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Cloning and characterization of a human electrogenic Na+-HCO-3 cotransporter isoform (hhNBC)
Authors:Choi, Inyeong   Romero, Michael F.   Khandoudi, Nassirah   Bril, Antoine   Boron, Walter F.
Abstract:Our group recentlycloned the electrogenicNa+-HCO-3cotransporter (NBC) from salamander kidney and later from mammaliankidney. Here we report cloning an NBC isoform (hhNBC) from a humanheart cDNA library. hhNBC is identical to human renal NBC (hkNBC),except for the amino terminus, where the first 85 amino acids in hhNBCreplace the first 41 amino acids of hkNBC. About 50% of the amino acidresidues in this unique amino terminus are charged, compared with~22% for the corresponding 41 residues in hkNBC. Northern blotanalysis, with the use of the unique 5' fragment of hhNBC as aprobe, shows strong expression in pancreas and expression in heart andbrain, although at much lower levels. InXenopus oocytes expressing hhNBC,adding 1.5% CO2/10 mMHCO-3 hyperpolarizes the membrane andcauses a rapid fall in intracellular pH(pHi), followed by apHi recovery. Subsequent removalof Na+ causes a depolarization anda reduced rate of pHi recovery.Removal of Cl- from the bathdoes not affect the pHi recovery.The stilbene derivative DIDS (200 µM) greatly reduces thehyperpolarization caused by addingCO2/HCO-3.In oocytes expressing hkNBC, the effects of addingCO2/HCO-3and then removing Na+ were similarto those observed in oocytes expressing hhNBC. We conclude that hhNBCis an electrogenicNa+-HCO-3cotransporter and that hkNBC is also electrogenic.
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