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Cetrimonium Bromide Inhibits Cell Migration and Invasion of Human Hepatic SK-HEP-1 Cells Through Modulating the Canonical and Non-canonical TGF-β Signaling Pathways.

Identifieur interne : 000376 ( Main/Exploration ); précédent : 000375; suivant : 000377

Cetrimonium Bromide Inhibits Cell Migration and Invasion of Human Hepatic SK-HEP-1 Cells Through Modulating the Canonical and Non-canonical TGF-β Signaling Pathways.

Auteurs : Tsai-Kun Wu [République populaire de Chine] ; Chung-Hung Chen [République populaire de Chine] ; Ying-Ru Pan [République populaire de Chine] ; Ching-Wen Hu [République populaire de Chine] ; Fu-Mei Huang [République populaire de Chine] ; Jer-Yuh Liu [République populaire de Chine] ; Chia-Jen Lee [République populaire de Chine]

Source :

RBID : pubmed:31262888

Descripteurs français

English descriptors

Abstract

BACKGROUND/AIM

Cetrimonium bromide (CTAB), a quaternary ammonium surfactant, is an antiseptic agent against bacteria and fungi. However, the mechanisms by which its pharmacological actions affect epithelial-mesenchymal transition (EMT) in hepatocellular carcinoma (HCC) cells, such as adenocarcinoma in SK-HEP-1 cells, have not been investigated. We, thereby, investigated whether CTAB inhibits cellular mobility and invasiveness of human hepatic adenocarcinoma in SK-HEP-1 cells.

MATERIALS AND METHODS

SK-HEP-1 cells were treated with CTAB, and subsequent migration and invasion were measured by wound healing and transwell assays. Protein expression was detected by immunoblotting analysis.

RESULTS

Our data revealed that treatment of SK-HEP-1 cells with CTAB altered their mesenchymal spindle-like morphology. CTAB exerted inhibitory effects on the migration and invasion of SK-HEP-1 cells dose-dependently, and reduced protein levels of matrix metalloproteinase-2 (MMP-2), MMP-9, snail, slug, twist, vimentin, fibronectin, N-cadherin, Smad2, Smad3, Smad4, phosphoinositide-3-kinase (PI3K), p-PI3K, Akt, p-Akt, β-catenin, mammalian target of rapamycin (mTOR), p-mTOR, p-p70S6K, p-extracellular signal-regulated kinases (ERK)1/2, p-p38 mitogen-activated protein kinase (MAPK) and p-c-Jun N-terminal kinase (JNK), but increased protein levels of tissue inhibitor matrix metalloproteinase-1 (TIMP-1), TIMP-2, claudin-1 and p-GSK3β. Based on these observations, we suggest that CTAB not only inhibits the canonical transforming growth factor-β (TGF-β) signaling pathway though reducing SMADs (an acronym from the fusion of Caenorhabditis elegans Sma genes and the Drosophila Mad, Mothers against decapentaplegic proteins), but also restrains the non-canonical TGF-β signaling including MAPK pathways like ERK1/2, p38 MAPK, JNK and PI3K.

CONCLUSION

CTAB is involved in the suppression of TGF-β-mediated mesenchymal phenotype and could be a potent medical agent for use in controlling the migration and invasion of hepatic adenocarcinoma.


DOI: 10.21873/anticanres.13510
PubMed: 31262888


Affiliations:

