Vectorial Proton Transport Mechanism of RxR, a Phylogenetically Distinct and Thermally Stable Microbial Rhodopsin

Keiichi Kojima; Tetsuya Ueta; Tomoyasu Noji; Keisuke Saito; Kanae Kanehara; Susumu Yoshizawa; Hiroshi Ishikita; Yuki Sudo

doi:10.1038/s41598-019-57122-2

Vectorial Proton Transport Mechanism of RxR, a Phylogenetically Distinct and Thermally Stable Microbial Rhodopsin

Keiichi Kojima, Tetsuya Ueta, Tomoyasu Noji, Keisuke Saito, Kanae Kanehara, Susumu Yoshizawa, Hiroshi Ishikita, Yuki Sudo

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Abstract

Rubrobacter xylanophilus rhodopsin (RxR) is a phylogenetically distinct and thermally stable seven-transmembrane protein that functions as a light-driven proton (H⁺) pump with the chromophore retinal. To characterize its vectorial proton transport mechanism, mutational and theoretical investigations were performed for carboxylates in the transmembrane region of RxR and the sequential proton transport steps were revealed as follows: (i) a proton of the retinylidene Schiff base (Lys209) is transferred to the counterion Asp74 upon formation of the blue-shifted M-intermediate in collaboration with Asp205, and simultaneously, a respective proton is released from the proton releasing group (Glu187/Glu197) to the extracellular side, (ii) a proton of Asp85 is transferred to the Schiff base during M-decay, (iii) a proton is taken up from the intracellular side to Asp85 during decay of the red-shifted O-intermediate. This ion transport mechanism of RxR provides valuable information to understand other ion transporters since carboxylates are generally essential for their functions.

Original language	English
Article number	282
Journal	Scientific reports
Volume	10
Issue number	1
DOIs	https://doi.org/10.1038/s41598-019-57122-2
Publication status	Published - Dec 1 2020

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@article{7590a20d7fe24e4c9125ba6e43b4624d,

title = "Vectorial Proton Transport Mechanism of RxR, a Phylogenetically Distinct and Thermally Stable Microbial Rhodopsin",

abstract = "Rubrobacter xylanophilus rhodopsin (RxR) is a phylogenetically distinct and thermally stable seven-transmembrane protein that functions as a light-driven proton (H+) pump with the chromophore retinal. To characterize its vectorial proton transport mechanism, mutational and theoretical investigations were performed for carboxylates in the transmembrane region of RxR and the sequential proton transport steps were revealed as follows: (i) a proton of the retinylidene Schiff base (Lys209) is transferred to the counterion Asp74 upon formation of the blue-shifted M-intermediate in collaboration with Asp205, and simultaneously, a respective proton is released from the proton releasing group (Glu187/Glu197) to the extracellular side, (ii) a proton of Asp85 is transferred to the Schiff base during M-decay, (iii) a proton is taken up from the intracellular side to Asp85 during decay of the red-shifted O-intermediate. This ion transport mechanism of RxR provides valuable information to understand other ion transporters since carboxylates are generally essential for their functions.",

author = "Keiichi Kojima and Tetsuya Ueta and Tomoyasu Noji and Keisuke Saito and Kanae Kanehara and Susumu Yoshizawa and Hiroshi Ishikita and Yuki Sudo",

note = "Funding Information: We thank Prof. Takeshi Murata for supplying structural information of RxR (AMED; JP18am0101083). This work was financially supported by JSPS KAKENHI Grant Numbers JP19K16090 to K. Kojima., JP17K18013 to T.N., JP18H01186 and JP16H06560 to K.S., JP26105012 and JP18H05155 to H.I., and JP15H04363, JP15H00878, JP25104005 and JP17H05726 to YS. This research was partially supported by CREST-JST (JPMJCR1656 to H.I. and Y.S.) and AMED (18ak0101084h0002 to H.I. and 18dm0207060h0002 to Y.S.). This research was also supported by the Interdisciplinary Computational Science Program in CCS, University of Tsukuba. Publisher Copyright: {\textcopyright} 2020, The Author(s).",

year = "2020",

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doi = "10.1038/s41598-019-57122-2",

language = "English",

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T1 - Vectorial Proton Transport Mechanism of RxR, a Phylogenetically Distinct and Thermally Stable Microbial Rhodopsin

AU - Kojima, Keiichi

AU - Ueta, Tetsuya

AU - Noji, Tomoyasu

AU - Saito, Keisuke

AU - Kanehara, Kanae

AU - Yoshizawa, Susumu

AU - Ishikita, Hiroshi

AU - Sudo, Yuki

N1 - Funding Information: We thank Prof. Takeshi Murata for supplying structural information of RxR (AMED; JP18am0101083). This work was financially supported by JSPS KAKENHI Grant Numbers JP19K16090 to K. Kojima., JP17K18013 to T.N., JP18H01186 and JP16H06560 to K.S., JP26105012 and JP18H05155 to H.I., and JP15H04363, JP15H00878, JP25104005 and JP17H05726 to YS. This research was partially supported by CREST-JST (JPMJCR1656 to H.I. and Y.S.) and AMED (18ak0101084h0002 to H.I. and 18dm0207060h0002 to Y.S.). This research was also supported by the Interdisciplinary Computational Science Program in CCS, University of Tsukuba. Publisher Copyright: © 2020, The Author(s).

PY - 2020/12/1

Y1 - 2020/12/1

N2 - Rubrobacter xylanophilus rhodopsin (RxR) is a phylogenetically distinct and thermally stable seven-transmembrane protein that functions as a light-driven proton (H+) pump with the chromophore retinal. To characterize its vectorial proton transport mechanism, mutational and theoretical investigations were performed for carboxylates in the transmembrane region of RxR and the sequential proton transport steps were revealed as follows: (i) a proton of the retinylidene Schiff base (Lys209) is transferred to the counterion Asp74 upon formation of the blue-shifted M-intermediate in collaboration with Asp205, and simultaneously, a respective proton is released from the proton releasing group (Glu187/Glu197) to the extracellular side, (ii) a proton of Asp85 is transferred to the Schiff base during M-decay, (iii) a proton is taken up from the intracellular side to Asp85 during decay of the red-shifted O-intermediate. This ion transport mechanism of RxR provides valuable information to understand other ion transporters since carboxylates are generally essential for their functions.

AB - Rubrobacter xylanophilus rhodopsin (RxR) is a phylogenetically distinct and thermally stable seven-transmembrane protein that functions as a light-driven proton (H+) pump with the chromophore retinal. To characterize its vectorial proton transport mechanism, mutational and theoretical investigations were performed for carboxylates in the transmembrane region of RxR and the sequential proton transport steps were revealed as follows: (i) a proton of the retinylidene Schiff base (Lys209) is transferred to the counterion Asp74 upon formation of the blue-shifted M-intermediate in collaboration with Asp205, and simultaneously, a respective proton is released from the proton releasing group (Glu187/Glu197) to the extracellular side, (ii) a proton of Asp85 is transferred to the Schiff base during M-decay, (iii) a proton is taken up from the intracellular side to Asp85 during decay of the red-shifted O-intermediate. This ion transport mechanism of RxR provides valuable information to understand other ion transporters since carboxylates are generally essential for their functions.

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U2 - 10.1038/s41598-019-57122-2

DO - 10.1038/s41598-019-57122-2

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AN - SCOPUS:85077843339

SN - 2045-2322

VL - 10

JO - Scientific reports

JF - Scientific reports

IS - 1

M1 - 282

ER -

Vectorial Proton Transport Mechanism of RxR, a Phylogenetically Distinct and Thermally Stable Microbial Rhodopsin

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