| Literature DB >> 24891954 |
Karli Rosner1, Darius R Mehregan2, Evangelia Kirou3, Judith Abrams4, Seongho Kim4, Michelle Campbell5, Jillian Frieder6, Kelsey Lawrence6, Brittany Haynes7, Malathy P V Shekhar8.
Abstract
We have previously demonstrated that Rad6 and β -catenin enhance each other's expression through a positive feedback loop to promote breast cancer development/progression. While β -catenin has been implicated in melanoma pathogenesis, Rad6 function has not been investigated. Here, we examined the relationship between Rad6 and β -catenin in melanoma development and progression. Eighty-eight cutaneous tumors, 30 nevi, 29 primary melanoma, and 29 metastatic melanomas, were immunostained with anti- β -catenin and anti-Rad6 antibodies. Strong expression of Rad6 was observed in only 27% of nevi as compared to 100% of primary and 96% of metastatic melanomas. β -Catenin was strongly expressed in 97% of primary and 93% of metastatic melanomas, and unlike Rad6, in 93% of nevi. None of the tumors expressed nuclear β -catenin. β -Catenin was exclusively localized on the cell membrane of 55% of primary, 62% of metastatic melanomas, and only 10% of nevi. Cytoplasmic β -catenin was detected in 90% of nevi, 17% of primary, and 8% of metastatic melanoma, whereas 28% of primary and 30% of metastatic melanomas exhibited β -catenin at both locations. These data suggest that melanoma development and progression are associated with Rad6 upregulation and membranous redistribution of β -catenin and that β -catenin and Rad6 play independent roles in melanoma development.Entities:
Year: 2014 PMID: 24891954 PMCID: PMC4033428 DOI: 10.1155/2014/439205
Source DB: PubMed Journal: J Skin Cancer ISSN: 2090-2913
Association of melanocytic nevi and melanoma with demographic characteristics of the patients.
| Melanocytic tumor type and subtype | No. Cases | Gender | Age | |||
|---|---|---|---|---|---|---|
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| Total | M | F | Median (Range) | ||
| Nevi | Junctional nevus | 5 | 30 | 11 | 19 | 43 (33–53) |
| Intradermal nevus | 7 | |||||
| Compound nevus | 10 | |||||
| Atypical nevus | 8 | |||||
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| PM | SSMM | 17 | 29 | 14 | 15 | 58 (48–68) |
| Nodular Melanoma | 7 | |||||
| Lentigo Malignant Melanoma | 5 | |||||
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| MM | Metastatic Melanoma | 29 | 29 | 19 | 10 | 67 (58–76) |
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| significance |
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M: male; F: female; CI: confidence interval; PM: primary melanoma; MM: metastatic melanoma; SSM: superficial spreading melanoma.
Rad6 positive cells by age groups.
| Age (years) |
| Rad6 Percent Median (IQR) |
|---|---|---|
| <50 | 31 | 65 (0, 96) |
| 50–60 | 16 | 86 (24, 95) |
| >60 | 38 | 96 (88, 100) |
N: number of patients, IQR: interquartile range.
Figure 1Representative pictures of β-catenin ((a)–(c)) and Rad6 ((d)–(f)) staining in nevus ((a), (d)), primary melanoma ((b), (e)), and metastatic melanoma ((c), (f)). Closed arrowheads point to positively immunostained cells. The highlighted square in panel (c) is magnified. Original magnification ×400.
Figure 2Percentages of nevi, primary melanomas, and metastatic melanomas with Rad6 and β-catenin positive cells shown in increments of 10 percentage points.
Figure 3Boxplots of Rad6 and β-catenin positive cells in nevi, primary melanoma (PM), and metastatic melanoma (MM). Kruskal-Wallis tests showed that there are significantly more Rad6 positive cells in primary and metastatic melanomas as compared to nevi. Median values are indicated by gray horizontal lines.
Figure 4Subcellular localization of β-catenin in nevi, primary melanomas (PM), and metastatic melanomas (MM). Percentages of tumors expressing β-catenin exclusively in the cytoplasm or on cell membrane, or in both compartments.