Signalling pathway for RKIP and Let-7 regulates and predicts metastatic breast cancer

Jieun Yun; Casey A. Frankenberger; Wen Liang Kuo; Mirjam C. Boelens; Eva M. Eves; Nancy Cheng; Han Liang; Wen Hsiung Li; Hemant Ishwaran; Andy J. Minn; Marsha Rich Rosner

doi:10.1038/emboj.2011.312

Signalling pathway for RKIP and Let-7 regulates and predicts metastatic breast cancer

Jieun Yun, Casey A. Frankenberger, Wen Liang Kuo, Mirjam C. Boelens, Eva M. Eves, Nancy Cheng, Han Liang, Wen Hsiung Li, Hemant Ishwaran, Andy J. Minn, Marsha Rich Rosner

Bioinformatics & Computational Biology

Research output: Contribution to journal › Article › peer-review

171 Scopus citations

Abstract

Tumour metastasis suppressors are inhibitors of metastasis but their mechanisms of action are generally not understood. We previously showed that the suppressor Raf kinase inhibitory protein (RKIP) inhibits breast tumour metastasis in part via let-7. Here, we demonstrate an integrated approach combining statistical analysis of breast tumour gene expression data and experimental validation to extend the signalling pathway for RKIP. We show that RKIP inhibits let-7 targets (HMGA2, BACH1) that in turn upregulate bone metastasis genes (MMP1, OPN, CXCR4). Our results reveal BACH1 as a novel let-7-regulated transcription factor that induces matrix metalloproteinase1 (MMP1) expression and promotes metastasis. An RKIP pathway metastasis signature (designated RPMS) derived from the complete signalling cascade predicts high metastatic risk better than the individual genes. These results highlight a powerful approach for identifying signalling pathways downstream of a key metastasis suppressor and indicate that analysis of genes in the context of their signalling environment is critical for understanding their predictive and therapeutic potential.

Original language	English (US)
Pages (from-to)	4500-4514
Number of pages	15
Journal	EMBO Journal
Volume	30
Issue number	21
DOIs	https://doi.org/10.1038/emboj.2011.312
State	Published - Nov 2 2011

Keywords

BACH1
Let-7
RKIP
gene signature
metastasis

ASJC Scopus subject areas

General Neuroscience
Molecular Biology
General Biochemistry, Genetics and Molecular Biology
General Immunology and Microbiology

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10.1038/emboj.2011.312

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title = "Signalling pathway for RKIP and Let-7 regulates and predicts metastatic breast cancer",

abstract = "Tumour metastasis suppressors are inhibitors of metastasis but their mechanisms of action are generally not understood. We previously showed that the suppressor Raf kinase inhibitory protein (RKIP) inhibits breast tumour metastasis in part via let-7. Here, we demonstrate an integrated approach combining statistical analysis of breast tumour gene expression data and experimental validation to extend the signalling pathway for RKIP. We show that RKIP inhibits let-7 targets (HMGA2, BACH1) that in turn upregulate bone metastasis genes (MMP1, OPN, CXCR4). Our results reveal BACH1 as a novel let-7-regulated transcription factor that induces matrix metalloproteinase1 (MMP1) expression and promotes metastasis. An RKIP pathway metastasis signature (designated RPMS) derived from the complete signalling cascade predicts high metastatic risk better than the individual genes. These results highlight a powerful approach for identifying signalling pathways downstream of a key metastasis suppressor and indicate that analysis of genes in the context of their signalling environment is critical for understanding their predictive and therapeutic potential.",

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author = "Jieun Yun and Frankenberger, {Casey A.} and Kuo, {Wen Liang} and Boelens, {Mirjam C.} and Eves, {Eva M.} and Nancy Cheng and Han Liang and Li, {Wen Hsiung} and Hemant Ishwaran and Minn, {Andy J.} and Rosner, {Marsha Rich}",

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doi = "10.1038/emboj.2011.312",

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AU - Yun, Jieun

AU - Frankenberger, Casey A.

AU - Kuo, Wen Liang

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AU - Eves, Eva M.

AU - Cheng, Nancy

AU - Liang, Han

AU - Li, Wen Hsiung

AU - Ishwaran, Hemant

AU - Minn, Andy J.

AU - Rosner, Marsha Rich

PY - 2011/11/2

Y1 - 2011/11/2

N2 - Tumour metastasis suppressors are inhibitors of metastasis but their mechanisms of action are generally not understood. We previously showed that the suppressor Raf kinase inhibitory protein (RKIP) inhibits breast tumour metastasis in part via let-7. Here, we demonstrate an integrated approach combining statistical analysis of breast tumour gene expression data and experimental validation to extend the signalling pathway for RKIP. We show that RKIP inhibits let-7 targets (HMGA2, BACH1) that in turn upregulate bone metastasis genes (MMP1, OPN, CXCR4). Our results reveal BACH1 as a novel let-7-regulated transcription factor that induces matrix metalloproteinase1 (MMP1) expression and promotes metastasis. An RKIP pathway metastasis signature (designated RPMS) derived from the complete signalling cascade predicts high metastatic risk better than the individual genes. These results highlight a powerful approach for identifying signalling pathways downstream of a key metastasis suppressor and indicate that analysis of genes in the context of their signalling environment is critical for understanding their predictive and therapeutic potential.

AB - Tumour metastasis suppressors are inhibitors of metastasis but their mechanisms of action are generally not understood. We previously showed that the suppressor Raf kinase inhibitory protein (RKIP) inhibits breast tumour metastasis in part via let-7. Here, we demonstrate an integrated approach combining statistical analysis of breast tumour gene expression data and experimental validation to extend the signalling pathway for RKIP. We show that RKIP inhibits let-7 targets (HMGA2, BACH1) that in turn upregulate bone metastasis genes (MMP1, OPN, CXCR4). Our results reveal BACH1 as a novel let-7-regulated transcription factor that induces matrix metalloproteinase1 (MMP1) expression and promotes metastasis. An RKIP pathway metastasis signature (designated RPMS) derived from the complete signalling cascade predicts high metastatic risk better than the individual genes. These results highlight a powerful approach for identifying signalling pathways downstream of a key metastasis suppressor and indicate that analysis of genes in the context of their signalling environment is critical for understanding their predictive and therapeutic potential.

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Signalling pathway for RKIP and Let-7 regulates and predicts metastatic breast cancer

Abstract

Keywords

ASJC Scopus subject areas

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