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Serotonin reverts age-related capillarization and failure of regeneration in the liver through a VEGF-dependent pathway
Authors:Furrer Katarzyna  Rickenbacher Andreas  Tian Yinghua  Jochum Wolfram  Bittermann Anne Greet  Käch Andres  Humar Bostjan  Graf Rolf  Moritz Wolfgang  Clavien Pierre-Alain
Institution:Department of Surgery, Laboratory of the Swiss Hepato-Pancreato-Biliary and Transplantation Center, University of Zurich, CH-8091 Zurich, Switzerland.
Abstract:The function of the liver is well-preserved during the aging process, although some evidence suggests that liver regeneration might be impaired with advanced age. We observed a decreased ability of the liver to restore normal volume after partial hepatectomy in elderly mice, and we identified a pathway that rescued regeneration and was triggered by serotonin. 2,5-dimethoxy-4-iodoamphetamine (DOI), a serotonin receptor agonist, reversed the age-related pseudocapillarization of old liver and improved hepatosinusoidal blood flow. After hepatectomy, the open fenestrae were associated with a restored attachment of platelets to endothelium and the initiation of a normal regenerative response, including the up-regulation of essential growth mediators and serotonin receptors. In turn, hepatocyte proliferation recovered along with regain of liver volume and animal survival. DOI operates through the release of VEGF, and its effects could be blocked with anti-VEGF antibodies both in vitro and in vivo. These results suggest that pseudocapillarization in the aged acts as a barrier to liver regeneration. DOI breaks this restraint through an endothelium-dependent mechanism driven by VEGF. This pathway highlights a target for reversing the age-associated decline in the capacity of the liver to regenerate.
Keywords:aging liver  fenestrations  sinusoidal microperfusion
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