Literature DB >> 30580922

A Model of Piezo1-Based Regulation of Red Blood Cell Volume.

Saša Svetina1, Tjaša Švelc Kebe2, Bojan Božič3.   

Abstract

A red blood cell (RBC) performs its function of adequately carrying respiratory gases in blood by its volume being ∼60% of that of a sphere with the same membrane area. For this purpose, human and most other vertebrate RBCs regulate their content of potassium (K+) and sodium (Na+) ions. The focus considered here is on K+ efflux through calcium-ion (Ca2+)-activated Gárdos channels. These channels open under conditions that allow Ca2+ to enter RBCs through Piezo1 mechanosensitive cation-permeable channels. It is postulated that the fraction of open Piezo1 channels depends on the RBC shape as a result of the curvature-dependent Piezo1-bilayer membrane interaction. The consequences of this postulate are studied by introducing a simple model of RBC osmotic behavior supplemented by the dependence of RBC membrane K+ permeability on the reduced volume (i.e., the ratio of cell volume to its maximal possible volume) of RBC discoid shapes. It is assumed that because of its intrinsic curvature and strong interaction with the surrounding membrane, Piezo1 tends to concentrate in the dimple regions of these shapes, and the fraction of open Piezo1 channels depends on the membrane curvature in that region. It is shown that the properties of the described model can provide the basis for the formation of the negative feedback loop that interrelates cell volume and its content of potassium ions. The model predicts the relation, valid for each cell in an RBC population, between RBC volume and membrane area, thus explaining the large value of the measured membrane area versus the volume correlation coefficient. The mechanism proposed here for RBC volume regulation is in accord with the loss of this correlation in RBCs of Piezo1 knockout mice.
Copyright © 2018 Biophysical Society. Published by Elsevier Inc. All rights reserved.

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Year:  2018        PMID: 30580922      PMCID: PMC6342734          DOI: 10.1016/j.bpj.2018.11.3130

Source DB:  PubMed          Journal:  Biophys J        ISSN: 0006-3495            Impact factor:   4.033


  52 in total

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Authors:  Harvey T McMahon; Jennifer L Gallop
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Authors:  Else K Hoffmann; Ian H Lambert; Stine F Pedersen
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3.  Sorting of integral membrane proteins mediated by curvature-dependent protein-lipid bilayer interaction.

Authors:  Bojan Božič; Sovan L Das; Saša Svetina
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Review 4.  Piezos thrive under pressure: mechanically activated ion channels in health and disease.

Authors:  Swetha E Murthy; Adrienne E Dubin; Ardem Patapoutian
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Journal:  Science       Date:  2010-09-02       Impact factor: 47.728

6.  Generation of normal human red cell volume, hemoglobin content, and membrane area distributions by "birth" or regulation?

Authors:  V L Lew; J E Raftos; M Sorette; R M Bookchin; N Mohandas
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7.  Mutations in the mechanotransduction protein PIEZO1 are associated with hereditary xerocytosis.

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Review 8.  Red blood cell shape and deformability in the context of the functional evolution of its membrane structure.

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Journal:  Cell Mol Biol Lett       Date:  2012-01-21       Impact factor: 5.787

9.  Mechanical sensitivity of Piezo1 ion channels can be tuned by cellular membrane tension.

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10.  Accelerating metabolism and transmembrane cation flux by distorting red blood cells.

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Journal:  Sci Adv       Date:  2017-10-18       Impact factor: 14.136

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2.  Membrane Localization of Piezo1 in the Context of Its Role in the Regulation of Red Blood Cell Volume.

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5.  Surface model of the human red blood cell simulating changes in membrane curvature under strain.

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