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Metabolic pre‐conditioning of cultured cells in physiological levels of insulin: Generating resistance to the lipid‐accumulating effects of plasma in hepatocytes
Author(s) -
Chan Christina,
Berthiaume François,
Washizu Junji,
Toner Mehmet,
Yarmush Martin L.
Publication year - 2002
Publication title -
biotechnology and bioengineering
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.136
H-Index - 189
eISSN - 1097-0290
pISSN - 0006-3592
DOI - 10.1002/bit.10275
Subject(s) - hepatocyte , albumin , bioartificial liver device , insulin , lipid metabolism , urea , lipid droplet , metabolism , medicine , chemistry , anabolism , endocrinology , triglyceride , biology , biochemistry , cholesterol , in vitro
Abstract Understanding the regulation of hepatocyte lipid metabolism is important for several biotechnological applications involving liver cells. During exposure of hepatocytes to plasma, as is the case in extracorporeal bioartificial liver assist devices, it has been reported that hepatic‐specific functions, e.g., albumin and urea synthesis and diazepam removal, are dramatically compromised and hepatocytes progressively accumulate cytoplasmic lipid droplets. We hypothesized that the composition of hepatocyte culture medium significantly affects lipid metabolism during subsequent plasma exposure. Rat hepatocytes were cultured in medium containing either physiological (50 μU/mL) or supra‐physiological (500 mU/mL) insulin levels for 1 week and then exposed to human plasma supplemented with or without amino acids. We found that insulin’s anabolic effects, such as stimulation of triglyceride storage, were carried over from the pre‐conditioning to the plasma exposure period. While hepatocytes cultured in high insulin medium accumulated large quantities of triglycerides during subsequent plasma exposure, culture in low insulin medium largely prevented lipid accumulation. Urea and albumin secretion, as well as the ammonia removal rate, were largely unaffected by insulin but increased with amino acid supplementation. Thus, hepatocyte metabolism during plasma exposure can be modulated by medium pre‐conditioning and supplements added to plasma. © 2002 Wiley Periodicals, Inc. Biotechnol Bioeng 78: 753–760, 2002.