Selective enhancement of glutathione S-transferase activity in liver and extrahepatic tissues of rat following oral administration of vanadate.

A Bishayee, M Chatterjee
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Abstract

The effect of oral administration of vanadate (100, 200 and 400 nM for 30 days) on the activity of the detoxifying enzyme system glutathione S-transferase (GST) in rat liver and in several extrahepatic tissues was examined. Vanadate showed a high activity as GST inducer in liver and in small intestine mucosa followed by large intestine mucosa and kidney in a dose-dependent manner. No significant alterations in GST activity were observed in forestomach and lung tissues after vanadate. Vanadate treatment that resulted in an enhancement of GST activity impaired neither hepatic nor renal function as evidenced by serum glutamic oxaloacetic transaminase, glutamic pyruvic transaminase, sorbitol dehydrogenase, urea, and creatinine. Since the ability to induce an increase of detoxifying enzyme activity by anticarcinogenic agents was found to correlate with their activity in the inhibition of tumorigenesis, the trace element vanadium might be considered a potential cancer chemopreventive agent.

口服钒酸盐对大鼠肝脏和肝外组织谷胱甘肽s转移酶活性的选择性增强。
研究了口服钒酸盐(100、200和400 nM,连续30 d)对大鼠肝脏和肝外组织解毒酶系统谷胱甘肽s转移酶(GST)活性的影响。钒酸盐在肝脏和小肠粘膜中表现出较高的GST诱导剂活性,其次是大肠黏膜和肾脏,并呈剂量依赖性。服用钒酸盐后,前胃和肺组织GST活性未见明显变化。血清谷草酰乙酸转氨酶、谷丙转氨酶、山梨醇脱氢酶、尿素和肌酐证明,钒酸盐治疗导致GST活性增强,不会损害肝肾功能。由于发现抗癌药物诱导解毒酶活性增加的能力与其抑制肿瘤发生的活性相关,微量元素钒可能被认为是一种潜在的癌症化学预防剂。
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