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Chamaejasmenin B, a novel candidate, inhibits breast tumor metastasis by rebalancing TGF-beta paradox

Metastasis is the leading lethal factor severely restraining the effectiveness of clinical treatment. TGF-beta is the key regulator for metastasis and influences paradoxically on cancer progression. The known TGF-beta blockers exert little selectivity on its functions, indiscriminately causing the a...

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Autores principales: Li, Qi, Wang, Yajie, Xiao, Hongbin, Li, Yujie, Kan, Xiaoxi, Wang, Xiaomin, Zhang, Ganlin, Wang, Zhixin, Yang, Qing, Chen, Xi, Weng, Xiaogang, Chen, Ying, Zhou, Bingbing, Guo, Yan, Liu, Xucen, Zhu, Xiaoxin
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5217010/
https://www.ncbi.nlm.nih.gov/pubmed/27374079
http://dx.doi.org/10.18632/oncotarget.10193
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author Li, Qi
Wang, Yajie
Xiao, Hongbin
Li, Yujie
Kan, Xiaoxi
Wang, Xiaomin
Zhang, Ganlin
Wang, Zhixin
Yang, Qing
Chen, Xi
Weng, Xiaogang
Chen, Ying
Zhou, Bingbing
Guo, Yan
Liu, Xucen
Zhu, Xiaoxin
author_facet Li, Qi
Wang, Yajie
Xiao, Hongbin
Li, Yujie
Kan, Xiaoxi
Wang, Xiaomin
Zhang, Ganlin
Wang, Zhixin
Yang, Qing
Chen, Xi
Weng, Xiaogang
Chen, Ying
Zhou, Bingbing
Guo, Yan
Liu, Xucen
Zhu, Xiaoxin
author_sort Li, Qi
collection PubMed
description Metastasis is the leading lethal factor severely restraining the effectiveness of clinical treatment. TGF-beta is the key regulator for metastasis and influences paradoxically on cancer progression. The known TGF-beta blockers exert little selectivity on its functions, indiscriminately causing the anti-metastatic and pro-growth effects. Under such circumstances, specifically rebalancing the oncological function of TGF-beta provides a crucial oncotarget against metastasis. In our study, we established the screening platform targeting cell motility and identified a potential flavonoid, Chamaejasmenin B (ICJ), extracted from Stellera chamaejasme L. It suppressed the migration and invasion in breast cancer cells in vitro. Moreover, by dynamical quantification of breast cancer progression in small-animal imaging system, ICJ was proved to be a potent inhibitor of metastasis with minimal toxic side effects. Mechanism study further revealed that ICJ efficiently blocked TGF-beta induced EMT, disrupted the interaction between β3 integrin-TβRII complex and, consequently, resulted in the selective inhibition of FAK:Src:p38 pathway. Meanwhile, specific blockage of this pathway largely attenuated the anti-metastatic function of ICJ. Importantly, in contrast with the antagonistic effects on TGF-beta induced metastasis, ICJ obviously sensitized its cytostatic activity, suggesting that it was not a pan-blocker but a rebalancer for the functional output of TGF-beta. Collectively, by targeting TGF-beta Paradox, we experimentally provided a promising candidate for metastatic intervention.
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spelling pubmed-52170102017-01-17 Chamaejasmenin B, a novel candidate, inhibits breast tumor metastasis by rebalancing TGF-beta paradox Li, Qi Wang, Yajie Xiao, Hongbin Li, Yujie Kan, Xiaoxi Wang, Xiaomin Zhang, Ganlin Wang, Zhixin Yang, Qing Chen, Xi Weng, Xiaogang Chen, Ying Zhou, Bingbing Guo, Yan Liu, Xucen Zhu, Xiaoxin Oncotarget Research Paper Metastasis is the leading lethal factor severely restraining the effectiveness of clinical treatment. TGF-beta is the key regulator for metastasis and influences paradoxically on cancer progression. The known TGF-beta blockers exert little selectivity on its functions, indiscriminately causing the anti-metastatic and pro-growth effects. Under such circumstances, specifically rebalancing the oncological function of TGF-beta provides a crucial oncotarget against metastasis. In our study, we established the screening platform targeting cell motility and identified a potential flavonoid, Chamaejasmenin B (ICJ), extracted from Stellera chamaejasme L. It suppressed the migration and invasion in breast cancer cells in vitro. Moreover, by dynamical quantification of breast cancer progression in small-animal imaging system, ICJ was proved to be a potent inhibitor of metastasis with minimal toxic side effects. Mechanism study further revealed that ICJ efficiently blocked TGF-beta induced EMT, disrupted the interaction between β3 integrin-TβRII complex and, consequently, resulted in the selective inhibition of FAK:Src:p38 pathway. Meanwhile, specific blockage of this pathway largely attenuated the anti-metastatic function of ICJ. Importantly, in contrast with the antagonistic effects on TGF-beta induced metastasis, ICJ obviously sensitized its cytostatic activity, suggesting that it was not a pan-blocker but a rebalancer for the functional output of TGF-beta. Collectively, by targeting TGF-beta Paradox, we experimentally provided a promising candidate for metastatic intervention. Impact Journals LLC 2016-06-21 /pmc/articles/PMC5217010/ /pubmed/27374079 http://dx.doi.org/10.18632/oncotarget.10193 Text en Copyright: © 2016 Li et al. http://creativecommons.org/licenses/by/2.5/ 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 credited.
spellingShingle Research Paper
Li, Qi
Wang, Yajie
Xiao, Hongbin
Li, Yujie
Kan, Xiaoxi
Wang, Xiaomin
Zhang, Ganlin
Wang, Zhixin
Yang, Qing
Chen, Xi
Weng, Xiaogang
Chen, Ying
Zhou, Bingbing
Guo, Yan
Liu, Xucen
Zhu, Xiaoxin
Chamaejasmenin B, a novel candidate, inhibits breast tumor metastasis by rebalancing TGF-beta paradox
title Chamaejasmenin B, a novel candidate, inhibits breast tumor metastasis by rebalancing TGF-beta paradox
title_full Chamaejasmenin B, a novel candidate, inhibits breast tumor metastasis by rebalancing TGF-beta paradox
title_fullStr Chamaejasmenin B, a novel candidate, inhibits breast tumor metastasis by rebalancing TGF-beta paradox
title_full_unstemmed Chamaejasmenin B, a novel candidate, inhibits breast tumor metastasis by rebalancing TGF-beta paradox
title_short Chamaejasmenin B, a novel candidate, inhibits breast tumor metastasis by rebalancing TGF-beta paradox
title_sort chamaejasmenin b, a novel candidate, inhibits breast tumor metastasis by rebalancing tgf-beta paradox
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5217010/
https://www.ncbi.nlm.nih.gov/pubmed/27374079
http://dx.doi.org/10.18632/oncotarget.10193
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