Identification of Distinct Changes in Gene Expression after Modulation of Melanoma Tumor Antigen p97 (Melanotransferrin) in Multiple Models In Vitro and In Vivo

doi:10.1093/carcin/bgm096

Carcinogenesis Advance Access published online on April 21, 2007
Carcinogenesis, doi:10.1093/carcin/bgm096

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Identification of Distinct Changes in Gene Expression after Modulation of Melanoma Tumor Antigen p97 (Melanotransferrin) in Multiple Models In Vitro and In Vivo

Y Suryo Rahmanto, LL Dunn and DR Richardson^*

Iron Metabolism and Chelation Program, Department of Pathology, Blackburn Building D06, University of Sydney, Sydney, New South Wales, 2006 Australia

^* Author for Correspondence: Dr. D. R. Richardson, Iron Metabolism and Chelation Program, Department of Pathology, University of Sydney, Sydney, New South Wales, 2006 Australia. Ph: +61-2-9036-6548; FAX:+ 61-2-9036-6549; Email: d.richardson{at}pathology.usyd.edu.au

Melanoma tumor antigen p97 or melanotransferrin (MTf) is aniron (Fe)-binding protein with high homology to serum transferrin.MTf is expressed at very low levels in normal tissues and inhigh amounts in melanoma cells although its function remainselusive. To understand the function of MTf, we utilized whole-genomemicroarray analysis to examine the gene expression profile offive models after modulating MTf expression. These models includedtwo new stably transfected MTf hyper-expression models (SK-N-MCneuroepithelioma and LMTK^– fibroblasts) and one cell type(SK-Mel-28 melanoma) where MTf was down-regulated by post-transcriptionalgene silencing. These findings were compared to alterationsin gene expression identified using the MTf ^–/–mouse. In addition, the changes identified from the microarraydata were also assessed in a new model of MTf down-regulationin SK-Mel-2 melanoma cells. In the cell line models, MTf hyper-expressionled to increased proliferation, while MTf down-regulation resultedin decreased proliferation. Across all five models of MTf down-and up-regulation, we identified three genes modulated by MTf.These included ATP-binding cassette sub-family B member 5 (Abcb5),whose change in expression mirrored MTf down- or up-regulation.In addition, thiamine triphosphatase (Thtpa) and transcriptionfactor 4 (Tcf4) were inversely expressed relative to MTf levelsacross all five models. The products of these three genes areinvolved in membrane transport, thiamine phosphorylation andproliferation/survival, respectively. This study identifiesnovel molecular targets directly or indirectly regulated byMTf and the potential pathways involved in its function, includingmodulation of proliferation.

Received January 23, 2007; revised March 17, 2007; accepted April 11, 2007.

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