Identification of a melanoma marker derived from melanoma-associated endogenous retroviruses.

Cancer Res

Department of Dermatology, Division of General Dermatology, Green Hills Biotechnology GmbH, Gersthoferstrasse 29-31, 1180 Vienna, Austria.

Published: February 2006

AI Article Synopsis

  • The study investigates the presence of antibodies against melanoma-associated endogenous retrovirus (MERV) proteins in melanoma patients, building on previous research that identified MERV expression in tumors.
  • Researchers used bioinformatics to predict B-cell epitopes on MERV proteins and confirmed an immunodominant peptide in the env protein through analyzing patient sera.
  • Results showed a significant difference in the prevalence of anti-MERV antibodies between melanoma patients and healthy subjects, suggesting the peptide could be a viable target for diagnosis and immunotherapy.

Article Abstract

We previously described the expression of melanoma-associated endogenous retrovirus (MERV) proteins and viral particles in human melanomas and metastases. The objective of the present study was to determine whether a humoral immune response to MERV proteins occurs in melanoma. Candidate B-cell epitopes on MERV proteins were predicted using bioinformatic screening. The reactivity of MERV peptides corresponding to the predicted epitopes with antibodies prevalent in sera of melanoma patients was analyzed. An immunodominant peptide located in the env protein of MERV was identified. Subsequent analyzes using 81 samples from stage I to stage IV melanoma patients and 95 sera from healthy subjects revealed statistically significant differences in seroprevalence of antibodies in melanoma sera samples when compared with reference samples from healthy subjects. The prevalence of anti-MERV antibodies in melanoma patient sera was confirmed by immunofluorescence on env-transfected cells. These data indicate the potential of this candidate peptide as target for diagnosis and immunotherapy.

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Source
http://dx.doi.org/10.1158/0008-5472.CAN-05-2452DOI Listing

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