Title of article :
Synergy between PPARγ Ligands and Platinum-Based Drugs in Cancer
Author/Authors :
Geoffrey D. Girnun، نويسنده , , Geoffrey D. and Naseri، نويسنده , , Elnaz and Vafai، نويسنده , , Scott B. and Qu، نويسنده , , Lishu and Szwaya، نويسنده , , Jeffrey D. and Bronson، نويسنده , , Roderick and Alberta، نويسنده , , John A. and Spiegelman، نويسنده , , Bruce M.، نويسنده ,
Issue Information :
روزنامه با شماره پیاپی سال 2007
Pages :
12
From page :
395
To page :
406
Abstract :
Summary is a member of the nuclear receptor family for which agonist ligands have antigrowth effects. However, clinical studies using PPARγ ligands as a monotherapy failed to show a beneficial effect. Here we have studied the effects of PPARγ activation with chemotherapeutic agents in current use for specific cancers. We observed a striking synergy between rosiglitazone and platinum-based drugs in several different cancers both in vitro and using transplantable and chemically induced “spontaneous” tumor models. The effect appears to be due in part to PPARγ-mediated downregulation of metallothioneins, proteins that have been shown to be involved in resistance to platinum-based therapy. These data strongly suggest combining PPARγ agonists and platinum-based drugs for the treatment of certain human cancers.
Keywords :
CELLCYCLE , Signaling
Journal title :
Cancer Cell
Serial Year :
2007
Journal title :
Cancer Cell
Record number :
1336444
Link To Document :
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