Attenuation of alcohol‐induced hepatocyte damage by ginsenoside Rg1 evaluated using atomic force microscopy

Abstract

AbstractAlcoholic liver disease is an important cause of death worldwide. Hepatocyte apoptosis is commonly observed in alcoholic liver disease. In this study, we investigated the effect of ginsenoside Rg1 (G‐Rg1), an organic component of ginseng, on the alcohol‐induced morphological and biophysical properties of hepatocytes. Human hepatocytes (HL‐7702) were treated in vitro with alcohol and G‐Rg1. The cell morphology was observed using scanning electron microscopy. Cell height, roughness, adhesion, and elastic modulus were detected using atomic force microscopy. We found that alcohol significantly induced hepatocyte apoptosis, whereas G‐Rg1 attenuated the alcohol‐induced hepatocyte damage. Scanning electron microscopy revealed that alcohol‐induced significant morphological changes in hepatocytes, including decreased cell contraction, roundness, and pseudopods, whereas G‐Rg1 inhibited these negative changes. Atomic force microscopy revealed that alcohol increased the cell height and decreased the adhesion and elastic modulus of hepatocytes. Following treatment with G‐Rg1, the cell height, adhesion, and elastic modulus of alcohol‐injured hepatocytes were all similar to those of normal cells. Thus, G‐Rg1 can attenuate the alcohol‐induced damage to hepatocytes by modulating the morphology and biomechanics of the cells.Research Highlights In this study, the morphological characteristics of hepatocytes were observed using SEM. The changes in hepatocyte three‐dimensional images and biomechanical action caused by alcohol and G‐Rg1 were examined at the nanoscale using AFM under near‐physiological conditions. Alcohol‐induced hepatocytes showed abnormal morphology and biophysical properties. G‐Rg1 attenuated the alcohol‐induced damage to hepatocytes by modulating the morphology and biomechanics of the cells.