Protein Sensing Device with Multi-Recognition Ability Composed of Self-Organized Glycopeptide Bundle

Protein Sensing Device with Multi-Recognition Ability Composed of Self-Organized Glycopeptide Bundle

We designed and synthesized amphiphilic glycopeptides with glucose or galactose at the <i>C</i>-terminals. We observed the protein-induced structural changes of the amphiphilic glycopeptide assembly in the lipid bilayer membrane using transmission electron microscopy (TEM) and Fourier tr...

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Main Authors: Mao Arai, Tomohiro Miura, Yuriko Ito, Takatoshi Kinoshita, Masahiro Higuchi
Format: Article
Language:English
Published: MDPI AG 2021-12-01
Series:International Journal of Molecular Sciences
Subjects:
sensing device
multi-recognition ability
protein-induced self-organization
amphiphilic glycopeptides
ion channel
Online Access:https://www.mdpi.com/1422-0067/22/1/366
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spelling doaj-d05722c876904a568ade298613d2c1672021-01-01T00:04:52ZengMDPI AGInternational Journal of Molecular Sciences1661-65961422-00672021-12-012236636610.3390/ijms22010366Protein Sensing Device with Multi-Recognition Ability Composed of Self-Organized Glycopeptide BundleMao Arai0Tomohiro Miura1Yuriko Ito2Takatoshi Kinoshita3Masahiro Higuchi4Department of Life Science and Applied Chemistry, Graduate School of Engineering, Nagoya Institute of Technology, Gokiso-cho, Show-ku, Nagoya 4668-555, JapanDepartment of Life Science and Applied Chemistry, Graduate School of Engineering, Nagoya Institute of Technology, Gokiso-cho, Show-ku, Nagoya 4668-555, JapanDepartment of Life Science and Applied Chemistry, Graduate School of Engineering, Nagoya Institute of Technology, Gokiso-cho, Show-ku, Nagoya 4668-555, JapanDepartment of Life Science and Applied Chemistry, Graduate School of Engineering, Nagoya Institute of Technology, Gokiso-cho, Show-ku, Nagoya 4668-555, JapanDepartment of Life Science and Applied Chemistry, Graduate School of Engineering, Nagoya Institute of Technology, Gokiso-cho, Show-ku, Nagoya 4668-555, JapanWe designed and synthesized amphiphilic glycopeptides with glucose or galactose at the <i>C</i>-terminals. We observed the protein-induced structural changes of the amphiphilic glycopeptide assembly in the lipid bilayer membrane using transmission electron microscopy (TEM) and Fourier transform infrared reflection-absorption spectra (FTIR-RAS) measurements. The glycopeptides re-arranged to form a bundle that acted as an ion channel due to the interaction among the target protein and the terminal sugar groups of the glycopeptides. The bundle in the lipid bilayer membrane was fixed on a gold-deposited quartz crystal microbalance (QCM) electrode by the membrane fusion method. The protein-induced re-arrangement of the terminal sugar groups formed a binding site that acted as a receptor, and the re-binding of the target protein to the binding site induced the closing of the channel. We monitored the detection of target proteins by the changes of the electrochemical properties of the membrane. The response current of the membrane induced by the target protein recognition was expressed by an equivalent circuit consisting of resistors and capacitors when a triangular voltage was applied. We used peanut lectin (PNA) and concanavalin A (ConA) as target proteins. The sensing membrane induced by PNA shows the specific response to PNA, and the ConA-induced membrane responded selectively to ConA. Furthermore, PNA-induced sensing membranes showed relatively low recognition ability for lectin from Ricinus Agglutinin (RCA120) and mushroom lectin (ABA), which have galactose binding sites. The protein-induced self-organization formed the spatial arrangement of the sugar chains specific to the binding site of the target protein. These findings demonstrate the possibility of fabricating a sensing device with multi-recognition ability that can recognize proteins even if the structure is unknown, by the protein-induced self-organization process.https://www.mdpi.com/1422-0067/22/1/366sensing devicemulti-recognition abilityprotein-induced self-organizationamphiphilic glycopeptidesion channel
