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Targeting nuclear factor‐κ B suppresses the negative effect of T oll‐like receptor 4 signaling on antimetastasis therapy based on targeting αvβ3
Author(s) -
Zhu JianHua,
Yuan Ye,
Li Dong,
Liao ShengJun,
Zhou YuanHong,
Wang Qi,
Shu Yu,
Yan Bin,
Wei JingJing,
Sun Rui,
Zhang GuiMei,
Feng ZuoHua
Publication year - 2012
Publication title -
cancer science
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.035
H-Index - 141
eISSN - 1349-7006
pISSN - 1347-9032
DOI - 10.1111/j.1349-7006.2012.02299.x
Subject(s) - tlr4 , extravasation , cancer research , metastasis , in vivo , receptor , chemistry , medicine , pharmacology , immunology , biology , cancer , microbiology and biotechnology
The targeting of αvβ3 is a promising therapeutic strategy for suppressing tumor metastasis. However, it is unclear whether the therapeutic efficacy could be influenced by metastasis‐promoting factor(s) in vivo . Here we report that Toll‐like receptor 4 ( TLR 4) ligand released from damaged tumor cells or bacteria had a negative effect on the therapeutic effect of a recombinant CBD ‐Hep II polypeptide of fibronectin ( CH 50) that suppresses tumor metastasis by targeting αvβ3. The TLR 4 ligand could antagonize the inhibitory effect of CH 50 on tumor cell adhesion and invasion by promoting the expression and activity of αvβ3 in tumor cells. The TLR 4 ligand also reduced the antimetastasis effect of CH 50 by promoting tumor cell survival in circulation. Moreover, TLR 4 ligands released by tumor cells in circulation could increase the survival and proliferation capacity of tumor cells after extravasation, resulting in the formation of more metastatic nodules. The effect of TLR 4 signaling was mainly mediated by nuclear factor‐κB ( NF ‐κB). Inhibiting NF ‐κB could abrogate the negative effect of TLR 4 ligand, and augment the inhibitory effect of CH 50 on tumor metastasis. Consistently, the combination of NF ‐κB inhibitor and CH 50 significantly inhibited metastasis of tumor cells in vivo and prolonged the survival of mice. The findings in this study suggest that the combination of NF ‐κB inhibitor and αvβ3 antagonist would be a novel therapeutic option for the prevention of tumor metastasis. ( Cancer Sci 2012; 103: 1319–1326)

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