Aurora-A down-regulates IkappaBα via Akt activation and interacts with insulin-like growth factor-1 induced phosphatidylinositol 3-kinase pathway for cancer cell survival

BACKGROUND: The mitotic Aurora-A kinase exerts crucial functions in maintaining mitotic fidelity. As a bona fide oncoprotein, Aurora-A aberrant overexpression leads to oncogenic transformation. Yet, the mechanisms by which Aurora-A enhances cancer cell survival remain to be elucidated. RESULTS: Here...

Descripción completa

Detalles Bibliográficos
Autores principales: Yao, Jin-e, Yan, Min, Guan, Zhong, Pan, Chao-bin, Xia, Liang-ping, Li, Chuan-xing, Wang, Li-hui, Long, Zi-jie, Zhao, Yan, Li, Ming-wei, Zheng, Fei-meng, Xu, Jie, Lin, Dong-jun, Liu, Quentin
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2009
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2780390/
https://www.ncbi.nlm.nih.gov/pubmed/19891769
http://dx.doi.org/10.1186/1476-4598-8-95
_version_ 1782174477454409728
author Yao, Jin-e
Yan, Min
Guan, Zhong
Pan, Chao-bin
Xia, Liang-ping
Li, Chuan-xing
Wang, Li-hui
Long, Zi-jie
Zhao, Yan
Li, Ming-wei
Zheng, Fei-meng
Xu, Jie
Lin, Dong-jun
Liu, Quentin
author_facet Yao, Jin-e
Yan, Min
Guan, Zhong
Pan, Chao-bin
Xia, Liang-ping
Li, Chuan-xing
Wang, Li-hui
Long, Zi-jie
Zhao, Yan
Li, Ming-wei
Zheng, Fei-meng
Xu, Jie
Lin, Dong-jun
Liu, Quentin
author_sort Yao, Jin-e
collection PubMed
description BACKGROUND: The mitotic Aurora-A kinase exerts crucial functions in maintaining mitotic fidelity. As a bona fide oncoprotein, Aurora-A aberrant overexpression leads to oncogenic transformation. Yet, the mechanisms by which Aurora-A enhances cancer cell survival remain to be elucidated. RESULTS: Here, we found that Aurora-A overexpression was closely correlated with clinic stage and lymph node metastasis in tongue carcinoma. Aurora-A inhibitory VX-680 suppressed proliferation, induced apoptosis and markedly reduced migration in cancer cells. We further showed that insulin-like growth factor-1, a PI3K physiological activator, reversed VX-680-decreased cell survival and motility. Conversely, wortmannin, a PI3K inhibitor, combined with VX-680 showed a synergistic effect on inducing apoptosis and suppressing migration. In addition, Aurora-A inhibition suppressed Akt activation, and VX-680-induced apoptosis was attenuated by Myr-Akt overexpression, revealing a cross-talk between Aurora-A and PI3K pathway interacting at Akt activation. Significantly, we showed that suppression of Aurora-A decreased phosphorylated Akt and was associated with increased IkappaBα expression. By contrast, Aurora-A overexpression upregulated Akt activity and downregulated IkappaBα, these changes were accompanied by nuclear translocation of nuclear factor-κB and increased expression of its target gene Bcl-xL. Lastly, Aurora-A overexpression induced IkappaBα reduction was abrogated by suppression of Akt either chemically or genetically. CONCLUSION: Taken together, our data established that Aurora-A, via activating Akt, stimulated nuclear factor-κB signaling pathway to promote cancer cell survival, and promised a novel combined chemotherapy targeting both Aurora-A and PI3K in cancer treatment.
format Text
id pubmed-2780390
institution National Center for Biotechnology Information
language English
publishDate 2009
publisher BioMed Central
record_format MEDLINE/PubMed
spelling pubmed-27803902009-11-21 Aurora-A down-regulates IkappaBα via Akt activation and interacts with insulin-like growth factor-1 induced phosphatidylinositol 3-kinase pathway for cancer cell survival Yao, Jin-e Yan, Min Guan, Zhong Pan, Chao-bin Xia, Liang-ping Li, Chuan-xing Wang, Li-hui Long, Zi-jie Zhao, Yan Li, Ming-wei Zheng, Fei-meng Xu, Jie Lin, Dong-jun Liu, Quentin Mol Cancer Research BACKGROUND: The mitotic Aurora-A kinase exerts crucial functions in maintaining mitotic fidelity. As a bona fide oncoprotein, Aurora-A aberrant overexpression leads to oncogenic transformation. Yet, the mechanisms by which Aurora-A enhances cancer cell survival remain to be elucidated. RESULTS: Here, we found that Aurora-A overexpression was closely correlated with clinic stage and lymph node metastasis in tongue carcinoma. Aurora-A inhibitory VX-680 suppressed proliferation, induced apoptosis and markedly reduced migration in cancer cells. We further showed that insulin-like growth factor-1, a PI3K physiological activator, reversed VX-680-decreased cell survival and motility. Conversely, wortmannin, a PI3K inhibitor, combined with VX-680 showed a synergistic effect on inducing apoptosis and suppressing migration. In addition, Aurora-A inhibition suppressed Akt activation, and VX-680-induced apoptosis was attenuated by Myr-Akt overexpression, revealing a cross-talk between Aurora-A and PI3K pathway interacting at Akt