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细胞外pH对氨在肝细胞膜上分布比例及尿素生成的调控作用。

Control of ammonia distribution ratio across the liver cell membrane and of ureogenesis by extracellular pH.

作者信息

Rémésy C, Demigné C, Fafournoux P

出版信息

Eur J Biochem. 1986 Jul 15;158(2):283-8. doi: 10.1111/j.1432-1033.1986.tb09748.x.

Abstract

The mechanisms involved in ammonia uptake by rat liver cells and the effects of changes in extracellular pH have been investigated in vivo and in vitro. When NH4Cl solutions were infused in the hepatic portal vein, ammonia uptake by the liver was practically quantitative up to about 1 mM in afferent blood. Ammonia transfer into hepatocytes was extremely rapid: for 2 mM ammonia in external medium, the intracellular concentration reached 5 mM within 10 s. Comparatively, [14C]methylamine influx was slower and the cell concentrations did not reach a steady-state level, probably in relation with diffusion into the acidic lysosomal compartment. Intracellular accumulation of ammonia was dependent on the delta pH across the plasma membrane: the distribution ratio (internal/external) was about 1 for an external pH of 6.8 and about 5 at pH 8. Urea synthesis was maximal at physiological pH and markedly declined at pH 7.05. This inhibition was not affected by manipulation of bicarbonate concentrations in the medium, down to 10 mM. Additional inhibition of ureogenesis by 100 microM acetazolamide was also observed, particularly at low concentrations of bicarbonate in the medium. Inhibition of ureogenesis when extracellular pH is decreased could be ascribed to a lower availability of the NH3 form. Assuming that NH3 readily equilibrates between the various compartments, the availability of free ammonia for carbamoyl-phosphate synthesis could be tightly dependent on extracellular pH.

摘要

已经在体内和体外研究了大鼠肝细胞摄取氨的机制以及细胞外pH变化的影响。当将NH4Cl溶液注入肝门静脉时,在传入血液中氨的摄取量实际上在高达约1 mM时是定量的。氨向肝细胞的转移极其迅速:对于外部培养基中2 mM的氨,细胞内浓度在10秒内达到5 mM。相比之下,[14C]甲胺的流入较慢,并且细胞浓度未达到稳态水平,这可能与扩散到酸性溶酶体区室有关。氨的细胞内积累取决于跨质膜的pH差值:对于外部pH为6.8,分布比(内部/外部)约为1,在pH 8时约为5。尿素合成在生理pH下最大,在pH 7.05时明显下降。这种抑制不受培养基中碳酸氢盐浓度调节的影响,低至10 mM。还观察到100 microM乙酰唑胺对尿素生成的额外抑制作用,特别是在培养基中碳酸氢盐浓度较低时。细胞外pH降低时尿素生成的抑制可能归因于NH3形式的可用性降低。假设NH3在各个区室之间容易达到平衡,用于氨基甲酰磷酸合成的游离氨的可用性可能紧密依赖于细胞外pH。

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