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降血脂药物ICI53072和氯贝丁酯与苯巴比妥对大鼠肝脏大小、血流量和DNA含量影响的比较。

Comparison of the effects of the hypolipidaemic agents ICI53072 and clofibrate with those of phenobarbitone on liver size, blood flow and DNA content in the rat.

作者信息

Berman J S, Hiley C R, Wilson A C

出版信息

Br J Pharmacol. 1983 Mar;78(3):533-41. doi: 10.1111/j.1476-5381.1983.tb08813.x.

Abstract

1 The effects of the hypolipidaemic agents ICI 53072 and clofibrate on cardiac output and its distribution to the hepatosplanchnic bed were determined by the use of radioactive microspheres in the rat. The effects of these agents on hepatic DNA content were compared with those of phenobarbitone. Also the effects of ICI 53072 on hepatic microsomal enzymes and bile flow were determined together with the effects of phenobarbitone. 2 ICI 53072 and clofibrate both increased liver size and liver blood flow. A daily dose of 25 mg kg-1 ICI 53072 for 5 days increased liver weight by 55% and liver blood flow by 43%, the latter by enhancing the proportion of cardiac output passing to the hepatosplanchnic bed. The increased liver blood flow with clofibrate (480 mg kg-1 daily for 5 days) was the result of greater cardiac output but the change (35%) was half the increase in liver weight. 3 Phenobarbitone (80 mg kg-1 daily for 5 days) produced a fall in DNA content per unit mass of liver but no change in hepatic DNA relative to body weight. ICI 53072 (25 mg kg-1 daily) increased hepatic DNA relative to body weight but by a lesser extent than it increased liver weight as a proportion of body weight; hence DNA content per unit mass of liver decreased. Clofibrate at three dose levels increased hepatic DNA relative to body weight but only one dose significantly decreased DNA content as a proportion of liver weight. 4 Phenobarbitone (80 mg kg-1 daily) increased bile flow whereas ICI 53072 (25 mg kg-1 daily) had no effect. Both treatments increased hepatic cytochrome P450 content and cytochrome c reductase activity. 5 It is concluded that phenobarbitone increases liver size by hepatocyte enlargement rather than cellular proliferation but that the hepatomegaly produced by the hypolipidaemic agents, at least at some doses, is due to a mixture of both processes. 6 It is further concluded that there is no simple relationship between the mechanism of hepatic enlargement resulting from drug treatment and changes in liver blood flow.

摘要
  1. 采用放射性微球法测定了降血脂药物ICI 53072和氯贝丁酯对大鼠心输出量及其向肝脾床分布的影响。将这些药物对肝脏DNA含量的影响与苯巴比妥的影响进行了比较。同时还测定了ICI 53072对肝微粒体酶和胆汁流量的影响以及苯巴比妥的影响。

  2. ICI 53072和氯贝丁酯均增加了肝脏大小和肝血流量。每日给予25mg/kg的ICI 53072,连续5天,肝脏重量增加55%,肝血流量增加43%,后者是通过增加流向肝脾床的心输出量比例实现的。氯贝丁酯(每日480mg/kg,连续5天)使肝血流量增加是心输出量增加的结果,但变化(35%)仅为肝脏重量增加量的一半。

  3. 苯巴比妥(每日80mg/kg,连续5天)使单位肝脏质量的DNA含量下降,但相对于体重,肝脏DNA无变化。ICI 53072(每日25mg/kg)使相对于体重的肝脏DNA增加,但增加程度小于其使肝脏重量占体重比例的增加程度;因此,单位肝脏质量的DNA含量下降。三个剂量水平的氯贝丁酯均使相对于体重的肝脏DNA增加,但只有一个剂量显著降低了DNA占肝脏重量的比例。

  4. 苯巴比妥(每日80mg/kg)增加胆汁流量,而ICI 53072(每日25mg/kg)无此作用。两种处理均增加了肝脏细胞色素P450含量和细胞色素c还原酶活性。

  5. 得出结论:苯巴比妥通过肝细胞肿大而非细胞增殖增加肝脏大小,但降血脂药物产生的肝肿大,至少在某些剂量下,是这两个过程共同作用的结果。

  6. 进一步得出结论:药物治疗导致肝脏肿大的机制与肝血流量变化之间不存在简单的关系。

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Effect of clofibrate on DNA synthesis in rat liver and kidney.
Arch Toxicol. 1987;60(1-3):131-2. doi: 10.1007/BF00296965.

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