Structural and Functional Diversity of Acidic Scorpion Potassium Channel Toxins

BACKGROUND: Although the basic scorpion K(+) channel toxins (KTxs) are well-known pharmacological tools and potential drug candidates, characterization the acidic KTxs still has the great significance for their potential selectivity towards different K(+) channel subtypes. Unfortunately, research on...

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Autores principales: Chen, Zong-Yun, Zeng, Dan-Yun, Hu, You-Tian, He, Ya-Wen, Pan, Na, Ding, Jiu-Ping, Cao, Zhi-Jian, Liu, Mai-Li, Li, Wen-Xin, Yi, Hong, Jiang, Ling, Wu, Ying-Liang
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3325286/
https://www.ncbi.nlm.nih.gov/pubmed/22511981
http://dx.doi.org/10.1371/journal.pone.0035154
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author Chen, Zong-Yun
Zeng, Dan-Yun
Hu, You-Tian
He, Ya-Wen
Pan, Na
Ding, Jiu-Ping
Cao, Zhi-Jian
Liu, Mai-Li
Li, Wen-Xin
Yi, Hong
Jiang, Ling
Wu, Ying-Liang
author_facet Chen, Zong-Yun
Zeng, Dan-Yun
Hu, You-Tian
He, Ya-Wen
Pan, Na
Ding, Jiu-Ping
Cao, Zhi-Jian
Liu, Mai-Li
Li, Wen-Xin
Yi, Hong
Jiang, Ling
Wu, Ying-Liang
author_sort Chen, Zong-Yun
collection PubMed
description BACKGROUND: Although the basic scorpion K(+) channel toxins (KTxs) are well-known pharmacological tools and potential drug candidates, characterization the acidic KTxs still has the great significance for their potential selectivity towards different K(+) channel subtypes. Unfortunately, research on the acidic KTxs has been ignored for several years and progressed slowly. PRINCIPAL FINDINGS: Here, we describe the identification of nine new acidic KTxs by cDNA cloning and bioinformatic analyses. Seven of these toxins belong to three new α-KTx subfamilies (α-KTx28, α-KTx29, and α-KTx30), and two are new members of the known κ-KTx2 subfamily. ImKTx104 containing three disulfide bridges, the first member of the α-KTx28 subfamily, has a low sequence homology with other known KTxs, and its NMR structure suggests ImKTx104 adopts a modified cystine-stabilized α-helix-loop-β-sheet (CS-α/β) fold motif that has no apparent α-helixs and β-sheets, but still stabilized by three disulfide bridges. These newly described acidic KTxs exhibit differential pharmacological effects on potassium channels. Acidic scorpion toxin ImKTx104 was the first peptide inhibitor found to affect KCNQ1 channel, which is insensitive to the basic KTxs and is strongly associated with human cardiac abnormalities. ImKTx104 selectively inhibited KCNQ1 channel with a K(d) of 11.69 µM, but was less effective against the basic KTxs-sensitive potassium channels. In addition to the ImKTx104 toxin, HeTx204 peptide, containing a cystine-stabilized α-helix-loop-helix (CS-α/α) fold scaffold motif, blocked both Kv1.3 and KCNQ1 channels. StKTx23 toxin, with a cystine-stabilized α-helix-loop-β-sheet (CS-α/β) fold motif, could inhibit Kv1.3 channel, but not the KCNQ1 channel. CONCLUSIONS/SIGNIFICANCE: These findings characterize the structural and functional diversity of acidic KTxs, and could accelerate the development and clinical use of acidic KTxs as pharmacological tools and potential drugs.
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spelling pubmed-33252862012-04-17 Structural and Functional Diversity of Acidic Scorpion Potassium Channel Toxins Chen, Zong-Yun Zeng, Dan-Yun Hu, You-Tian He, Ya-Wen Pan, Na Ding, Jiu-Ping Cao, Zhi-Jian Liu, Mai-Li Li, Wen-Xin Yi, Hong Jiang, Ling Wu, Ying-Liang PLoS One Research Article BACKGROUND: Although the basic scorpion K(+) channel toxins (KTxs) are well-known pharmacological tools and potential drug candidates, characterization the acidic KTxs still has the great significance for their potential selectivity towards different K(+) channel subtypes. Unfortunately, research on the acidic KTxs has been ignored for several years and progressed slowly. PRINCIPAL FINDINGS: Here, we describe the identification of nine new acidic KTxs by cDNA cloning and bioinformatic analyses. Seven of these toxins belong to three new α-KTx subfamilies (α-KTx28, α-KTx29, and α-KTx30), and two are new members of the known κ-KTx2 subfamily. ImKTx104 containing three disulfide bridges, the first member of the α-KTx28 subfamily, has a low sequence homology with other known KTxs, and its NMR structure suggests ImKTx104 adopts a modified cystine-stabilized α-helix-loop-β-sheet (CS-α/β) fold motif that has no apparent α-helixs and β-sheets, but still stabilized by three disulfide bridges. These newly described acidic KTxs exhibit differential pharmacological effects on potassium channels. Acidic scorpion toxin ImKTx104 was the first peptide inhibitor found to affect KCNQ1 channel, which is insensitive to the basic KTxs and is strongly associated with human cardiac abnormalities. ImKTx104 selectively inhibited KCNQ1 channel with a K(d) of 11.69 µM, but was less effective against the basic KTxs-sensitive potassium channels. In addition to the ImKTx104 toxin, HeTx204 peptide, containing a cystine-stabilized α-helix-loop-helix (CS-α/α) fold scaffold motif, blocked both Kv1.3 and KCNQ1 channels. StKTx23 toxin, with a cystine-stabilized α-helix-loop-β-sheet (CS-α/β) fold motif, could inhibit Kv1.3 channel, but not the KCNQ1 channel. CONCLUSIONS/SIGNIFICANCE: These findings characterize the structural and functional diversity of acidic KTxs, and could accelerate the development and clinical use of acidic KTxs as pharmacological tools and potential drugs. Public Library of Science 2012-04-12 /pmc/articles/PMC3325286/ /pubmed/22511981 http://dx.doi.org/10.1371/journal.pone.0035154 Text en Chen et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Chen, Zong-Yun
Zeng, Dan-Yun
Hu, You-Tian
He, Ya-Wen
Pan, Na
Ding, Jiu-Ping
Cao, Zhi-Jian
Liu, Mai-Li
Li, Wen-Xin
Yi, Hong
Jiang, Ling
Wu, Ying-Liang
Structural and Functional Diversity of Acidic Scorpion Potassium Channel Toxins
title Structural and Functional Diversity of Acidic Scorpion Potassium Channel Toxins
title_full Structural and Functional Diversity of Acidic Scorpion Potassium Channel Toxins
title_fullStr Structural and Functional Diversity of Acidic Scorpion Potassium Channel Toxins
title_full_unstemmed Structural and Functional Diversity of Acidic Scorpion Potassium Channel Toxins
title_short Structural and Functional Diversity of Acidic Scorpion Potassium Channel Toxins
title_sort structural and functional diversity of acidic scorpion potassium channel toxins
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3325286/
https://www.ncbi.nlm.nih.gov/pubmed/22511981
http://dx.doi.org/10.1371/journal.pone.0035154
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