皮肤损伤的原因。但是,有关卤代BA,尤其是3-BBA的信息不多。设计实验对BA和3-BBA进行比较安全性评估,对豚鼠口服10天内剂量为50 mg / kg体重。 3-BBA的体重显着降低(25%),而BA治疗未引起任何变化。发现3-BBA-以及BA治疗的动物的血清谷氨酸草酰乙酸转氨酶和谷氨酸丙酮酸转氨酶显着增加(P <0.05)。 3-BBA和BA导致肝脏和肾上腺的抗坏血酸大量消耗。但是,3-BBA(19.2-28.3%)比BA(13.5-16.6%)的抗坏血酸消耗更为明显。 3-BBA和BA处理导致80%和24%的肝游离巯基含量减少,而脂质过氧化分别显着增加73%和47%。 BA和3-BBA引起细胞色素P-450含量下降,I相酶,特别是乙氧基间苯二酚-O-脱乙基酶和芳基烃羟化酶,而II期酶(醌还原酶和谷胱甘肽-S-转移酶)显着增加。在3-BBA处理组中,生物抗氧化剂酶的活性,即谷胱甘肽过氧化物酶,谷胱甘肽还原酶,超氧化物歧化酶和过氧化氢酶的活性分别显着增加了153%,104%,20%和67%,而这些参数的升高程度在BA治疗组中相对较少。数据表明,BA和3-BBA均可通过降低内源性谷胱甘肽和抗坏血酸水平以及脂类过氧化损伤的增加而干扰膜的完整性。这可能反过来导致肝P-450依赖的单加氧酶受损,而抗氧化酶的变化揭示了氧化应激。 3-BBA治疗引起门三联征扩张,伴有动脉壁增厚,Kupffer细胞增生和肝索之间炎性细胞流入,这可能是由于Br(*)自由基的形成或半醌类型中间体的继发氧化。结果可能解释为,暴露于3-BBA的工业工人比暴露于BA的工业工人风险更高,因此应采取必要的预防措施以保护其暴露风险。

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