activation. Significantly, we showed that suppression of Aurora-A decreased phosphorylated Akt and was associated with increased IkappaBα expression. By contrast, Aurora-A overexpression upregulated Akt activity and downregulated IkappaBα, these changes were accompanied by nuclear translocation of nuclear factor-κB and increased expression of its target gene Bcl-xL. Lastly, Aurora-A overexpression induced IkappaBα reduction was abrogated by suppression of Akt either chemically or genetically. CONCLUSION: Taken together, our data established that Aurora-A, via activating Akt, stimulated nuclear factor-κB signaling pathway to promote cancer cell survival, and promised a novel combined chemotherapy targeting both Aurora-A and PI3K in cancer treatment. BioMed Central 2009-11-05 /pmc/articles/PMC2780390/ /pubmed/19891769 http://dx.doi.org/10.1186/1476-4598-8-95 Text en Copyright ©2009 Yao et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Yao, Jin-e
Yan, Min
Guan, Zhong
Pan, Chao-bin
Xia, Liang-ping
Li, Chuan-xing
Wang, Li-hui
Long, Zi-jie
Zhao, Yan
Li, Ming-wei
Zheng, Fei-meng
Xu, Jie
Lin, Dong-jun
Liu, Quentin
Aurora-A down-regulates IkappaBα via Akt activation and interacts with insulin-like growth factor-1 induced phosphatidylinositol 3-kinase pathway for cancer cell survival
title Aurora-A down-regulates IkappaBα via Akt activation and interacts with insulin-like growth factor-1 induced phosphatidylinositol 3-kinase pathway for cancer cell survival
title_full Aurora-A down-regulates IkappaBα via Akt activation and interacts with insulin-like growth factor-1 induced phosphatidylinositol 3-kinase pathway for cancer cell survival
title_fullStr Aurora-A down-regulates IkappaBα via Akt activation and interacts with insulin-like growth factor-1 induced phosphatidylinositol 3-kinase pathway for cancer cell survival
title_full_unstemmed Aurora-A down-regulates IkappaBα via Akt activation and interacts with insulin-like growth factor-1 induced phosphatidylinositol 3-kinase pathway for cancer cell survival
title_short Aurora-A down-regulates IkappaBα via Akt activation and interacts with insulin-like growth factor-1 induced phosphatidylinositol 3-kinase pathway for cancer cell survival
title_sort aurora-a down-regulates ikappabα via akt activation and interacts with insulin-like growth factor-1 induced phosphatidylinositol 3-kinase pathway for cancer cell survival
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2780390/
https://www.ncbi.nlm.nih.gov/pubmed/19891769
http://dx.doi.org/10.1186/1476-4598-8-95
work_keys_str_mv AT yaojine auroraadownregulatesikappabaviaaktactivationandinteractswithinsulinlikegrowthfactor1inducedphosphatidylinositol3kinasepathwayforcancercellsurvival
AT yanmin auroraadownregulatesikappabaviaaktactivationandinteractswithinsulinlikegrowthfactor1inducedphosphatidylinositol3kinasepathwayforcancercellsurvival
AT guanzhong auroraadownregulatesikappabaviaaktactivationandinteractswithinsulinlikegrowthfactor1inducedphosphatidylinositol3kinasepathwayforcancercellsurvival
AT panchaobin auroraadownregulatesikappabaviaaktactivationandinteractswithinsulinlikegrowthfactor1inducedphosphatidylinositol3kinasepathwayforcancercellsurvival
AT xialiangping auroraadownregulatesikappabaviaaktactivationandinteractswithinsulinlikegrowthfactor1inducedphosphatidylinositol3kinasepathwayforcancercellsurvival
AT lichuanxing auroraadownregulatesikappabaviaaktactivationandinteractswithinsulinlikegrowthfactor1inducedphosphatidylinositol3kinasepathwayforcancercellsurvival
AT wanglihui auroraadownregulatesikappabaviaaktactivationandinteractswithinsulinlikegrowthfactor1inducedphosphatidylinositol3kinasepathwayforcancercellsurvival
AT longzijie auroraadownregulatesikappabaviaaktactivationandinteractswithinsulinlikegrowthfactor1inducedphosphatidylinositol3kinasepathwayforcancercellsurvival
AT zhaoyan auroraadownregulatesikappabaviaaktactivationandinteractswithinsulinlikegrowthfactor1inducedphosphatidylinositol3kinasepathwayforcancercellsurvival
AT limingwei auroraadownregulatesikappabaviaaktactivationandinteractswithinsulinlikegrowthfactor1inducedphosphatidylinositol3kinasepathwayforcancercellsurvival
AT zhengfeimeng auroraadownregulatesikappabaviaaktactivationandinteractswithinsulinlikegrowthfactor1inducedphosphatidylinositol3kinasepathwayforcancercellsurvival
AT xujie auroraadownregulatesikappabaviaaktactivationandinteractswithinsulinlikegrowthfactor1inducedphosphatidylinositol3kinasepathwayforcancercellsurvival
AT lindongjun auroraadownregulatesikappabaviaaktactivationandinteractswithinsulinlikegrowthfactor1inducedphosphatidylinositol3kinasepathwayforcancercellsurvival
AT liuquentin auroraadownregulatesikappabaviaaktactivationandinteractswithinsulinlikegrowthfactor1inducedphosphatidylinositol3kinasepathwayforcancercellsurvival

Ejemplares similares