E-Cadherin–dependent Growth Suppression is Mediated by the Cyclin-dependent Kinase Inhibitor p27KIP1
摘要:
Recent studies have demonstrated the importance of E-cadherin, a homophilic cell-cell adhesion molecule, in contact inhibition of growth of normal epithelial cells. Many tumor cells also maintain strong intercellular adhesion, and are growth-inhibited by cell-cell contact, especially when grown in three-dimensional culture. To determine if E-cadherin could mediate contact-dependent growth inhibition of nonadherent EMT/6 mouse mammary carcinoma cells that lack E-cadherin, we transfected these cells with an exogenous E-cadherin expression vector. E-cadherin expression in EMT/6 cells resulted in tighter adhesion of multicellular spheroids and a reduced proliferative fraction in three-dimensional culture. In addition to increased cell-cell adhesion, E-cadherin expression also resulted in dephosphorylation of the retinoblastoma protein, an increase in the level of the cyclin-dependent kinase inhibitor p27kip1 and a late reduction in cyclin D1 protein. Tightly adherent spheroids also showed increased levels of p27 bound to the cyclin E-cdk2 complex, and a reduction in cyclin E-cdk2 activity. Exposure to E-cadherin-neutralizing antibodies in three-dimensional culture simultaneously prevented adhesion and stimulated proliferation of E-cadherin transfectants as well as a panel of human colon, breast, and lung carcinoma cell lines that express functional E-cadherin. To test the importance of p27 in E-cadherin-dependent growth inhibition, we engineered E-cadherin-positive cells to express inducible p27. By forcing expression of p27 levels similar to those observed in aggregated cells, the stimulatory effect of E-cadherin-neutralizing antibodies on proliferation could be inhibited. This study demonstrates that E-cadherin, classically described as an invasion suppressor, is also a major growth suppressor, and its ability to inhibit proliferation involves upregulation of the cyclin-dependent kinase inhibitor p27.
展开
DOI:
10.1083/jcb.142.2.557
被引量:
年份:
1998
万方
Wiley
掌桥科研
Semantic Scholar
Semantic Scholar
(全网免费下载)
查看更多
万方医学
dx.doi.org
Oxford Univ Press
NCBI
JSTOR
Pubmed Central
(全网免费下载)
Europe PMC
(全网免费下载)
NCBI
Europe PMC
AACR
JBC
ResearchGate
(全网免费下载)
EureKaMag.com
(全网免费下载)
ResearchGate
ProQuest
Citeseer
(全网免费下载)
EBSCO
Citeseer
EBSCO
journalacs.org
jacionline.org
mendeley.com
jcs.biologists.org
gastrojournal.org
jasn.asnjournals.org
jleukbio.org
jcb.rupress.org
molpharm.aspetjournals.org
scienceopen.com
fasebj.org
bloodjournal.org
molbiolcell.org
mcb.asm.org
rupress.org
biomedsearch.com
(全网免费下载)
SAGE
jme.endocrinology-journals.org
www.socolar.com
mysciencework.com
ajpendo.physiology.org
emboj.embopress.org
deepdyve.com
ar.iiarjournals.org
rsif.royalsocietypublishing.org
miami.pure.elsevier.com
onAcademic
bvsalud.org
jcb.rupress.org
(全网免费下载)
core.ac.uk
Semantic Scholar
(全网免费下载)
Pubmed Central
(全网免费下载)
Europe PMC
(全网免费下载)
ResearchGate
(全网免费下载)
EureKaMag.com
(全网免费下载)
Citeseer
(全网免费下载)
jcb.rupress.org
(全网免费下载)
biomedsearch.com
(全网免费下载)
通过文献互助平台发起求助,成功后即可免费获取论文全文。
相似文献
参考文献
引证文献
引用走势
辅助模式
引用
文献可以批量引用啦~
欢迎点我试用!
