WNT5A Expression Increases during Melanoma Progression and Correlates with Outcome

Purpose: Wnt ligands play a major role in development and are important in cancer. Expression microarray analysis correlates one member of this family, WNT5A, to a subclass of melanomas with increased motility and invasion. There are no large studies of clinical samples primarily addressing the impo...

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Veröffentlicht in:Clinical cancer research 2008-09, Vol.14 (18), p.5825-5832
Hauptverfasser: DA FORNO, Philip D, PRINGLE, J. Howard, HUTCHINSON, Peter, OSBORN, Joy, QIANG HUANG, POTTER, Linda, HANCOX, Rachael A, FLETCHER, Alan, SALDANHA, Gerald S
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Sprache:eng
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Zusammenfassung:Purpose: Wnt ligands play a major role in development and are important in cancer. Expression microarray analysis correlates one member of this family, WNT5A, to a subclass of melanomas with increased motility and invasion. There are no large studies of clinical samples primarily addressing the importance of WNT5A in melanoma progression or outcome. Therefore, this study aimed to assess the protein expression of WNT5A during melanoma progression and its effect on outcome. Experimental Design: Expression of WNT5A was determined in a series of 59 primary melanomas with matched metastases. To provide a benchmark of progression against which to assess WNT5A, expression of p16 ink4a was analyzed, as this has been previously well documented in melanoma. The effect of WNT5A protein expression on outcome was assessed in 102 melanomas. Results: Cytoplasmic WNT5A showed a trend of increasing expression with melanoma progression ( P = 0.013), whereas there was diminishing p16 ink4a expression ( P = 0.006). Nevi showed relatively strong WNT5A expression. Strong cytoplasmic WNT5A was an independent risk factor for reduced metastasis-free and overall survival in multivariate analysis ( P = 0.001 and 0.003, respectively). Conclusion: Cytoplasmic WNT5A increases with melanoma progression and strong expression is associated with poor outcome.
ISSN:1078-0432
1557-3265
DOI:10.1158/1078-0432.CCR-07-5104