Pharmacologic Approach to Defective Protein Trafficking in the E637K-hERG Mutant with PD-118057 and Thapsigargin

BACKGROUND: Treatment of LQT2 is inadequate. Many drugs which can pharmacologically rescue defective protein trafficking in LQT2 also result in potent blockade of HERG current, negating their therapeutic benefit. It is reported that PD-118057 and thapsigargin can rescue LQT2 without hERG channel blo...

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Autores principales: Mao, Haiyan, Lu, Xiaoli, Karush, Justin Michael, Huang, Xiaoyan, Yang, Xi, Ba, Yanna, Wang, Ying, Liu, Ningsheng, Zhou, Jianqing, Lian, Jiangfang
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3686757/
https://www.ncbi.nlm.nih.gov/pubmed/23840331
http://dx.doi.org/10.1371/journal.pone.0065481
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author Mao, Haiyan
Lu, Xiaoli
Karush, Justin Michael
Huang, Xiaoyan
Yang, Xi
Ba, Yanna
Wang, Ying
Liu, Ningsheng
Zhou, Jianqing
Lian, Jiangfang
author_facet Mao, Haiyan
Lu, Xiaoli
Karush, Justin Michael
Huang, Xiaoyan
Yang, Xi
Ba, Yanna
Wang, Ying
Liu, Ningsheng
Zhou, Jianqing
Lian, Jiangfang
author_sort Mao, Haiyan
collection PubMed
description BACKGROUND: Treatment of LQT2 is inadequate. Many drugs which can pharmacologically rescue defective protein trafficking in LQT2 also result in potent blockade of HERG current, negating their therapeutic benefit. It is reported that PD-118057 and thapsigargin can rescue LQT2 without hERG channel blockade, but the precise mechanism of action is unknown. Furthermore, the effect of PD-118057 and thapsigargin on the dominant negative E637K-hERG mutant has not been previously investigated. OBJECTIVE: In this study, we investigated: (a) the effect of PD-118057 and thapsigargin on the current amplitudes of WT-hERG and WT/E637K-hERG channels; (b) the effect of PD-118057 and thapsigargin on the biophysical properties of WT-hERG and WT/E637K-hERG channels; (c) whether drug treatment can rescue channel processing and trafficking defects of the WT/E637K-hERG mutant. METHODS: The whole-cell Patch-clamp technique was used to assess the effect of PD-118057 and thapsigargin on the electrophysiological characteristics of the rapidly activating delayed rectifier K(+) current (I(kr)) of the hERG protein channel. Western blot was done to investigate pharmacological rescue on hERG protein channel function. RESULTS: In our study, PD-118057 was shown to significantly enhance both the maximum current amplitude and tail current amplitude, but did not alter the gating and kinetic properties of the WT-hERG channel, with the exception of accelerating steady-state inactivation. Additionally, thapsigargin shows a similar result as PD-118057 for the WT-hERG channel, but with the exception of attenuating steady-state inactivation. However, for the WT/E637K-hERG channel, PD-118057 had no effect on either the current or on the gating and kinetic properties. Furthermore, thapsigargin treatment did not alter the current or the gating and kinetic properties of the WT/E637K-hERG channel, with the exception of opening at more positive voltages. CONCLUSION: Our findings illustrate that neither PD-118057 nor thapsigargin play a role in correcting the dominant-negative effect of the E637K-hERG mutant.
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spelling pubmed-36867572013-07-09 Pharmacologic Approach to Defective Protein Trafficking in the E637K-hERG Mutant with PD-118057 and Thapsigargin Mao, Haiyan Lu, Xiaoli Karush, Justin Michael Huang, Xiaoyan Yang, Xi Ba, Yanna Wang, Ying Liu, Ningsheng Zhou, Jianqing Lian, Jiangfang PLoS One Research Article BACKGROUND: Treatment of LQT2 is inadequate. Many drugs which can pharmacologically rescue defective protein trafficking in LQT2 also result in potent blockade of HERG current, negating their therapeutic benefit. It is reported that PD-118057 and thapsigargin can rescue LQT2 without hERG channel blockade, but the precise mechanism of action is unknown. Furthermore, the effect of PD-118057 and thapsigargin on the dominant negative E637K-hERG mutant has not been previously investigated. OBJECTIVE: In this study, we investigated: (a) the effect of PD-118057 and thapsigargin on the current amplitudes of WT-hERG and WT/E637K-hERG channels; (b) the effect of PD-118057 and thapsigargin on the biophysical properties of WT-hERG and WT/E637K-hERG channels; (c) whether drug treatment can rescue channel processing and trafficking defects of the WT/E637K-hERG mutant. METHODS: The whole-cell Patch-clamp technique was used to assess the effect of PD-118057 and thapsigargin on the electrophysiological characteristics of the rapidly activating delayed rectifier K(+) current (I(kr)) of the hERG protein channel. Western blot was done to investigate pharmacological rescue on hERG protein channel function. RESULTS: In our study, PD-118057 was shown to significantly enhance both the maximum current amplitude and tail current amplitude, but did not alter the gating and kinetic properties of the WT-hERG channel, with the exception of accelerating steady-state inactivation. Additionally, thapsigargin shows a similar result as PD-118057 for the WT-hERG channel, but with the exception of attenuating steady-state inactivation. However, for the WT/E637K-hERG channel, PD-118057 had no effect on either the current or on the gating and kinetic properties. Furthermore, thapsigargin treatment did not alter the current or the gating and kinetic properties of the WT/E637K-hERG channel, with the exception of opening at more positive voltages. CONCLUSION: Our findings illustrate that neither PD-118057 nor thapsigargin play a role in correcting the dominant-negative effect of the E637K-hERG mutant. Public Library of Science 2013-06-19 /pmc/articles/PMC3686757/ /pubmed/23840331 http://dx.doi.org/10.1371/journal.pone.0065481 Text en © 2013 Mao 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
Mao, Haiyan
Lu, Xiaoli
Karush, Justin Michael
Huang, Xiaoyan
Yang, Xi
Ba, Yanna
Wang, Ying
Liu, Ningsheng
Zhou, Jianqing
Lian, Jiangfang
Pharmacologic Approach to Defective Protein Trafficking in the E637K-hERG Mutant with PD-118057 and Thapsigargin
title Pharmacologic Approach to Defective Protein Trafficking in the E637K-hERG Mutant with PD-118057 and Thapsigargin
title_full Pharmacologic Approach to Defective Protein Trafficking in the E637K-hERG Mutant with PD-118057 and Thapsigargin
title_fullStr Pharmacologic Approach to Defective Protein Trafficking in the E637K-hERG Mutant with PD-118057 and Thapsigargin
title_full_unstemmed Pharmacologic Approach to Defective Protein Trafficking in the E637K-hERG Mutant with PD-118057 and Thapsigargin
title_short Pharmacologic Approach to Defective Protein Trafficking in the E637K-hERG Mutant with PD-118057 and Thapsigargin
title_sort pharmacologic approach to defective protein trafficking in the e637k-herg mutant with pd-118057 and thapsigargin
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3686757/
https://www.ncbi.nlm.nih.gov/pubmed/23840331
http://dx.doi.org/10.1371/journal.pone.0065481
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