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微囊藻毒素对小鳐(Raja erinacea)肝脏的毒性及丝氨酸/苏氨酸蛋白磷酸酶抑制作用的持续性

Hepatic toxicity and persistence of ser/thr protein phosphatase inhibition by microcystin in the little skate Raja erinacea.

作者信息

Runnegar M, Seward D J, Ballatori N, Crawford J M, Boyer J L

机构信息

Mount Desert Island Biological Laboratory, Salsbury Cove, Maine, 04672, USA.

出版信息

Toxicol Appl Pharmacol. 1999 Nov 15;161(1):40-9. doi: 10.1006/taap.1999.8783.

Abstract

Microcystin-induced ser/thr protein phosphatase (PP) inhibition and toxicity were examined in the little skate (Raja erinacea), an evolutionarily primitive marine vertebrate. As in mammals, PP inhibition and toxicity were exclusively hepatocellular, but were much more persistent in the skate. A dose of 63 microg/kg given iv to adult male skates resulted in the near complete inhibition of hepatic PP activity at 24 h. PP activity was still 95% inhibited 7 days after dosing in skates given 125 microg/kg microcystin. Mortality occurred at doses of 500 microg/kg or more. Hepatic lesions were only seen in animals with fully inhibited PP activity in liver. The histological changes seen at 125 microg/kg were mild periportal inflammatory changes increasing in severity together with hepatocyte necrosis at higher doses of microcystin. Microcystin persisted and could be detected in plasma up to 7 days after dosing. This finding shows that, in the skate, as in mammals, the liver is the only organ capable of uptake of microcystin, since there was no significant inhibition of PP activity in the rectal gland and small decreases in PP activity of the kidney that were not time or dose dependent. In vitro microcystin caused dose-dependent inhibition of PP activity in isolated skate hepatocytes, while it was without effect in cultured rectal glands. Uptake of microcystin and the accompanying inhibition of PP activity in skate hepatocytes was prevented by the addition of a series of organic dyes and bile acids. The spectrum of inhibitors of microcystin uptake in skate is similar to that seen in the rat, indicating common features of the carrier(s) in these diverse species.

摘要

在小斑鳐(Raja erinacea,一种进化上原始的海洋脊椎动物)中研究了微囊藻毒素诱导的丝氨酸/苏氨酸蛋白磷酸酶(PP)抑制作用和毒性。与哺乳动物一样,PP抑制作用和毒性仅发生在肝细胞中,但在鳐鱼中持续时间长得多。给成年雄性鳐鱼静脉注射63微克/千克的剂量,在24小时时导致肝脏PP活性几乎完全被抑制。给鳐鱼注射125微克/千克微囊藻毒素后7天,PP活性仍被抑制95%。剂量达到500微克/千克或更高时出现死亡。肝脏病变仅在肝脏PP活性完全被抑制的动物中出现。在125微克/千克剂量下观察到的组织学变化为轻度门周炎症变化,随着微囊藻毒素剂量增加,严重程度增加,同时伴有肝细胞坏死。微囊藻毒素持续存在,给药后7天血浆中仍可检测到。这一发现表明,在鳐鱼中,与哺乳动物一样,肝脏是唯一能够摄取微囊藻毒素的器官,因为直肠腺中PP活性没有明显抑制,肾脏中PP活性仅有轻微下降,且与时间或剂量无关。体外实验中,微囊藻毒素对分离的鳐鱼肝细胞中的PP活性产生剂量依赖性抑制,而对培养的直肠腺无作用。添加一系列有机染料和胆汁酸可阻止微囊藻毒素在鳐鱼肝细胞中的摄取及随之而来的PP活性抑制。鳐鱼中微囊藻毒素摄取抑制剂的谱与大鼠中所见相似,表明这些不同物种中载体的共同特征。

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