期刊
JOURNAL OF HEPATOLOGY
卷 40, 期 5, 页码 766-773出版社
ELSEVIER SCIENCE BV
DOI: 10.1016/j.jhep.2004.01.023
关键词
cGMP transport; nitric oxide; soluble guanylate cyclase; cGMP homeostasis; hepatic encephalopathy
Background/Aims: Patients with liver disease show increased plasma cGMP and decreased intracellular cGMP in lymphocytes. The initial aim of this work was to assess whether decreased intracellular cGMP and increased plasma cGMP may be due to increased ATP-dependent release of cGMP from cells. The results obtained led to a new aim: to identify and quantify a protein responsible for the increased cGMP binding found in erythrocyte membranes from patients with liver disease. Methods: ATP-dependent cGMP transport was determined in inside-out vesicles from erythrocyte membranes. cGMP-binding proteins were isolated from the membranes and identified by MALDI-TOF peptide mass fingerprint. Protein kinase A was quantified by immunoblotting. Results: ATP-independent cGMP binding is increased in erythrocyte membranes from patients. There is a significant increase in the membrane content of a cGMP-binding protein with Mr 48,000, which was identified as the regulatory subunit of protein kinase A. Conclusions: The content of the regulatory subunit of protein kinase A is significantly increased (twice) in erythrocyte membranes from patients with liver cirrhosis. This protein binds cGMP strongly and may be responsible for the decrease in intracellular cGMP in liver disease. (C) 2004 European Association for the Study of the Liver. Published by Elsevier B.V. All rights reserved.
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