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黄曲霉毒素B1体内处理对肝脏和肝外谷胱甘肽S-转移酶体外活性的影响。

Effect of aflatoxin B1 treatment in vivo on the in vitro activity of hepatic and extrahepatic glutathione S-transferase.

作者信息

Carrillo M C, Carnovale C E, Monti J A

机构信息

Instituto de Fisiologia Experimental, Facultad de Ciencias Bioquimicas y Farmaceuticas, Rosario, Argentina.

出版信息

Toxicol Lett. 1990 Jan;50(1):107-16. doi: 10.1016/0378-4274(90)90257-m.

DOI:10.1016/0378-4274(90)90257-m
PMID:2104996
Abstract

The effect of aflatoxin B1 (AFB1) on the glutathione S-transferase activity (GST) and on non-protein thiol levels of different tissues was studied in adult male Wistar rats. Animals received a single dose of the toxin (100 or 500 micrograms/kg body wt., p.o.), and were studied 6 or 24 h after administration. GST was determined in liver, renal cortex, duodenum, jejunum-ileum and distal ileum, using 3 substrates: 1-chloro-2,4-dinitrobenzene (CDNB), trans-4-phenyl-3-buten-2-one (PBO) and 1,2-epoxyethylbenzene (STOX). The non-protein thiol content of all tissues tested increased with the lowest dose at 6 h, returning to normal values at 24 h, while the higher dose produced a significant decrease in reduced thiol levels at 6 h, returning to normal values at 24 h. AFB1 administration induced, independently of dose and tissue, total GST (CDNB) and epoxide-transferase activity (STOX) while A--C-type transferases (PBO) were inhibited. Almost all activities returned to normal values at 24 h. In cases of enzyme induction there was in general an increase in Vmax and a decrease in apparent Km. The opposite was seen in cases of inhibition. In conclusion, the results provide evidence that extrahepatic GST could be important in the overall process of detoxification of AFB1. The behavior seen in hepatic and extrahepatic tissues revealed the functions of catalysis (B-type transferases) and covalent bond formation, as well as inactivation by probable AFB1 metabolites (A--C-type transferases).

摘要

在成年雄性Wistar大鼠中研究了黄曲霉毒素B1(AFB1)对不同组织中谷胱甘肽S-转移酶活性(GST)和非蛋白巯基水平的影响。动物接受单次剂量的毒素(100或500微克/千克体重,口服),并在给药后6或24小时进行研究。使用3种底物在肝脏、肾皮质、十二指肠、空肠-回肠和回肠末端测定GST:1-氯-2,4-二硝基苯(CDNB)、反式-4-苯基-3-丁烯-2-酮(PBO)和1,2-环氧乙基苯(STOX)。所有测试组织的非蛋白巯基含量在6小时时随着最低剂量增加,在24小时时恢复到正常值,而较高剂量在6小时时导致还原型巯基水平显著降低,在24小时时恢复到正常值。AFB1给药独立于剂量和组织诱导总GST(CDNB)和环氧化物转移酶活性(STOX),而A - C型转移酶(PBO)受到抑制。几乎所有活性在24小时时恢复到正常值。在酶诱导的情况下,通常Vmax增加而表观Km降低。在抑制的情况下则相反。总之,结果提供了证据表明肝外GST在AFB1解毒的整个过程中可能很重要。在肝脏和肝外组织中观察到的行为揭示了催化功能(B型转移酶)和共价键形成,以及可能的AFB1代谢物的失活作用(A - C型转移酶)。

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