Toxin acidic residue evolutionary function-guided design of de novo peptide drugs for the immunotherapeutic target, the Kv1.3 channel

During the long-term evolution of animal toxins acting on potassium channels, the acidic residues can orientate the toxin binding interfaces by adjusting the molecular polarity. Based on the evolutionary function of toxin acidic residues, de novo peptide drugs with distinct binding interfaces were d...

Descripción completa

Detalles Bibliográficos
Autores principales: Chen, Zongyun, Hu, Youtian, Hong, Jing, Hu, Jun, Yang, Weishan, Xiang, Fang, Yang, Fan, Xie, Zili, Cao, Zhijian, Li, Wenxin, Lin, Donghai, Wu, Yingliang
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group 2015
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4424837/
https://www.ncbi.nlm.nih.gov/pubmed/25955787
http://dx.doi.org/10.1038/srep09881
_version_ 1782370386575360000
author Chen, Zongyun
Hu, Youtian
Hong, Jing
Hu, Jun
Yang, Weishan
Xiang, Fang
Yang, Fan
Xie, Zili
Cao, Zhijian
Li, Wenxin
Lin, Donghai
Wu, Yingliang
author_facet Chen, Zongyun
Hu, Youtian
Hong, Jing
Hu, Jun
Yang, Weishan
Xiang, Fang
Yang, Fan
Xie, Zili
Cao, Zhijian
Li, Wenxin
Lin, Donghai
Wu, Yingliang
author_sort Chen, Zongyun
collection PubMed
description During the long-term evolution of animal toxins acting on potassium channels, the acidic residues can orientate the toxin binding interfaces by adjusting the molecular polarity. Based on the evolutionary function of toxin acidic residues, de novo peptide drugs with distinct binding interfaces were designed for the immunotherapeutic target, the Kv1.3 channel. Using a natural basic toxin, BmKTX, as a template, which contains 2 acidic residues (Asp19 and Asp33), we engineered two new peptides BmKTX-19 with 1 acidic residue (Asp33), and BmKTX-196 with 2 acidic residues (Asp6 and Asp33) through only adjusting acidic residue distribution for reorientation of BmKTX binding interface. Pharmacological experiments indicated that BmKTX-19 and BmKTX-196 peptides were specific inhibitors of the Kv1.3 channel and effectively suppressed cytokine secretion. In addition to the structural similarity between the designed and native peptides, both experimental alanine-scanning mutagenesis and computational simulation further indicated that the binding interface of wild-type BmKTX was successfully reoriented in BmKTX-19 and BmKTX-196, which adopted distinct toxin surfaces as binding interfaces. Together, these findings indicate not only the promising prospect of BmKTX-19 and BmKTX-196 as drug candidates but also the desirable feasibility of the evolution-guided peptide drug design for discovering numerous peptide drugs for the Kv1.3 channel.
format Online
Article
Text
id pubmed-4424837
institution National Center for Biotechnology Information
language English
publishDate 2015
publisher Nature Publishing Group
record_format MEDLINE/PubMed
spelling pubmed-44248372015-05-13 Toxin acidic residue evolutionary function-guided design of de novo peptide drugs for the immunotherapeutic target, the Kv1.3 channel Chen, Zongyun Hu, Youtian Hong, Jing Hu, Jun Yang, Weishan Xiang, Fang Yang, Fan Xie, Zili Cao, Zhijian Li, Wenxin Lin, Donghai Wu, Yingliang Sci Rep Article During the long-term evolution of animal toxins acting on potassium channels, the acidic residues can orientate the toxin binding interfaces by adjusting the molecular polarity. Based on the evolutionary function of toxin acidic residues, de novo peptide drugs with distinct binding interfaces were designed for the immunotherapeutic target, the Kv1.3 channel. Using a natural basic toxin, BmKTX, as a template, which contains 2 acidic residues (Asp19 and Asp33), we engineered two new peptides BmKTX-19 with 1 acidic residue (Asp33), and BmKTX-196 with 2 acidic residues (Asp6 and Asp33) through only adjusting acidic residue distribution for reorientation of BmKTX binding interface. Pharmacological experiments indicated that BmKTX-19 and BmKTX-196 peptides were specific inhibitors of the Kv1.3 channel and effectively suppressed cytokine secretion. In addition to the structural similarity