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Experimental Therapeutics |
Department of Nuclear Receptor Discovery, Ligand Pharmaceuticals Inc., San Diego, California 92121
Targretin (LGD1069; a high-affinity ligand for the retinoid X receptors)
is an efficacious chemotherapeutic and chemopreventive agent in the
N-nitroso-N-methylurea-induced rat
mammary carcinoma model. To evaluate the molecular action of LGD1069 in
mammary carcinoma we have examined gene expression patterns in controls
and nonresponding tumors compared with tumors undergoing regression
(responding) by LGD1069. When compared with controls or nonresponding
tumors, the expression of adipocyte-related genes such as
adipocyte P2 (aP2), adipsin, peroxisome
proliferator-activated receptor
(PPAR
), and
lipoprotein lipase was elevated in LGD1069-responding tumors. Further
analysis showed that gene expression changes occurred rapidly, in as
little as 6 h, after the first dose of LGD1069.
Immunohistochemical analysis showed that aP2 protein was also highly
expressed in responding tumors when compared with control or
nonresponding tumors. More importantly, aP2 protein was localized in
the tumor cells in addition to the adipocytes present in the tumors.
Similar changes in gene expression and inhibition in growth were seen
in tumor cells (cloned from
N-nitroso-N-methylurea-induced carcinoma)
exposed to LGD1069 in vitro. These data suggest that
tumor regression by LGD1069 involves differentiation induction along
the adipocyte lineage.
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