NME1L Negatively Regulates IGF1-Dependent Proliferation of Breast Cancer Cells

Title
NME1L Negatively Regulates IGF1-Dependent Proliferation of Breast Cancer Cells
Authors
이철주유동주Sunam Mander박초롱구옥재오성현안규리성재영황종익
Issue Date
2016-01
Publisher
Journal of cellular biochemistry
Citation
VOL 117, NO 6-1463
Abstract
Non-metastatic cells 1 (NME1) or nm23 is the first metastasis suppressor gene discovered. It functions through various enzymatic activities and interacts with many intracellular proteins. The NME1 gene encodes two splicing variants, NME1 and NME1L. Most studies have focused on NME1 because of its abundance in cells. We previously reported NME1L-mediated suppression of NF-B signaling by interacting with and inhibiting IKK. In this study, we demonstrated that NME1L, but not NME1, mediated inhibition of cell proliferation, although both NME1 and NME1L were involved in suppressing metastasis. A reporter gene assay was performed to determine the growth signaling pathway regulated by NME1L but none of the growth factors tested could induce an NF-B-dependent luciferase expression except TNF. Interestingly, SRE-reporter gene activation by IGF1 was significantly downregulated, along with reduction of ERK phosphorylation in NME1L expressing cells, compared to vector or NME1 expressing cells. NME1L directly interacted with KSR1, which is a scaffold for Raf-1, MEK, and ERK, that regulates ERK activation. Hence, NME1L plays a crucial role in regulation of cell proliferation by inhibiting IGF1-stimulated ERK phosphorylation through N-terminal 25 amino acid-mediated interaction with KSR1. J. Cell. Biochem. 117: 1454-1463, 2016. (c) 2015 Wiley Periodicals, Inc.
URI
http://pubs.kist.re.kr/handle/201004/65034
ISSN
0730-2312
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