Literature DB >> 23878365

Activity and distribution of intracellular carbonic anhydrase II and their effects on the transport activity of anion exchanger AE1/SLC4A1.

Samer Al-Samir1, Symeon Papadopoulos, Renate J Scheibe, Joachim D Meißner, Jean-Pierre Cartron, William S Sly, Seth L Alper, Gerolf Gros, Volker Endeward.   

Abstract

We have investigated the previously published 'metabolon hypothesis' postulating that a close association of the anion exchanger 1 (AE1) and cytosolic carbonic anhydrase II (CAII) exists that greatly increases the transport activity of AE1. We study whether there is a physical association of and direct functional interaction between CAII and AE1 in the native human red cell and in tsA201 cells coexpressing heterologous fluorescent fusion proteins CAII-CyPet and YPet-AE1. In these doubly transfected tsA201 cells, YPet-AE1 is clearly associated with the cell membrane, whereas CAII-CyPet is homogeneously distributed throughout the cell in a cytoplasmic pattern. Förster resonance energy transfer measurements fail to detect close proximity of YPet-AE1 and CAII-CyPet. The absence of an association of AE1 and CAII is supported by immunoprecipitation experiments using Flag-antibody against Flag-tagged AE1 expressed in tsA201 cells, which does not co-precipitate native CAII but co-precipitates coexpressed ankyrin. Both the CAII and the AE1 fusion proteins are fully functional in tsA201 cells as judged by CA activity and by cellular HCO3(-) permeability (P(HCO3(-))) sensitive to inhibition by 4,4-Diisothiocyano-2,2-stilbenedisulfonic acid. Expression of the non-catalytic CAII mutant V143Y leads to a drastic reduction of endogenous CAII and to a corresponding reduction of total intracellular CA activity. Overexpression of an N-terminally truncated CAII lacking the proposed site of interaction with the C-terminal cytoplasmic tail of AE1 substantially increases intracellular CA activity, as does overexpression of wild-type CAII. These variously co-transfected tsA201 cells exhibit a positive correlation between cellular P(HCO3(-)) and intracellular CA activity. The relationship reflects that expected from changes in cytoplasmic CA activity improving substrate supply to or removal from AE1, without requirement for a CAII-AE1 metabolon involving physical interaction. A functional contribution of the hypothesized CAII-AE1 metabolon to erythroid AE1-mediated HCO3(-) transport was further tested in normal red cells and red cells from CAII-deficient patients that retain substantial CA activity associated with the erythroid CAI protein lacking the proposed AE1-binding sequence. Erythroid P(HCO3(-)) was indistinguishable in these two cell types, providing no support for the proposed functional importance of the physical interaction of CAII and AE1. A theoretical model predicts that homogeneous cytoplasmic distribution of CAII is more favourable for cellular transport of HCO3(-) and CO2 than is association of CAII with the cytoplasmic surface of the plasma membrane. This is due to the fact that the relatively slow intracellular transport of H(+) makes it most efficient to place the CA in the vicinity of the haemoglobin molecules, which are homogeneously distributed over the cytoplasm.

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Year:  2013        PMID: 23878365      PMCID: PMC3810803          DOI: 10.1113/jphysiol.2013.251181

Source DB:  PubMed          Journal:  J Physiol        ISSN: 0022-3751            Impact factor:   5.182


  54 in total

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  22 in total

1.  Carbonic anhydrase II binds to and increases the activity of the epithelial sodium-proton exchanger, NHE3.

Authors:  Devishree Krishnan; Lei Liu; Shane A Wiebe; Joseph R Casey; Emmanuelle Cordat; R Todd Alexander
Journal:  Am J Physiol Renal Physiol       Date:  2015-06-03

2.  Carbonic anhydrase inhibitors modify intracellular pH transients and contractions of rat middle cerebral arteries during CO2/HCO3- fluctuations.

Authors:  Jacob K Rasmussen; Ebbe Boedtkjer
Journal:  J Cereb Blood Flow Metab       Date:  2017-03-20       Impact factor: 6.200

Review 3.  Tumour acidosis: from the passenger to the driver's seat.

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Journal:  Nat Rev Cancer       Date:  2017-09-15       Impact factor: 60.716

4.  Transgenic expression of carbonic anhydrase III in cardiac muscle demonstrates a mechanism to tolerate acidosis.

Authors:  Han-Zhong Feng; J-P Jin
Journal:  Am J Physiol Cell Physiol       Date:  2019-08-07       Impact factor: 4.249

5.  Carbonic anhydrases enhance activity of endogenous Na-H exchangers and not the electrogenic Na/HCO3 cotransporter NBCe1-A, expressed in Xenopus oocytes.

Authors:  Fraser J Moss; Walter F Boron
Journal:  J Physiol       Date:  2020-10-11       Impact factor: 5.182

6.  Zebrafish and mouse TASK-2 K(+) channels are inhibited by increased CO2 and intracellular acidification.

Authors:  Gaspar Peña-Münzenmayer; María Isabel Niemeyer; Francisco V Sepúlveda; L Pablo Cid
Journal:  Pflugers Arch       Date:  2013-10-01       Impact factor: 3.657

Review 7.  Regulators of Slc4 bicarbonate transporter activity.

Authors:  Ian M Thornell; Mark O Bevensee
Journal:  Front Physiol       Date:  2015-06-12       Impact factor: 4.566

Review 8.  How does carbon dioxide permeate cell membranes? A discussion of concepts, results and methods.

Authors:  Volker Endeward; Samer Al-Samir; Fabian Itel; Gerolf Gros
Journal:  Front Physiol       Date:  2014-01-08       Impact factor: 4.566

9.  Dusp3 and Psme3 are associated with murine susceptibility to Staphylococcus aureus infection and human sepsis.

Authors:  Qin Yan; Batu K Sharma-Kuinkel; Hitesh Deshmukh; Ephraim L Tsalik; Derek D Cyr; Joseph Lucas; Christopher W Woods; William K Scott; Gregory D Sempowski; Joshua T Thaden; Joshua Thaden; Thomas H Rude; Sun Hee Ahn; Vance G Fowler
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10.  Transport metabolons with carbonic anhydrases.

Authors:  Joachim W Deitmer; Holger M Becker
Journal:  Front Physiol       Date:  2013-10-10       Impact factor: 4.566

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