Lipogenesis from n-butyrate in colonocytes |
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| Authors: | W E W Roediger O Kapaniris S Millard |
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| Institution: | (1) Cell Physiology Laboratory of the University of Adelaide Department of Surgery, Queen Elizabeth Hospital, 5011 Adelaide, S.A., Australia;(2) University of Adelaide, Department of Surgery, The Queen Elizabeth Hospital, 5011 Woodville, S.A., Australia |
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| Abstract: | Cell membranes of colonic epithelial cells (CEC) in ulcerative colitis show structural abnormalities which are specific to the disease and which suggest impaired lipogenesis in CECs. Lipogenesis from 1-14C]-n-butyrate, the chief oxidative fuel of colonic epithelial cells, was measured in isolated CECs under control conditions, with or without glucose and in the presence of mercaptoacetate, a major reducing agent in the colonic lumen- Glucose significantly (p < 0.01) stimulated lipogenesis from 1-14C]-butyrate which was reversed by 5 mM mercaptoacetate. Mercaptoacetate significantly diminished CEC thiolase activity (EC 2.3.1.9). 5-Aminosalicylic acid reversed the adverse effects of mercaptoacetate in the saponifiable fraction of extracted lipids. Changes in lipogenesis due to colonic luminal reducing agents would affect the barrier function of CECs a feature relevant to the disease process of ulcerative colitis. |
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| Keywords: | lipogenesis colonocyte n-butyrate mercaptoacetate ulcerative colitis |
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