between the designed and native peptides, both experimental alanine-scanning mutagenesis and computational simulation further indicated that the binding interface of wild-type BmKTX was successfully reoriented in BmKTX-19 and BmKTX-196, which adopted distinct toxin surfaces as binding interfaces. Together, these findings indicate not only the promising prospect of BmKTX-19 and BmKTX-196 as drug candidates but also the desirable feasibility of the evolution-guided peptide drug design for discovering numerous peptide drugs for the Kv1.3 channel. Nature Publishing Group 2015-05-08 /pmc/articles/PMC4424837/ /pubmed/25955787 http://dx.doi.org/10.1038/srep09881 Text en Copyright © 2015, Macmillan Publishers Limited. All rights reserved http://creativecommons.org/licenses/by/4.0/ This work is licensed under a Creative Commons Attribution 4.0 International License. The images or other third party material in this article are included in the article's Creative Commons license, unless indicated otherwise in the credit line; if the material is not included under the Creative Commons license, users will need to obtain permission from the license holder in order to reproduce the material. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/
spellingShingle Article
Chen, Zongyun
Hu, Youtian
Hong, Jing
Hu, Jun
Yang, Weishan
Xiang, Fang
Yang, Fan
Xie, Zili
Cao, Zhijian
Li, Wenxin
Lin, Donghai
Wu, Yingliang
Toxin acidic residue evolutionary function-guided design of de novo peptide drugs for the immunotherapeutic target, the Kv1.3 channel
title Toxin acidic residue evolutionary function-guided design of de novo peptide drugs for the immunotherapeutic target, the Kv1.3 channel
title_full Toxin acidic residue evolutionary function-guided design of de novo peptide drugs for the immunotherapeutic target, the Kv1.3 channel
title_fullStr Toxin acidic residue evolutionary function-guided design of de novo peptide drugs for the immunotherapeutic target, the Kv1.3 channel
title_full_unstemmed Toxin acidic residue evolutionary function-guided design of de novo peptide drugs for the immunotherapeutic target, the Kv1.3 channel
title_short Toxin acidic residue evolutionary function-guided design of de novo peptide drugs for the immunotherapeutic target, the Kv1.3 channel
title_sort toxin acidic residue evolutionary function-guided design of de novo peptide drugs for the immunotherapeutic target, the kv1.3 channel
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4424837/
https://www.ncbi.nlm.nih.gov/pubmed/25955787
http://dx.doi.org/10.1038/srep09881
work_keys_str_mv AT chenzongyun toxinacidicresidueevolutionaryfunctionguideddesignofdenovopeptidedrugsfortheimmunotherapeutictargetthekv13channel
AT huyoutian toxinacidicresidueevolutionaryfunctionguideddesignofdenovopeptidedrugsfortheimmunotherapeutictargetthekv13channel
AT hongjing toxinacidicresidueevolutionaryfunctionguideddesignofdenovopeptidedrugsfortheimmunotherapeutictargetthekv13channel
AT hujun toxinacidicresidueevolutionaryfunctionguideddesignofdenovopeptidedrugsfortheimmunotherapeutictargetthekv13channel
AT yangweishan toxinacidicresidueevolutionaryfunctionguideddesignofdenovopeptidedrugsfortheimmunotherapeutictargetthekv13channel
AT xiangfang toxinacidicresidueevolutionaryfunctionguideddesignofdenovopeptidedrugsfortheimmunotherapeutictargetthekv13channel
AT yangfan toxinacidicresidueevolutionaryfunctionguideddesignofdenovopeptidedrugsfortheimmunotherapeutictargetthekv13channel
AT xiezili toxinacidicresidueevolutionaryfunctionguideddesignofdenovopeptidedrugsfortheimmunotherapeutictargetthekv13channel
AT caozhijian toxinacidicresidueevolutionaryfunctionguideddesignofdenovopeptidedrugsfortheimmunotherapeutictargetthekv13channel
AT liwenxin toxinacidicresidueevolutionaryfunctionguideddesignofdenovopeptidedrugsfortheimmunotherapeutictargetthekv13channel
AT lindonghai toxinacidicresidueevolutionaryfunctionguideddesignofdenovopeptidedrugsfortheimmunotherapeutictargetthekv13channel
AT wuyingliang toxinacidicresidueevolutionaryfunctionguideddesignofdenovopeptidedrugsfortheimmunotherapeutictargetthekv13channel

Ejemplares similares