Literature DB >> 9516379

Molecular identification and expression of erythroid K:Cl cotransporter in human and mouse erythroleukemic cells.

C M Pellegrino1, A C Rybicki, S Musto, R L Nagel, R S Schwartz.   

Abstract

A major pathway for K+ efflux in human reticulocytes and young RBCs is K:Cl cotransport (K:Cl-CT). The activity of K:Cl-CT is increased in pathologic RBCs containing hemoglobins S and C and may contribute to the abnormal dehydration state of these cells. Human K:Cl-CT (gene product KCC1) has been recently sequenced from human (hKCC1), rabbit and rat tissue by Gillen et al. (J Biol Chem 271:16237, 1996). We report here the sequence of KCC1 from human and mouse erythroleukemic cells (K562 and MEL cells, respectively). The cDNA for human erythroid-KCC1 is 100% identical to hKCC1 and the cDNA for mouse erythroid-KCC1 shares 89% identity with hKCC1, which translates to 96% identity at the amino acid level. Mammalian KCC1 is strongly conserved with >95% identity between human, rabbit, rat, and mouse KCC1 proteins. We did not detect any full-length mRNA transcripts of human erythroid-KCC1 in circulating reticulocytes. We detected two mRNA isoforms of human erythroid-KCC1 that resulted in C-terminal truncated proteins (73 amino acid and 17 amino acids, respectively). Human and mouse erythroidKCC1 differed at several consensus sites including a predicted PKC phosphorylation site at 108threonine and a predicted CK2 phosphorylation site at 51serine, within the predicted cytoplasmic N-terminal, that are present in human but not mouse erythroid-KCC1. Expression of MEL-KCC1 mRNA increases substantially upon DMSO-induced differentiation opening the possibility that erythroid-KCC1 plays a role in early erythroid maturation events. The molecular identification of erythroid-KCC1 is an important step towards understanding the physiologic role mediated by this protein in young and pathologic RBCs and during erythropoiesis, as well as providing a new tool for the elucidation of pathways and signals involved in RBC volume regulation. Copyright 1998 The Blood Cells Foundation.

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Year:  1998        PMID: 9516379     DOI: 10.1006/bcmd.1998.0168

Source DB:  PubMed          Journal:  Blood Cells Mol Dis        ISSN: 1079-9796            Impact factor:   3.039


  15 in total

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Review 4.  K-Cl cotransporters, cell volume homeostasis, and neurological disease.

Authors:  Kristopher T Kahle; Arjun R Khanna; Seth L Alper; Norma C Adragna; Peter K Lauf; Dandan Sun; Eric Delpire
Journal:  Trends Mol Med       Date:  2015-07-01       Impact factor: 11.951

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7.  Effect of intracellular magnesium and oxygen tension on K+-Cl- cotransport in normal and sickle human red cells.

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9.  Disruption of erythroid K-Cl cotransporters alters erythrocyte volume and partially rescues erythrocyte dehydration in SAD mice.

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