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Le document en format XML

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<term>Adenocarcinoma (drug therapy)</term>
<term>Adenocarcinoma (metabolism)</term>
<term>Antineoplastic Agents (pharmacology)</term>
<term>Cell Line, Tumor (MeSH)</term>
<term>Cell Movement (drug effects)</term>
<term>Cetrimonium (pharmacology)</term>
<term>Humans (MeSH)</term>
<term>Liver Neoplasms (drug therapy)</term>
<term>Liver Neoplasms (metabolism)</term>
<term>Neoplasm Invasiveness (MeSH)</term>
<term>Signal Transduction (drug effects)</term>
<term>Transforming Growth Factor beta (metabolism)</term>
</keywords>
<keywords scheme="KwdFr" xml:lang="fr">
<term>Adénocarcinome (métabolisme)</term>
<term>Adénocarcinome (traitement médicamenteux)</term>
<term>Antinéoplasiques (pharmacologie)</term>
<term>Bromure de cétrimonium (pharmacologie)</term>
<term>Facteur de croissance transformant bêta (métabolisme)</term>
<term>Humains (MeSH)</term>
<term>Invasion tumorale (MeSH)</term>
<term>Lignée cellulaire tumorale (MeSH)</term>
<term>Mouvement cellulaire (effets des médicaments et des substances chimiques)</term>
<term>Transduction du signal (effets des médicaments et des substances chimiques)</term>
<term>Tumeurs du foie (métabolisme)</term>
<term>Tumeurs du foie (traitement médicamenteux)</term>
</keywords>
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<term>Transforming Growth Factor beta</term>
</keywords>
<keywords scheme="MESH" type="chemical" qualifier="pharmacology" xml:lang="en">
<term>Antineoplastic Agents</term>
<term>Cetrimonium</term>
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<term>Cell Movement</term>
<term>Signal Transduction</term>
</keywords>
<keywords scheme="MESH" qualifier="drug therapy" xml:lang="en">
<term>Adenocarcinoma</term>
<term>Liver Neoplasms</term>
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<term>Mouvement cellulaire</term>
<term>Transduction du signal</term>
</keywords>
<keywords scheme="MESH" qualifier="metabolism" xml:lang="en">
<term>Adenocarcinoma</term>
<term>Liver Neoplasms</term>
</keywords>
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<term>Adénocarcinome</term>
<term>Facteur de croissance transformant bêta</term>
<term>Tumeurs du foie</term>
</keywords>
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<term>Antinéoplasiques</term>
<term>Bromure de cétrimonium</term>
</keywords>
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<term>Tumeurs du foie</term>
</keywords>
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<term>Humans</term>
<term>Neoplasm Invasiveness</term>
</keywords>
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<p>
<b>BACKGROUND/AIM</b>
</p>
<p>Cetrimonium bromide (CTAB), a quaternary ammonium surfactant, is an antiseptic agent against bacteria and fungi. However, the mechanisms by which its pharmacological actions affect epithelial-mesenchymal transition (EMT) in hepatocellular carcinoma (HCC) cells, such as adenocarcinoma in SK-HEP-1 cells, have not been investigated. We, thereby, investigated whether CTAB inhibits cellular mobility and invasiveness of human hepatic adenocarcinoma in SK-HEP-1 cells.</p>
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<div type="abstract" xml:lang="en">
<p>
<b>MATERIALS AND METHODS</b>
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<p>SK-HEP-1 cells were treated with CTAB, and subsequent migration and invasion were measured by wound healing and transwell assays. Protein expression was detected by immunoblotting analysis.</p>
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<div type="abstract" xml:lang="en">
<p>
<b>RESULTS</b>
</p>
<p>Our data revealed that treatment of SK-HEP-1 cells with CTAB altered their mesenchymal spindle-like morphology. CTAB exerted inhibitory effects on the migration and invasion of SK-HEP-1 cells dose-dependently, and reduced protein levels of matrix metalloproteinase-2 (MMP-2), MMP-9, snail, slug, twist, vimentin, fibronectin, N-cadherin, Smad2, Smad3, Smad4, phosphoinositide-3-kinase (PI3K), p-PI3K, Akt, p-Akt, β-catenin, mammalian target of rapamycin (mTOR), p-mTOR, p-p70S6K, p-extracellular signal-regulated kinases (ERK)1/2, p-p38 mitogen-activated protein kinase (MAPK) and p-c-Jun N-terminal kinase (JNK), but increased protein levels of tissue inhibitor matrix metalloproteinase-1 (TIMP-1), TIMP-2, claudin-1 and p-GSK3β. Based on these observations, we suggest that CTAB not only inhibits the canonical transforming growth factor-β (TGF-β) signaling pathway though reducing SMADs (an acronym from the fusion of Caenorhabditis elegans Sma genes and the Drosophila Mad, Mothers against decapentaplegic proteins), but also restrains the non-canonical TGF-β signaling including MAPK pathways like ERK1/2, p38 MAPK, JNK and PI3K.</p>
