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Evidence of a link between erythrocyte band 3 phosphorylation and anion transport in patients with 'idiopathic' calcium oxalate nephrolithiasis.
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1993
Year
Electrolyte DisorderCalcium Oxalate NephrolithiasisRenal PathologyPathologyCytoskeletonCellular AnomaliesCellular PhysiologyRenal FunctionMembrane TransportElectrolyte DisturbanceChronic Kidney DiseaseCell SignalingBiochemistryAnion TransportProtein TransportRenal PathophysiologyCell BiologyProtein PhosphorylationUrologySignal TransductionNatural SciencesPhysiologyErythrocyte Band 3Band 3Oxalate Transmembrane FluxCellular BiochemistryMedicineNephrologyKidney Research
This study was carried out to verify the hypothesis of a link between faster endogenous phosphorylation of band 3 protein, the anion carrier, and anomalous oxalate transmembrane self-exchange found in erythrocyte from calcium oxalate renal stone formers. Agents able to modify 32P-labelling of band 3 protein induced a concurrent modification in oxalate transmembrane flux. Cyclic AMP- and phospholipid-sensitive Ca(2+)-independent protein kinases seem to be critical modulators of band 3 function. These observations demonstrate a close link between the band 3 phosphorylation state and its anion transport function, and provide new insights into the pathogenetic mechanisms of the cellular anomalies observed in calcium-oxalate renal stone disease.