Liver aging and pseudocapillarization in a Werner syndrome mouse model.

[werner syndrome]

Werner syndrome is a progeric syndrome characterized by premature atherosclerosis , diabetes , cancer , and death in humans . The knockout mouse model created by deletion of the RecQ helicase domain of the mouse Wrn homologue gene (Wrn (∆hel /∆hel )) is of great interest because it develops atherosclerosis and hypertriglyceridemia , conditions associated with aging liver and sinusoidal changes . Here , we show that Wrn (∆hel /∆hel ) mice exhibit increased extracellular matrix , defenestration , decreased fenestration diameter , and changes in markers of liver sinusoidal endothelial cell inflammation , consistent with age-related pseudocapilliarization . In addition , hepatocytes are larger , have increased lipofuscin deposition , more frequent nuclear morphological anomalies , decreased mitochondria number , and increased mitochondrial diameter compared to wild-type mice . The Wrn (∆hel /∆hel ) mice also have altered mitochondrial function and altered nuclei . Microarray data revealed that the Wrn (∆hel /∆hel ) genotype does not affect the expression of many genes within the isolated hepatocytes or liver sinusoidal endothelial cells . This study reveals that Wrn (∆hel /∆hel ) mice have accelerated typical age-related liver changes including pseudocapillarization . This confirms that pseudocapillarization of the liver sinusoid is a consistent feature of various aging models . Moreover , it implies that DNA repair may be implicated in normal aging changes in the liver .