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Peter J. Wild, MD; Stefanie Meyer, MD; Frauke Bataille, MD; Matthias Woenckhaus, MD; Markus Ameres, MD; Thomas Vogt, MD; Michael Landthaler, MD; Armin Pauer; Monika Klinkhammer-Schalke, MD; Ferdinand Hofstaedter, MD; Anja K. Bosserhoff, PhD

Arch Dermatol. 2006;142:471-476.

Background  Using tissue microarrays, we investigated whether methylthioadenosine phosphorylase (MTAP) protein expression is associated with clinicopathologic variables in benign and malignant melanocytic skin tumors.

Observations  Cytoplasmic MTAP expression was detected in 227 (72.1%) of 315 informative cases. Expression was significantly reduced in primary malignant melanomas and in melanoma metastases compared with benign nevi (P<.001 for both). No difference was noted in MTAP expression between primary malignant melanomas and melanoma metastases. In primary malignant melanomas, a Ki67-labeling index less than 5% was associated with MTAP expression (P = .04), suggesting that loss of MTAP expression is associated with proliferation. No other variables had significant associations with MTAP expression. Lymph node metastases demonstrated significantly higher MTAP expression compared with skin metastases (P = .01). In the overall cohort, MTAP expression was not associated with prognosis. Among 26 patients with MTAP-positive melanomas and tumor recurrence, 18 patients who received interferon therapy had a significant benefit compared with 8 patients who did not receive interferon therapy (P = .009). This was not seen in the patients with MTAP-negative tumors.

Conclusion  Methylthioadenosine phosphorylase protein expression may be a predictive marker of interferon therapy resistance in patients with melanoma and disease progression.

Author Affiliations: Institute of Pathology (Drs Wild, Bataille, Woenckhaus, Hofstaedter, and Bosserhoff) and Department of Dermatology (Drs Meyer, Ameres, Vogt, and Landthaler), University of Regensburg, and Central Tumor Registry (Mr Pauer and Drs Klinkhammer-Schalke and Hofstaedter), Regensburg, Germany.