[78] It was reported that platelets were recruited to the liver, delaying virus elimination and promoting immunopathological liver cell damage after viral infection.[38] Viral hepatitis in human is a disease arising from destruction of virus-infected hepatocytes caused by immune-mediated mechanisms.[79, 80] It is generally recognized that T cell-mediated cellular immunity is responsible for the liver damage. Lang et al. reported that lack of platelet-derived serotonin in serotonin-deficient mice normalized hepatic microcirculatory dysfunction, accelerated virus clearance in the liver, and reduced CD8+ T cell-dependent acute liver injury.[38] Iannacone et al. also revealed a harmful role of
find more activated platelets in mediating cytotoxic T lymphocyte-induced liver damage in mouse models with acute viral hepatitis.[36] In drug-induced hepatitis model, inhibition of platelet activation resulted in the reduction of hepatic platelet accumulation and liver necrosis.[81] Furthermore, it was reported that platelet activation and subsequent adherence to liver sinusoidal selleck chemicals endothelial cells (LSECs) promote the accumulation of neutrophils, which mediates hepatic injury after ischemia-reperfusion.[15, 82] Sindram et al. reported
that platelets caused the apoptosis of LSECs upon reperfusion of the cold ischemic rat liver.[37] On the other hand, it is well known that platelets immediately accumulate at injured tissue, where they release key mediators of hemostasis and promote healing.[21] Recently it was reported that tissue repair is delayed in platelet-depleted tuclazepam animals after postischemic liver injury, suggesting that platelets could have a protective effect against acute liver injury.[83] Hepatocytes are very sensitive to Fas-mediated apoptosis because the Fas antigen is constitutively expressed on hepatocytes.[84] Hepatocytic upregulation of Fas has been observed in hepatitis B and C, suggesting that the Fas/Fas Ligand system plays important roles in the trigger of hepatitis and other liver diseases.[85-87] In addition, because severe damage to LSECs and the disruption of the sinusoidal
lining are known to be major causes of acute liver injury, the protection of LSECs is very important for preventing acute liver injury, just like the proliferation of LSECs is a crucial requirement for liver regeneration.[37, 88-90] Hisakura et al. reported that platelets have a potent role in protecting against acute liver injuries.[31] The increment of platelets ameliorated Fas-induced hepatitis by preventing both the apoptosis of hepatocytes through the activation of the Akt signaling pathway, which is known to suppress apoptosis and promote cell survival, and the disruption of the sinusoidal lining.[31] The result suggested that platelets could play pivotal roles in preventing acute liver injury through the protection of non-parenchymal cells in addition to hepatocytes.