Voltage-Dependent Inactivation of MscS Occurs Independently of the Positively Charged Residues in the Transmembrane Domain

MscS (mechanosensitive channel of small conductance) is ubiquitously found among bacteria and plays a major role in avoiding cell lysis upon rapid osmotic downshock. The gating of MscS is modulated by voltage, but little is known about how MscS senses membrane potential. Three arginine residues (Arg...

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Main Authors: Takeshi Nomura, Masahiro Sokabe, Kenjiro Yoshimura
Format: Article
Language:English
Published: Hindawi Limited 2016-01-01
Series:BioMed Research International
Online Access:http://dx.doi.org/10.1155/2016/2401657
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spelling doaj-7f1ce14e7ec242988d6fbbbc6e45cb4b2020-11-24T20:57:51ZengHindawi LimitedBioMed Research International2314-61332314-61412016-01-01201610.1155/2016/24016572401657Voltage-Dependent Inactivation of MscS Occurs Independently of the Positively Charged Residues in the Transmembrane DomainTakeshi Nomura0Masahiro Sokabe1Kenjiro Yoshimura2International Cooperative Research Project (ICORP)/Solution Oriented Research for Science and Technology (SORST), Cell-Mechanosensing Project, Japan Science and Technology Agency, Nagoya 466-8550, JapanInternational Cooperative Research Project (ICORP)/Solution Oriented Research for Science and Technology (SORST), Cell-Mechanosensing Project, Japan Science and Technology Agency, Nagoya 466-8550, JapanInternational Cooperative Research Project (ICORP)/Solution Oriented Research for Science and Technology (SORST), Cell-Mechanosensing Project, Japan Science and Technology Agency, Nagoya 466-8550, JapanMscS (mechanosensitive channel of small conductance) is ubiquitously found among bacteria and plays a major role in avoiding cell lysis upon rapid osmotic downshock. The gating of MscS is modulated by voltage, but little is known about how MscS senses membrane potential. Three arginine residues (Arg-46, Arg-54, and Arg-74) in the transmembrane (TM) domain are possible to respond to voltage judging from the MscS structure. To examine whether these residues are involved in the voltage dependence of MscS, we neutralized the charge of each residue by substituting with asparagine (R46N, R54N, and R74N). Mechanical threshold for the opening of the expressed wild-type MscS and asparagine mutants did not change with voltage in the range from -40 to +100 mV. By contrast, inactivation process of wild-type MscS was strongly affected by voltage. The wild-type MscS inactivated at +60 to +80 mV but not at -60 to +40 mV. The voltage dependence of the inactivation rate of all mutants tested, that is, R46N, R54N, R74N, and R46N/R74N MscS, was almost indistinguishable from that of the wild-type MscS. These findings indicate that the voltage dependence of the inactivation occurs independently of the positive charges of R46, R54, and R74.http://dx.doi.org/10.1155/2016/2401657
collection DOAJ
language English
format Article
sources DOAJ
author Takeshi Nomura
Masahiro Sokabe
Kenjiro Yoshimura
spellingShingle Takeshi Nomura
Masahiro Sokabe
Kenjiro Yoshimura
Voltage-Dependent Inactivation of MscS Occurs Independently of the Positively Charged Residues in the Transmembrane Domain
BioMed Research International
author_facet Takeshi Nomura
Masahiro Sokabe
Kenjiro Yoshimura
author_sort Takeshi Nomura
title Voltage-Dependent Inactivation of MscS Occurs Independently of the Positively Charged Residues in the Transmembrane Domain
title_short Voltage-Dependent Inactivation of MscS Occurs Independently of the Positively Charged Residues in the Transmembrane Domain
title_full Voltage-Dependent Inactivation of MscS Occurs Independently of the Positively Charged Residues in the Transmembrane Domain
title_fullStr Voltage-Dependent Inactivation of MscS Occurs Independently of the Positively Charged Residues in the Transmembrane Domain
title_full_unstemmed Voltage-Dependent Inactivation of MscS Occurs Independently of the Positively Charged Residues in the Transmembrane Domain
title_sort voltage-dependent inactivation of mscs occurs independently of the positively charged residues in the transmembrane domain
publisher Hindawi Limited
series BioMed Research International
issn 2314-6133
2314-6141
publishDate 2016-01-01
description MscS (mechanosensitive channel of small conductance) is ubiquitously found among bacteria and plays a major role in avoiding cell lysis upon rapid osmotic downshock. The gating of MscS is modulated by voltage, but little is known about how MscS senses membrane potential. Three arginine residues (Arg-46, Arg-54, and Arg-74) in the transmembrane (TM) domain are possible to respond to voltage judging from the MscS structure. To examine whether these residues are involved in the voltage dependence of MscS, we neutralized the charge of each residue by substituting with asparagine (R46N, R54N, and R74N). Mechanical threshold for the opening of the expressed wild-type MscS and asparagine mutants did not change with voltage in the range from -40 to +100 mV. By contrast, inactivation process of wild-type MscS was strongly affected by voltage. The wild-type MscS inactivated at +60 to +80 mV but not at -60 to +40 mV. The voltage dependence of the inactivation rate of all mutants tested, that is, R46N, R54N, R74N, and R46N/R74N MscS, was almost indistinguishable from that of the wild-type MscS. These findings indicate that the voltage dependence of the inactivation occurs independently of the positive charges of R46, R54, and R74.
url http://dx.doi.org/10.1155/2016/2401657
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