PLoS ONE (Apr 2011)

Monitoring the systemic human memory B cell compartment of melanoma patients for anti-tumor IgG antibodies.

  • Amy E Gilbert,
  • Panagiotis Karagiannis,
  • Tihomir Dodev,
  • Alexander Koers,
  • Katie Lacy,
  • Debra H Josephs,
  • Pooja Takhar,
  • Jenny L C Geh,
  • Ciaran Healy,
  • Mark Harries,
  • Katharine M Acland,
  • Sarah M Rudman,
  • Rebecca L Beavil,
  • Philip J Blower,
  • Andrew J Beavil,
  • Hannah J Gould,
  • James Spicer,
  • Frank O Nestle,
  • Sophia N Karagiannis

DOI
https://doi.org/10.1371/journal.pone.0019330
Journal volume & issue
Vol. 6, no. 4
p. e19330

Abstract

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Melanoma, a potentially lethal skin cancer, is widely thought to be immunogenic in nature. While there has been much focus on T cell-mediated immune responses, limited knowledge exists on the role of mature B cells. We describe an approach, including a cell-based ELISA, to evaluate mature IgG antibody responses to melanoma from human peripheral blood B cells. We observed a significant increase in antibody responses from melanoma patients (n = 10) to primary and metastatic melanoma cells compared to healthy volunteers (n = 10) (P<0.0001). Interestingly, we detected a significant reduction in antibody responses to melanoma with advancing disease stage in our patient cohort (n = 21) (P<0.0001). Overall, 28% of melanoma patient-derived B cell cultures (n = 1,800) compared to 2% of cultures from healthy controls (n = 600) produced antibodies that recognized melanoma cells. Lastly, a patient-derived melanoma-specific monoclonal antibody was selected for further study. This antibody effectively killed melanoma cells in vitro via antibody-mediated cellular cytotoxicity. These data demonstrate the presence of a mature systemic B cell response in melanoma patients, which is reduced with disease progression, adding to previous reports of tumor-reactive antibodies in patient sera, and suggesting the merit of future work to elucidate the clinical relevance of activating humoral immune responses to cancer.