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Molecular prognostic markers in intermediate-thickness cutaneous malignant melanoma

✍ Scribed by Tina J. Hieken; Salve G. Ronan; Miguel Farolan; Anne L. Shilkaitis; Tapas K. Das Gupta


Publisher
John Wiley and Sons
Year
1999
Tongue
English
Weight
233 KB
Volume
85
Category
Article
ISSN
0008-543X

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✦ Synopsis


Background:

The limitations of morphologic criteria alone in determining the prognosis for a patient with a particular intermediate-thickness primary melanoma have prompted efforts to identify other markers.

Methods:

In this study, the authors analyzed expression of p53, beta1 integrin, and beta3 integrin in primary tumors from 111 patients with intermediate-thickness malignant melanoma.

Results:

Eighty-nine (80%) had detectable p53 protein, 58 (52%) expressed beta1 integrin, and 71 (64%) expressed beta3 integrin. patients with beta3 positive melanomas were more likely to die of their disease (32 of 71 patients, 45%) than those with beta3 negative tumors (3 of 40 patients, 8%) (p < 0.0001). the number of involved lymph nodes, clark's level, beta1 integrin expression, thickness, and mitotic rate also had prognostic significance. beta3 integrin was associated with subsequent lung metastases and beta1 integrin with lymph node involvement.

Conclusions:

Integrin expression, along with histopathologic criteria, is a prognostic marker for intermediate-thickness malignant melanoma and may indicate the site of subsequent metastasis. these observations may have clinical utility and suggest areas for future investigation.


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