Expression of the Cancer/testis Antigen NY-ESO-1 in Primary and Metastatic Malignant Melanoma (MM)--correlation with Prognostic Factors

Overview

Journal Cancer Immun

Specialties Allergy & Immunology
Oncology

Date 2007 Jul 13

PMID 17625806

Citations 60

Authors

Elsa F Velazquez

Achim A Jungbluth

Molly Yancovitz

Sacha Gnjatic

Sylvia Adams

David ONeill

Kira Zavilevich

Tatyana Albukh

Paul Christos

Madhu Mazumdar

Anna Pavlick

David Polsky

Richard Shapiro

Russell Berman

Joanna Spira

Klaus Busam

Iman Osman

Nina Bhardwaj

Affiliations

Soon will be listed here.

Abstract

Cancer/testis (CT) antigens are potential targets for cancer immunotherapy, with NY-ESO-1 being among the most immunogenic. In several clinical trials in malignant melanoma (MM) patients, NY-ESO-1 protein/peptides showed clear evidence of inducing specific immunity. However, little is known about NY-ESO-1 expression in primary and metastatic MM and its relationship to disease progression. We analyzed NY-ESO-1 expression immunohistochemically in a series of primary and metastatic MMs and its relation to prognostic parameters and survival. We studied 61 primary and 63 metastatic MM specimens (from 61 and 56 patients, respectively). The prevalence of NY-ESO-1 expression was significantly higher in metastatic versus primary tumors [18/56 (32%) versus 8/61 (13%), P = 0.015]. There was a significant association between initial stage at presentation and NY-ESO-1 expression [stage I (3.45%), stage II (9.52%) and stage III (45.45%), P = 0.0014]. Primary MMs expressing NY-ESO-1 were significantly thicker than NY-ESO-1 negative cases (median thickness 4.7 mm versus 1.53 mm respectively, P = 0.03). No significant difference was seen in overall survival. In conclusion, NY-ESO-1 is more frequently expressed in metastatic than in primary MM and its expression is associated with thicker primary lesions and a higher frequency of metastatic disease, indicative of a worse prognosis. Our study suggests that patients with metastatic MM who express NY-ESO-1 may benefit from NY-ESO-1-based immunotherapy.

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