</div>
<div type="abstract" xml:lang="en">
<p>
<b>CONCLUSION</b>
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<p>CTAB is involved in the suppression of TGF-β-mediated mesenchymal phenotype and could be a potent medical agent for use in controlling the migration and invasion of hepatic adenocarcinoma.</p>
</div>
</front>
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<Month>07</Month>
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<ISSN IssnType="Electronic">1791-7530</ISSN>
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<AbstractText Label="BACKGROUND/AIM" NlmCategory="OBJECTIVE">Cetrimonium bromide (CTAB), a quaternary ammonium surfactant, is an antiseptic agent against bacteria and fungi. However, the mechanisms by which its pharmacological actions affect epithelial-mesenchymal transition (EMT) in hepatocellular carcinoma (HCC) cells, such as adenocarcinoma in SK-HEP-1 cells, have not been investigated. We, thereby, investigated whether CTAB inhibits cellular mobility and invasiveness of human hepatic adenocarcinoma in SK-HEP-1 cells.</AbstractText>
<AbstractText Label="MATERIALS AND METHODS" NlmCategory="METHODS">SK-HEP-1 cells were treated with CTAB, and subsequent migration and invasion were measured by wound healing and transwell assays. Protein expression was detected by immunoblotting analysis.</AbstractText>
<AbstractText Label="RESULTS" NlmCategory="RESULTS">Our data revealed that treatment of SK-HEP-1 cells with CTAB altered their mesenchymal spindle-like morphology. CTAB exerted inhibitory effects on the migration and invasion of SK-HEP-1 cells dose-dependently, and reduced protein levels of matrix metalloproteinase-2 (MMP-2), MMP-9, snail, slug, twist, vimentin, fibronectin, N-cadherin, Smad2, Smad3, Smad4, phosphoinositide-3-kinase (PI3K), p-PI3K, Akt, p-Akt, β-catenin, mammalian target of rapamycin (mTOR), p-mTOR, p-p70S6K, p-extracellular signal-regulated kinases (ERK)1/2, p-p38 mitogen-activated protein kinase (MAPK) and p-c-Jun N-terminal kinase (JNK), but increased protein levels of tissue inhibitor matrix metalloproteinase-1 (TIMP-1), TIMP-2, claudin-1 and p-GSK3β. Based on these observations, we suggest that CTAB not only inhibits the canonical transforming growth factor-β (TGF-β) signaling pathway though reducing SMADs (an acronym from the fusion of Caenorhabditis elegans Sma genes and the Drosophila Mad, Mothers against decapentaplegic proteins), but also restrains the non-canonical TGF-β signaling including MAPK pathways like ERK1/2, p38 MAPK, JNK and PI3K.</AbstractText>
<AbstractText Label="CONCLUSION" NlmCategory="CONCLUSIONS">CTAB is involved in the suppression of TGF-β-mediated mesenchymal phenotype and could be a potent medical agent for use in controlling the migration and invasion of hepatic adenocarcinoma.</AbstractText>
<CopyrightInformation>Copyright© 2019, International Institute of Anticancer Research (Dr. George J. Delinasios), All rights reserved.</CopyrightInformation>
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<LastName>Wu</LastName>
<ForeName>Tsai-Kun</ForeName>
<Initials>TK</Initials>
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<Affiliation>Division of Renal Medicine, Tungs' Taichung Metroharbor Hospital, Taichung, Taiwan, R.O.C.</Affiliation>
</AffiliationInfo>
<AffiliationInfo>
<Affiliation>Department of Nutrition, Master Program of Biomedical Nutrition, Hungkuang University, Taichung, Taiwan, R.O.C.</Affiliation>
</AffiliationInfo>
<AffiliationInfo>
<Affiliation>Department of Nursing, Jen-Teh Junior College of Medicine, Nursing and Management, Miaoli, Taiwan, R.O.C.</Affiliation>
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<Affiliation>Department of Gastroenterology, Chang Bing Show Chwan Memorial Hospital, Changhua, Taiwan, R.O.C.</Affiliation>
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<ForeName>Ying-Ru</ForeName>
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<ForeName>Fu-Mei</ForeName>
