Mutational Analysis of Selected Genes in the TGF{beta}, Wnt, pRb, and p53 Pathways in Primary Uveal Melanoma

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Mutational Analysis of Selected Genes in the TGFß, Wnt, pRb, and p53 Pathways in Primary Uveal Melanoma

Scott C. Edmunds¹^,2, David P. Kelsell¹, John L. Hungerford³ and Ian A. Cree²^,4

^¹ From the Centre for Cutaneous Research, St Bartholomew’s and the London School of Medicine and Dentistry, Queen Mary College, University of London, London, United Kingdom; the ^² Department of Pathology, Institute of Ophthalmology, London, United Kingdom; the ^³ Ocular Oncology Service, St. Bartholomew’s and Moorfields Eye Hospital, London, United Kingdom; and the ^⁴ Translational Oncology Research Centre, Queen Alexandra Hospital, Portsmouth, United Kingdom.

PURPOSE. It is known that the pRb pathway cell-cycle inhibitorp16^INK4A plays a significant role in cutaneous melanoma andthat alteration of p16^INK4A, which resides within the 9p21-22locus that also contains p15^INK4B and p14^ARF, may occur in upto one third of uveal melanomas. The absence of TGFßresponsiveness noted in cultured uveal melanoma cells also suggeststhat the TGFß pathway plays a role in the formationof this tumor. Therefore, mutational screening was performedin several key genes in tumor-suppressor pathways that are knownto be altered in some uveal melanomas.

METHODS. Using denaturing high-performance liquid chromatography(DHPLC) analysis and DNA sequencing, a series of 67 uveal melanomaswere screened for inactivating mutations in the TGFßpathway members Smad4 and TGFß receptor type 2 (TGFßR2),the downstream cell-cycle inhibitor p15^INK4B, and the cell-cycleinhibitors p14^ARF and p16^INK4A. p16^INK4A was also investigatedfor promoter hypermethylation. Mutational analysis was alsoperformed on the Wnt pathway gene ß-catenin, knownto be mutated in approximately one quarter of cutaneous melanomacell lines.

RESULTS. Polymorphisms in p16^INK4A were detected in 3 of 50samples, but no inactivating mutations were detected in anyof the genes screened. Promoter hypermethylation of p16^INK4Awas detected in 5 of 55 tumors, and loss of heterozygosity ofthe p16^INK4A locus was detected in 5 of 16 tumors.

CONCLUSIONS. Most primary uveal melanomas do not appear to containsomatic mutations in Smad4, TGFßR2, p14^ARF, p15^INK4B,p16^INK4A, or ß-catenin. However, methylation of thep16^INK4A promoter and loss of heterozygosity of the p14^ARF-p16^INK4Alocus occurs in some tumors.

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