4.0 Article Proceedings Paper

Role of RhAG and AQP1 in NH3 and CO2 gas transport in red cell ghosts:: a stopped-flow analysis

期刊

TRANSFUSION CLINIQUE ET BIOLOGIQUE
卷 13, 期 1-2, 页码 117-122

出版社

ELSEVIER FRANCE-EDITIONS SCIENTIFIQUES MEDICALES ELSEVIER
DOI: 10.1016/j.tracli.2006.03.004

关键词

gas permeability; NH3 transport; CO2 transport; stopped-flow; red cells; human and mouse variants

资金

  1. NIDDK NIH HHS [DK35124] Funding Source: Medline

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To clarify the potential role Rh/RhAG and AQP1 proteins in erythrocyte gas transport, NH3 and CO2 transport was measured in erythrocyte ghost membrane vesicles from rare human variants (Rh-null, COnull) and knockout mice (homozygous AQPI(-/-), Rh-/- and Rhag(-/-)) exhibiting well-characterized protein defects. Transport was measured from intracellular pH (pH(i)) changes in a stopped-flow fluorimeter. NH3 transport was measured in chloride-free conditions with ghosts exposed to 20 mM inwardly directed gradients of gluconate salts of ammonium, hydrazine and methylammonium at 15 degrees C. Alkalinization rates of control samples were 6.5 +/- 0.3, 4.03 +/- 0.17, 0.95 +/- 0.08 s(-1) for each solute, respectively, but were significantly reduced for Rh-null and Co-null samples that are deficient in RhAG and AQP1 proteins, respectively. Alkalinization rates of Rh-null ghosts were about 60%, 83% and 94% lower than that in control ghosts, respectively, for each Solute. In COnull ghosts, the lack of AQP1 resulted in about 30% reduction of the alkalinization rates as compared to controls, but the transport selectivity of RhAG for the three solutes was preserved. Similar observations were made with ghosts from KO mice Rhag(-/-) and AQPI(-/-). These results confirm the major contribution of RhAG/Rhag in the NH3 conductance of erythrocytes and Suggest that the reduction of transport rates in the absence of AQPI would be better explained by a direct or indirect effect on RhAG/Rhag-mediated transport. When ghosts were preloaded with carbonic anhydrase and exposed to a 25 mM CO2/HCO3- gradient at 6 degrees C, an extremely rapid kinetics of acidification corresponding to CO2 influx was observed. The rate constants were not significantly different between controls and human variants (125 +/- 6 s(-1)), or between wild-type and KO mice, Suggesting no major role of RhAG or AQP1 in CO2 transport, at least in our experimental conditions. (c) 2006 Elsevier SAS. All rights reserved.

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