Curcumin inhibition of STEM cells
Kim HI1, Huang H, Cheepala S, Huang S, Chung J.
Abstract
(integrin (alpha6beta4) - dependent breast cancer cell motility and invasion and reverts cells to apoptosis (normal growth) including HER2)
Curcumin, a
polyphenol natural product isolated from the rhizome of the plant Curcuma
longa, has emerged as a promising anticancer therapeutic agent. However, the
mechanism by which curcumin inhibits cancer cell functions such as cell growth,
survival, and cell motility is largely unknown. We explored whether curcumin
affects the function of integrin alpha(6)beta(4), a laminin adhesion receptor
with an established role in invasion and migration of cancer cells. Here we
show that curcumin significantly reduced alpha(6)beta(4)-dependent breast
cancer cell motility and invasion in a concentration-dependent manner without
affecting apoptosis in MDA-MB-435/beta4 (beta(4)-integrin transfectants) and
MDA-MB-231 breast cancer cell lines. Further, curcumin selectively reduced the
basal phosphorylation of beta(4) integrin (Y1494), which has been reported to
be essential in mediating alpha(6)beta(4)-dependent phosphatidylinositol
3-kinase activation and cell motility. Consistent with this finding, curcumin
also blocked alpha(6)beta(4)-dependent Akt activation and expression of the
cell motility-promoting factor ENPP2 in MDA-MB-435/beta4 cell line. A
multimodality approach using curcumin in combination with other pharmacologic
inhibitors of alpha(6)beta(4) signaling pathways showed an additive effect to
block breast cancer cell motility and invasion. Taken together, these findings
show that curcumin inhibits breast cancer cell motility and invasion by
directly inhibiting the function of alpha(6)beta(4) integrin, and suggest that curcumin
can serve as an effective therapeutic agent in tumors that overexpress
alpha(6)beta(4).
Curcumin inhibition of STEM cells
(integrin (alpha6beta4) - dependent breast cancer cell motility and invasion and reverts cells to apoptosis (normal growth) including HER2)
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