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α-萘异硫氰酸酯(ANIT)给药后大鼠肝胆功能和形态变化的时间关系。

Temporal relationship of changes in hepatobiliary function and morphology in rats following alpha-naphthylisothiocyanate (ANIT) administration.

作者信息

Kossor D C, Meunier P C, Handler J A, Sozio R S, Goldstein R S

机构信息

Department of Toxicology, SmithKline Beecham Pharmaceuticals, King of Prussia, Pennsylvania 19406.

出版信息

Toxicol Appl Pharmacol. 1993 Mar;119(1):108-14. doi: 10.1006/taap.1993.1049.

Abstract

These studies were designed to evaluate ANIT-induced changes in both hepatobiliary function and morphology during the onset, progression, and recovery of ANIT-induced cholestasis. A single oral dose of 150 mg/kg of ANIT or vehicle was administered by gavage to male Sprague-Dawley rats and hepatobiliary structure and function were evaluated 16, 24, 48, 72, and 168 hr later. Increased hepatocellular tight junction permeability, increased serum bile acids, and decreased bile acid excretion were observed 16 hr after ANIT administration. At 24 hr, bile flow was decreased in ANIT-treated rats, an effect accompanied by increased tight junction permeability, decreased bile acid excretion, and decreased erythritol clearance (estimate of canalicular flow). In addition, scattered small loci of hepatocellular necrosis accompanied by an inflammatory cell response were observed in ANIT-treated rats at this time, with no microscopic evidence of bile duct obstruction (BDO). These data suggest that the onset of ANIT-induced cholestasis was associated with hepatocanalicular changes and not BDO. In contrast, at 48 and 72 hr after ANIT treatment, cholestasis was more profound and was accompanied by mild hepatocellular necrosis and widespread BDO. Hepatocyte tight junction permeability in ANIT-treated rats was not different from controls at 72 hr. These data suggest that the pathogenesis of ANIT-induced cholestasis is biphasic; the onset of cholestasis appears to be associated with changes in hepatocanalicular function and increased tight junction permeability whereas the later and more profound phase of cholestasis appears to be related to a combination of BDO and hepatocellular dysfunction. The time course of biochemical and morphologic changes following ANIT treatment further suggests that the pathophysiologic changes during the onset or initiation phase of cholestasis differ from those involved in the later and more profound phase of ANIT-induced cholestasis.

摘要

这些研究旨在评估α-萘异硫氰酸酯(ANIT)诱导的胆汁淤积症在发病、进展和恢复过程中对肝胆功能和形态的影响。通过灌胃给雄性Sprague-Dawley大鼠单次口服150mg/kg的ANIT或赋形剂,在给药后16、24、48、72和168小时评估肝胆结构和功能。ANIT给药16小时后,观察到肝细胞紧密连接通透性增加、血清胆汁酸增加和胆汁酸排泄减少。在24小时时,ANIT处理的大鼠胆汁流量减少,同时伴有紧密连接通透性增加、胆汁酸排泄减少和赤藓醇清除率降低(小管流量估计值)。此外,此时在ANIT处理的大鼠中观察到散在的小灶性肝细胞坏死并伴有炎症细胞反应,无胆管阻塞(BDO)的微观证据。这些数据表明,ANIT诱导的胆汁淤积症的发病与肝小管变化有关,而非BDO。相比之下,在ANIT处理后48和72小时,胆汁淤积更为严重,并伴有轻度肝细胞坏死和广泛的BDO。在72小时时,ANIT处理的大鼠肝细胞紧密连接通透性与对照组无差异。这些数据表明,ANIT诱导的胆汁淤积症的发病机制是双相的;胆汁淤积的起始似乎与肝小管功能变化和紧密连接通透性增加有关,而胆汁淤积的后期和更严重阶段似乎与BDO和肝细胞功能障碍的组合有关。ANIT处理后生化和形态学变化的时间进程进一步表明,胆汁淤积症起始或启动阶段的病理生理变化与ANIT诱导的胆汁淤积症后期和更严重阶段的变化不同。

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