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谷胱甘肽补充能力在分离的肝静脉周围肝细胞中比在肝门周围肝细胞中更低。

Glutathione replenishment capacity is lower in isolated perivenous than in periportal hepatocytes.

作者信息

Kera Y, Penttilä K E, Lindros K O

机构信息

Research Laboratories of the Finnish State Alcohol Company (Alko Ltd.), Helsinki, Finland.

出版信息

Biochem J. 1988 Sep 1;254(2):411-7. doi: 10.1042/bj2540411.

Abstract

The zonal distribution of GSH metabolism was investigated by comparing hepatocytes obtained from the periportal (zone 1) or perivenous (zone 3) region by digitonin/collagenase perfusion. Freshly isolated periportal and perivenous cells had similar viability (dye exclusion, lactate dehydrogenase leakage and ATP content) and GSH content (2.4 and 2.7 mumol/g respectively). During incubation, periportal cells slowly accumulated GSH (0.35 mumol/h per g), whereas in perivenous cells a decrease occurred (-0.14 mumol/h per g). Also, in the presence of either L-methionine or L-cysteine (0.5 mM) periportal hepatocytes accumulated GSH much faster (3.5 mumol/h per g) than did perivenous cells (1.9 mumol/h per g). These periportal-perivenous differences were also found in cells from fasted rats. Efflux of GSH was faster from perivenous cells than from periportal cells, but this difference only explained 10-20% of the periportal-perivenous difference in accumulation. Furthermore, periportal cells accumulated GSH to a plateau 26-40% higher than in perivenous cells. There was no significant difference in gamma-glutamylcysteine synthetase or glutathione synthetase activity between the periportal and perivenous cell preparations. The periportal-perivenous difference in GSH accumulation was unaffected by inhibition of gamma-glutamyl transpeptidase or by 5 mM-glutamate or -glutamine, but was slightly diminished by 2 mM-L-methionine. This suggests differences between periportal and perivenous cells in their metabolism and/or transport of (sulphur) amino acids. Our results suggest that a lower GSH replenishment capacity of the hepatocytes from the perivenous region may contribute to the greater vulnerability of this region to xenobiotic damage.

摘要

通过用洋地黄皂苷/胶原酶灌注法比较从门静脉周围(1区)或肝静脉周围(3区)获取的肝细胞,研究了谷胱甘肽(GSH)代谢的区域分布。新鲜分离的门静脉周围和肝静脉周围细胞具有相似的活力(染料排斥、乳酸脱氢酶泄漏和ATP含量)和GSH含量(分别为2.4和2.7 μmol/g)。在孵育过程中,门静脉周围细胞缓慢积累GSH(每克每小时0.35 μmol),而肝静脉周围细胞则出现下降(每克每小时-0.14 μmol)。此外,在存在L-蛋氨酸或L-半胱氨酸(0.5 mM)的情况下,门静脉周围肝细胞积累GSH的速度比肝静脉周围细胞快得多(每克每小时3.5 μmol)(每克每小时1.9 μmol)。在禁食大鼠的细胞中也发现了这些门静脉周围与肝静脉周围的差异。肝静脉周围细胞中GSH的流出速度比门静脉周围细胞快,但这种差异仅解释了积累过程中门静脉周围与肝静脉周围差异的10-20%。此外,门静脉周围细胞积累的GSH达到的平台水平比肝静脉周围细胞高26-40%。门静脉周围和肝静脉周围细胞制剂中γ-谷氨酰半胱氨酸合成酶或谷胱甘肽合成酶活性没有显著差异。GSH积累的门静脉周围与肝静脉周围差异不受γ-谷氨酰转肽酶抑制或5 mM谷氨酸或谷氨酰胺的影响,但2 mM L-蛋氨酸使其略有降低。这表明门静脉周围和肝静脉周围细胞在(硫)氨基酸的代谢和/或转运方面存在差异。我们的结果表明,肝静脉周围区域肝细胞较低的GSH补充能力可能导致该区域对异源生物损伤的更大易感性。

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