collection DOAJ
language English
format Article
sources DOAJ
author Mao Arai
Tomohiro Miura
Yuriko Ito
Takatoshi Kinoshita
Masahiro Higuchi
spellingShingle Mao Arai
Tomohiro Miura
Yuriko Ito
Takatoshi Kinoshita
Masahiro Higuchi
Protein Sensing Device with Multi-Recognition Ability Composed of Self-Organized Glycopeptide Bundle
International Journal of Molecular Sciences
sensing device
multi-recognition ability
protein-induced self-organization
amphiphilic glycopeptides
ion channel
author_facet Mao Arai
Tomohiro Miura
Yuriko Ito
Takatoshi Kinoshita
Masahiro Higuchi
author_sort Mao Arai
title Protein Sensing Device with Multi-Recognition Ability Composed of Self-Organized Glycopeptide Bundle
title_short Protein Sensing Device with Multi-Recognition Ability Composed of Self-Organized Glycopeptide Bundle
title_full Protein Sensing Device with Multi-Recognition Ability Composed of Self-Organized Glycopeptide Bundle
title_fullStr Protein Sensing Device with Multi-Recognition Ability Composed of Self-Organized Glycopeptide Bundle
title_full_unstemmed Protein Sensing Device with Multi-Recognition Ability Composed of Self-Organized Glycopeptide Bundle
title_sort protein sensing device with multi-recognition ability composed of self-organized glycopeptide bundle
publisher MDPI AG
series International Journal of Molecular Sciences
issn 1661-6596
1422-0067
publishDate 2021-12-01
description We designed and synthesized amphiphilic glycopeptides with glucose or galactose at the <i>C</i>-terminals. We observed the protein-induced structural changes of the amphiphilic glycopeptide assembly in the lipid bilayer membrane using transmission electron microscopy (TEM) and Fourier transform infrared reflection-absorption spectra (FTIR-RAS) measurements. The glycopeptides re-arranged to form a bundle that acted as an ion channel due to the interaction among the target protein and the terminal sugar groups of the glycopeptides. The bundle in the lipid bilayer membrane was fixed on a gold-deposited quartz crystal microbalance (QCM) electrode by the membrane fusion method. The protein-induced re-arrangement of the terminal sugar groups formed a binding site that acted as a receptor, and the re-binding of the target protein to the binding site induced the closing of the channel. We monitored the detection of target proteins by the changes of the electrochemical properties of the membrane. The response current of the membrane induced by the target protein recognition was expressed by an equivalent circuit consisting of resistors and capacitors when a triangular voltage was applied. We used peanut lectin (PNA) and concanavalin A (ConA) as target proteins. The sensing membrane induced by PNA shows the specific response to PNA, and the ConA-induced membrane responded selectively to ConA. Furthermore, PNA-induced sensing membranes showed relatively low recognition ability for lectin from Ricinus Agglutinin (RCA120) and mushroom lectin (ABA), which have galactose binding sites. The protein-induced self-organization formed the spatial arrangement of the sugar chains specific to the binding site of the target protein. These findings demonstrate the possibility of fabricating a sensing device with multi-recognition ability that can recognize proteins even if the structure is unknown, by the protein-induced self-organization process.
topic sensing device
multi-recognition ability
protein-induced self-organization
amphiphilic glycopeptides
ion channel
url https://www.mdpi.com/1422-0067/22/1/366
work_keys_str_mv AT maoarai proteinsensingdevicewithmultirecognitionabilitycomposedofselforganizedglycopeptidebundle
AT tomohiromiura proteinsensingdevicewithmultirecognitionabilitycomposedofselforganizedglycopeptidebundle
AT yurikoito proteinsensingdevicewithmultirecognitionabilitycomposedofselforganizedglycopeptidebundle
AT takatoshikinoshita proteinsensingdevicewithmultirecognitionabilitycomposedofselforganizedglycopeptidebundle
AT masahirohiguchi proteinsensingdevicewithmultirecognitionabilitycomposedofselforganizedglycopeptidebundle
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