Downregulation of MCT4 for lactate exchange promotes the cytotoxicity of NK cells in breast carcinoma
Abstract Monocarboxylate transporter‐4 (MCT4), a monocarboxylic acid transporter, demonstrates significantly increased expression in the majority of malignancies. We performed an experiment using BALB/C mice, and our results showed that ShMCT4 transfection or the pharmaceutic inhibition of MCT4 with...
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doaj-7109586e26c64ca9a106413ca37a7ac52020-11-25T03:16:36ZengWileyCancer Medicine2045-76342018-09-01794690470010.1002/cam4.1713Downregulation of MCT4 for lactate exchange promotes the cytotoxicity of NK cells in breast carcinomaYaping Long0Zihe Gao1Xiao Hu2Feng Xiang3Zhaozhen Wu4Jiahui Zhang5Xiao Han6Liyong Yin7Junfang Qin8Lan Lan9Fuzai Yin10Yue Wang11School of Medicine Nankai University Tianjin ChinaSchool of Medicine Nankai University Tianjin ChinaSchool of Medicine Nankai University Tianjin ChinaSchool of Medicine Nankai University Tianjin ChinaSchool of Medicine Nankai University Tianjin ChinaSchool of Medicine Nankai University Tianjin ChinaSchool of Medicine Nankai University Tianjin ChinaFirst Hospital of Qinhuangdao Qinhuangdao Hebei ChinaSchool of Medicine Nankai University Tianjin ChinaTianjin Cancer Hospital Tianjin Medical University Tianjin ChinaFirst Hospital of Qinhuangdao Qinhuangdao Hebei ChinaSchool of Medicine Nankai University Tianjin ChinaAbstract Monocarboxylate transporter‐4 (MCT4), a monocarboxylic acid transporter, demonstrates significantly increased expression in the majority of malignancies. We performed an experiment using BALB/C mice, and our results showed that ShMCT4 transfection or the pharmaceutic inhibition of MCT4 with 7acc1 strengthens the activity of NK cells. The results of a calcein assay revealed that the cytotoxicity of NK cells was strengthened via inhibition of MCT4. In addition, ELISA testing showed that the content of perforin and CD107a was increased, and PCR amplification and immunoblotting revealed that the expression of NKG2D and H60 was upregulated after the inhibition of MCT4. Further, we observed an elevated pH value, decreased extracellular lactate flow, and attenuated tumor growth. Therefore, we concluded that the inhibition of MCT4 enhanced the cytotoxicity of NK cells by blocking lactate flux and reversing the acidified tumor microenvironment. In addition to these findings, we also discovered that MCT4 depletion may have a pronounced impact on autophagy, which was surmised by observing that the inhibition of autophagy (3MA) pulled the enhanced cytotoxicity of NK cells downwards. Together, these data suggest that the key effect of MCT4 depletion on NK cells probably utilizes inductive autophagy as a compensatory metabolic mechanism to minimize the acidic extracellular microenvironment associated with lactate export in tumors.https://doi.org/10.1002/cam4.1713lactateMCT4NK cytotoxicityNKG2DNKG2DLs (H60) |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Yaping Long Zihe Gao Xiao Hu Feng Xiang Zhaozhen Wu Jiahui Zhang Xiao Han Liyong Yin Junfang Qin Lan Lan Fuzai Yin Yue Wang |
spellingShingle |
Yaping Long Zihe Gao Xiao Hu Feng Xiang Zhaozhen Wu Jiahui Zhang Xiao Han Liyong Yin Junfang Qin Lan Lan Fuzai Yin Yue Wang Downregulation of MCT4 for lactate exchange promotes the cytotoxicity of NK cells in breast carcinoma Cancer Medicine lactate MCT4 NK cytotoxicity NKG2D NKG2DLs (H60) |
author_facet |
Yaping Long Zihe Gao Xiao Hu Feng Xiang Zhaozhen Wu Jiahui Zhang Xiao Han Liyong Yin Junfang Qin Lan Lan Fuzai Yin Yue Wang |
author_sort |
Yaping Long |
title |
Downregulation of MCT4 for lactate exchange promotes the cytotoxicity of NK cells in breast carcinoma |
title_short |
Downregulation of MCT4 for lactate exchange promotes the cytotoxicity of NK cells in breast carcinoma |
title_full |
Downregulation of MCT4 for lactate exchange promotes the cytotoxicity of NK cells in breast carcinoma |
title_fullStr |
Downregulation of MCT4 for lactate exchange promotes the cytotoxicity of NK cells in breast carcinoma |
title_full_unstemmed |
Downregulation of MCT4 for lactate exchange promotes the cytotoxicity of NK cells in breast carcinoma |
title_sort |
downregulation of mct4 for lactate exchange promotes the cytotoxicity of nk cells in breast carcinoma |
publisher |
Wiley |
series |
Cancer Medicine |
issn |
2045-7634 |
publishDate |
2018-09-01 |
description |
Abstract Monocarboxylate transporter‐4 (MCT4), a monocarboxylic acid transporter, demonstrates significantly increased expression in the majority of malignancies. We performed an experiment using BALB/C mice, and our results showed that ShMCT4 transfection or the pharmaceutic inhibition of MCT4 with 7acc1 strengthens the activity of NK cells. The results of a calcein assay revealed that the cytotoxicity of NK cells was strengthened via inhibition of MCT4. In addition, ELISA testing showed that the content of perforin and CD107a was increased, and PCR amplification and immunoblotting revealed that the expression of NKG2D and H60 was upregulated after the inhibition of MCT4. Further, we observed an elevated pH value, decreased extracellular lactate flow, and attenuated tumor growth. Therefore, we concluded that the inhibition of MCT4 enhanced the cytotoxicity of NK cells by blocking lactate flux and reversing the acidified tumor microenvironment. In addition to these findings, we also discovered that MCT4 depletion may have a pronounced impact on autophagy, which was surmised by observing that the inhibition of autophagy (3MA) pulled the enhanced cytotoxicity of NK cells downwards. Together, these data suggest that the key effect of MCT4 depletion on NK cells probably utilizes inductive autophagy as a compensatory metabolic mechanism to minimize the acidic extracellular microenvironment associated with lactate export in tumors. |
topic |
lactate MCT4 NK cytotoxicity NKG2D NKG2DLs (H60) |
url |
https://doi.org/10.1002/cam4.1713 |
work_keys_str_mv |
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1724635238212042752 |