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<Affiliation>Operating Theatre, Chung Shan Medical University Hospital, Taichung, Taiwan, R.O.C.</Affiliation>
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<LastName>Liu</LastName>
<ForeName>Jer-Yuh</ForeName>
<Initials>JY</Initials>
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<Affiliation>Center for Molecular Medicine, China Medical University Hospital, Taichung, Taiwan, R.O.C.</Affiliation>
</AffiliationInfo>
<AffiliationInfo>
<Affiliation>Graduate Institute of Biomedical Sciences, China Medical University, Taichung, Taiwan, R.O.C.</Affiliation>
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</Author>
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<LastName>Lee</LastName>
<ForeName>Chia-Jen</ForeName>
<Initials>CJ</Initials>
<AffiliationInfo>
<Affiliation>Department of Medical Research, Tungs' Taichung Metroharbor Hospital, Taichung, Taiwan, R.O.C. chiajenlee54@gmail.com.</Affiliation>
</AffiliationInfo>
<AffiliationInfo>
<Affiliation>Department of Rehabilitation, Jen-Teh Junior College of Medicine, Nursing and Management, Miaoli, Taiwan R.O.C.</Affiliation>
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<Country>Greece</Country>
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<ISSNLinking>0250-7005</ISSNLinking>
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<Chemical>
<RegistryNumber>0</RegistryNumber>
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<Chemical>
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<DescriptorName UI="D008113" MajorTopicYN="N">Liver Neoplasms</DescriptorName>
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<MeshHeading>
<DescriptorName UI="D016212" MajorTopicYN="N">Transforming Growth Factor beta</DescriptorName>
<QualifierName UI="Q000378" MajorTopicYN="Y">metabolism</QualifierName>
</MeshHeading>
</MeshHeadingList>
<KeywordList Owner="NOTNLM">
<Keyword MajorTopicYN="N">Cetrimonium bromide (CTAB)</Keyword>
<Keyword MajorTopicYN="N">SK-HEP-1</Keyword>
<Keyword MajorTopicYN="N">hepatic cancer</Keyword>
<Keyword MajorTopicYN="N">transforming growth factor-β (TGF-β)</Keyword>
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</MedlineCitation>
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<Year>2019</Year>
<Month>05</Month>
<Day>20</Day>
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<Year>2019</Year>
<Month>06</Month>
<Day>18</Day>
</PubMedPubDate>
<PubMedPubDate PubStatus="accepted">
<Year>2019</Year>
<Month>06</Month>
<Day>20</Day>
</PubMedPubDate>
<PubMedPubDate PubStatus="entrez">
<Year>2019</Year>
<Month>7</Month>
<Day>3</Day>
<Hour>6</Hour>
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<PubMedPubDate PubStatus="medline">
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<Day>10</Day>
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<PublicationStatus>ppublish</PublicationStatus>
<ArticleIdList>
<ArticleId IdType="pubmed">31262888</ArticleId>
<ArticleId IdType="pii">39/7/3621</ArticleId>
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<country>
<li>République populaire de Chine</li>
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<name sortKey="Wu, Tsai Kun" sort="Wu, Tsai Kun" uniqKey="Wu T" first="Tsai-Kun" last="Wu">Tsai-Kun Wu</name>
</noRegion>
<name sortKey="Chen, Chung Hung" sort="Chen, Chung Hung" uniqKey="Chen C" first="Chung-Hung" last="Chen">Chung-Hung Chen</name>
<name sortKey="Hu, Ching Wen" sort="Hu, Ching Wen" uniqKey="Hu C" first="Ching-Wen" last="Hu">Ching-Wen Hu</name>
<name sortKey="Huang, Fu Mei" sort="Huang, Fu Mei" uniqKey="Huang F" first="Fu-Mei" last="Huang">Fu-Mei Huang</name>
<name sortKey="Lee, Chia Jen" sort="Lee, Chia Jen" uniqKey="Lee C" first="Chia-Jen" last="Lee">Chia-Jen Lee</name>
<name sortKey="Liu, Jer Yuh" sort="Liu, Jer Yuh" uniqKey="Liu J" first="Jer-Yuh" last="Liu">Jer-Yuh Liu</name>
<name sortKey="Liu, Jer Yuh" sort="Liu, Jer Yuh" uniqKey="Liu J" first="Jer-Yuh" last="Liu">Jer-Yuh Liu</name>
<name sortKey="Pan, Ying Ru" sort="Pan, Ying Ru" uniqKey="Pan Y" first="Ying-Ru" last="Pan">Ying-Ru Pan</name>
<name sortKey="Wu, Tsai Kun" sort="Wu, Tsai Kun" uniqKey="Wu T" first="Tsai-Kun" last="Wu">Tsai-Kun Wu</name>
<name sortKey="Wu, Tsai Kun" sort="Wu, Tsai Kun" uniqKey="Wu T" first="Tsai-Kun" last="Wu">Tsai-Kun Wu</name>
</country>
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