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:10.1371/journal.pone.0019330

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

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Abstract

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.

Original language	English
Article number	e19330
Journal	PL o S One
Volume	6
Issue number	4
DOIs	https://doi.org/10.1371/journal.pone.0019330
Publication status	Published - 2011

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Gilbert, A. E., Karagiannis, P., Dodev, T., Koers, A., Lacy, K., Josephs, D. H., Takhar, P., Geh, J. L. C., Healy, C., Harries, M., Acland, K. M., Rudman, S. M., Beavil, R. L., Blower, P. J., Beavil, A. J., Gould, H. J., Spicer, J., Nestle, F. O., & Karagiannis, S. N. (2011). Monitoring the Systemic Human Memory B Cell Compartment of Melanoma Patients for Anti-Tumor IgG Antibodies. PL o S One , 6(4), Article e19330. https://doi.org/10.1371/journal.pone.0019330

@article{e37b248982524ad99e83b5527f03bd29,

title = "Monitoring the Systemic Human Memory B Cell Compartment of Melanoma Patients for Anti-Tumor IgG Antibodies",

abstract = "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.",

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

year = "2011",

doi = "10.1371/journal.pone.0019330",

language = "English",

volume = "6",

journal = "PL o S One ",

issn = "1932-6203",

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Gilbert, AE, Karagiannis, P, Dodev, T, