Effects of acidosis on acute phase protein metabolism in liver cells.

C Ulrich, B Krüger, H Köhler, W Riegel
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引用次数: 8

Abstract

Metabolic acidosis has been shown to act as a causative factor in muscle protein breakdown and negative nitrogen balance, as well as in decreased albumin synthesis. Albumin and other acute phase proteins (APP) are mainly synthesized in the liver following induction by interleukins, hormones and other mediators. Acute phase proteins have been shown to be predictors of cardiovascular mortality in the general population and in patients with end stage renal disease (ESRD). Clinical investigation gives evidence that albumin is reduced by acidosis in ESRD patients. The aim of our study was to investigate the role of the liver in acidosis, i.e. the influence of acidosis on metabolic activity and secretion of APP by liver cells (HepG2). Cells were cultured in a medium containing different amounts of bicarbonate. Metabolic activity was significantly diminished when the bicarbonate concentration of the extracellular medium was reduced (86.13+/-1.90% (pH 7.0) vs. 99. 53+/-90% (pH 7.4); p<0.01). While cellular release of negative APP was significantly decreased (albumin: 4.6+/-0.41 (pH 7.0) vs. 7.54+/-0.62 (pH 7.4) [ng/microg protein], p<0.001, transferrin: (0. 78+/-0.08 (pH 7.0) vs. 1.07+/-0.07 (pH 7.4) [ng/microg protein], p<0. 05), no significant influence of acidosis (pH 7.0) on the positive APP, alpha(1)-acid glycoprotein (AGP) (1.69+/-0.25) (pH 7.0) vs. 1.62+/-0.23 (pH 7.4) [ng/microg protein]), could be shown. Our data indicate that acidosis results in inhibition of liver cell metabolic activity and in reduced secretion of the negative acute phase proteins albumin and transferrin. In contrast, secretion of the positive acute phase protein AGP seems to be unchanged at pH 7.0 as compared to pH 7.4. We conclude that negative and positive APP in liver cells (HepG2) appear to be differently regulated by acidosis.

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酸中毒对肝细胞急性期蛋白代谢的影响。
代谢性酸中毒已被证明是肌肉蛋白质分解和负氮平衡以及白蛋白合成减少的一个致病因素。白蛋白等急性期蛋白(APP)主要在肝脏内由白细胞介素、激素等介质诱导合成。急性期蛋白已被证明是一般人群和终末期肾病(ESRD)患者心血管死亡率的预测因子。临床研究表明,ESRD患者酸中毒导致白蛋白减少。我们的研究目的是探讨肝脏在酸中毒中的作用,即酸中毒对肝细胞(HepG2)代谢活性和APP分泌的影响。细胞在含有不同量碳酸氢盐的培养基中培养。当细胞外培养基中碳酸氢盐浓度降低时,代谢活性显著降低(86.13+/-1.90% (pH 7.0) vs. 99)。53+/-90% (pH 7.4);p
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Author Index Vol. 25, 1999 Manuscript Consultants Contents Vol. 25, 1999 Subject Index Vol. 25, 1999 Subject Index Vol. 25, No. 4–6, 1999
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