首页   按字顺浏览 期刊浏览 卷期浏览 The Hepatic Sinusoid in Aging and CirrhosisEffects on Hepatic Substrate Disposition and...
The Hepatic Sinusoid in Aging and CirrhosisEffects on Hepatic Substrate Disposition and Drug Clearance

 

作者: David G Le Couteur,   Robin Fraser,   Sarah Hilmer,   Laurent P Rivory,   Allan J McLean,  

 

期刊: Clinical Pharmacokinetics  (ADIS Available online 2005)
卷期: Volume 44, issue 2  

页码: 187-200

 

ISSN:0312-5963

 

年代: 2005

 

出版商: ADIS

 

关键词: Cirrhosis;Liver dysfunction;Clinical pharmacokinetics

 

数据来源: ADIS

 

摘要:

The fenestrated sinusoidal endothelium (‘liver sieve’) and space of Disse in the healthy liver do not impede the transfer of most substrates, including drugs and oxygen, from the sinusoidal lumen to the hepatocyte. Plasma components transfer freely in both directions through the endothelial fenestrations and into the space of Disse. The endothelium is attenuated, there is no basement membrane and there is minimum collagen in the space of Disse, thus minimising any barriers to substrate diffusion.Both cirrhosis and aging are associated with marked structural changes in the sinusoidal endothelium and space of Disse that are likely to influence bulk plasma transfer into the space of Disse, and diffusion through the endothelium and space of Disse. These changes, termed capillarisation and pseudocapillarisation in cirrhosis and aging, respectively, impede the transfer of various substrates. Capillarisation is associated with exclusion of albumin, protein-bound drugs and macromolecules from the space of Disse, and the progressive transformation of flow-limited to barrier-limited distribution of some substrates.There is evidence that the sinusoidal changes in cirrhosis and aging contribute to hepatocyte hypoxia, thus providing a mechanism for the apparent differential reduction of oxygen-dependent phase I metabolic pathways in these conditions. Structural change and subsequent dysfunction of the liver sieve warrant consideration as a significant factor in the impairment of overall substrate handling and hepatic drug metabolism in cirrhosis and aging.

 

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