Lovastatin blocks Kv1.3 channel in human T cells: a new mechanism to explain its immunomodulatory properties

Lovastatin is a member of Statins, which are beneficial in a lot of immunologic cardiovascular diseases and T cell-mediated autoimmune diseases. Kv1.3 channel plays important roles in the activation and proliferation of T cells, and have become attractive target for immune-related disorders. The pre...

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Autores principales: Zhao, Ning, Dong, Qian, Qian, Cheng, Li, Sen, Wu, Qiong-Feng, Ding, Dan, Li, Jing, Wang, Bin-Bin, Guo, Ke-fang, Xie, Jiang-jiao, Cheng, Xiang, Liao, Yu-Hua, Du, Yi-Mei
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group 2015
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4663632/
https://www.ncbi.nlm.nih.gov/pubmed/26616555
http://dx.doi.org/10.1038/srep17381
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author Zhao, Ning
Dong, Qian
Qian, Cheng
Li, Sen
Wu, Qiong-Feng
Ding, Dan
Li, Jing
Wang, Bin-Bin
Guo, Ke-fang
Xie, Jiang-jiao
Cheng, Xiang
Liao, Yu-Hua
Du, Yi-Mei
author_facet Zhao, Ning
Dong, Qian
Qian, Cheng
Li, Sen
Wu, Qiong-Feng
Ding, Dan
Li, Jing
Wang, Bin-Bin
Guo, Ke-fang
Xie, Jiang-jiao
Cheng, Xiang
Liao, Yu-Hua
Du, Yi-Mei
author_sort Zhao, Ning
collection PubMed
description Lovastatin is a member of Statins, which are beneficial in a lot of immunologic cardiovascular diseases and T cell-mediated autoimmune diseases. Kv1.3 channel plays important roles in the activation and proliferation of T cells, and have become attractive target for immune-related disorders. The present study was designed to examine the block effect of Lovastatin on Kv1.3 channel in human T cells, and to clarify its new immunomodulatory mechanism. We found that Lovastatin inhibited Kv1.3 currents in a concentration- and voltage-dependent manner, and the IC50 for peak, end of the pulse was 39.81 ± 5.11, 6.92 ± 0.95 μM, respectively. Lovastatin also accelerated the decay rate of current inactivation and negatively shifted the steady-state inactivation curves concentration-dependently, without affecting the activation curve. However, 30 μM Lovastatin had no apparent effect on K(Ca) current in human T cells. Furthermore, Lovastatin inhibited Ca(2+) influx, T cell proliferation as well as IL-2 production. The activities of NFAT1 and NF-κB p65/50 were down-regulated by Lovastatin, too. At last, Mevalonate application only partially reversed the inhibition of Lovastatin on IL-2 secretion, and the siRNA against Kv1.3 also partially reduced this inhibitory effect of Lovastatin. In conclusion, Lovastatin can exert immunodulatory properties through the new mechanism of blocking Kv1.3 channel.
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spelling pubmed-46636322015-12-03 Lovastatin blocks Kv1.3 channel in human T cells: a new mechanism to explain its immunomodulatory properties Zhao, Ning Dong, Qian Qian, Cheng Li, Sen Wu, Qiong-Feng Ding, Dan Li, Jing Wang, Bin-Bin Guo, Ke-fang Xie, Jiang-jiao Cheng, Xiang Liao, Yu-Hua Du, Yi-Mei Sci Rep Article Lovastatin is a member of Statins, which are beneficial in a lot of immunologic cardiovascular diseases and T cell-mediated autoimmune diseases. Kv1.3 channel plays important roles in the activation and proliferation of T cells, and have become attractive target for immune-related disorders. The present study was designed to examine the block effect of Lovastatin on Kv1.3 channel in human T cells, and to clarify its new immunomodulatory mechanism. We found that Lovastatin inhibited Kv1.3 currents in a concentration- and voltage-dependent manner, and the IC50 for peak, end of the pulse was 39.81 ± 5.11, 6.92 ± 0.95 μM, respectively. Lovastatin also accelerated the decay rate of current inactivation and negatively shifted the steady-state inactivation curves concentration-dependently, without affecting the activation curve. However, 30 μM Lovastatin had no apparent effect on K(Ca) current in human T cells. Furthermore, Lovastatin inhibited Ca(2+) influx, T cell proliferation as well as IL-2 production. The activities of NFAT1 and NF-κB p65/50 were down-regulated by Lovastatin, too. At last, Mevalonate application only partially reversed the inhibition of Lovastatin on IL-2 secretion, and the siRNA against Kv1.3 also partially reduced this inhibitory effect of Lovastatin. In conclusion, Lovastatin can exert immunodulatory properties through the new mechanism of blocking Kv1.3 channel. Nature Publishing Group 2015-11-30 /pmc/articles/PMC4663632/ /pubmed/26616555 http://dx.doi.org/10.1038/srep17381 Text en Copyright © 2015, Macmillan Publishers Limited 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 to reproduce the material. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/
spellingShingle Article
Zhao, Ning
Dong, Qian
Qian, Cheng
Li, Sen
Wu, Qiong-Feng
Ding, Dan
Li, Jing
Wang, Bin-Bin
Guo, Ke-fang
Xie, Jiang-jiao
Cheng, Xiang
Liao, Yu-Hua
Du, Yi-Mei
Lovastatin blocks Kv1.3 channel in human T cells: a new mechanism to explain its immunomodulatory properties
title Lovastatin blocks Kv1.3 channel in human T cells: a new mechanism to explain its immunomodulatory properties
title_full Lovastatin blocks Kv1.3 channel in human T cells: a new mechanism to explain its immunomodulatory properties
title_fullStr Lovastatin blocks Kv1.3 channel in human T cells: a new mechanism to explain its immunomodulatory properties
title_full_unstemmed Lovastatin blocks Kv1.3 channel in human T cells: a new mechanism to explain its immunomodulatory properties
title_short Lovastatin blocks Kv1.3 channel in human T cells: a new mechanism to explain its immunomodulatory properties
title_sort lovastatin blocks kv1.3 channel in human t cells: a new mechanism to explain its immunomodulatory properties
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4663632/
https://www.ncbi.nlm.nih.gov/pubmed/26616555
http://dx.doi.org/10.1038/srep17381
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