P21CIP1 mediates reciprocal switching between proliferation and invasion during metastasis Journal Article


Authors: Qian, X.; Hulit, J.; Suyama, K.; Eugenin, E. A.; Belbin, T. J.; Loudig, O.; Smirnova, T.; Zhou, Z. N.; Segall, J.; Locker, J.; Phillips, G. R.; Norton, L.; Hazan, R. B.
Article Title: P21CIP1 mediates reciprocal switching between proliferation and invasion during metastasis
Abstract: Cell proliferation and invasion are critical for malignant progression, yet how these processes relate to each other and whether they regulate one another during metastasis is unknown. We show that invasiveness of breast cancer cells is associated with growth arrest due to p21CIP1 upregulation. Knockdown of p21CIP1 increases cell proliferation and suppresses invasion. Since p21CIP1 acts to inhibit cyclin E during cell-cycle progression, we demonstrated that a constitutively active form of cyclin E had similar effects to p21CIP1 inhibition resulting in enhanced cell growth and suppressed invasiveness. We tested these findings in vivo in the Polyoma middle T mammary tumor model in which p21CIP1 was deleted. p21CIP1 knockout mice exhibited dramatic suppression of metastasis, independent of tumor growth, which was rescued by p21CIP1. Metastasis suppression by p21CIP1 ablation was associated with striking cytoskeletal reorganization leading to a non-invasive and highly proliferative state. Thus, p21CIP1 regulates metastasis by mediating reciprocal switching between invasion and proliferation. © 2013 Macmillan Publishers Limited.
Keywords: cell cycle; metastasis; breast cancer; cytoskeleton; invasion; cyclin e; p21cip1
Journal Title: Oncogene
Volume: 32
Issue: 18
ISSN: 0950-9232
Publisher: Nature Publishing Group  
Date Published: 2013-05-02
Start Page: 2292
End Page: 2303
Language: English
DOI: 10.1038/onc.2012.249
PROVIDER: scopus
PUBMED: 22751124
PMCID: PMC4350674
DOI/URL:
Notes: --- - "Export Date: 3 June 2013" - "CODEN: ONCNE" - "Source: Scopus"
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  1. Larry Norton
    758 Norton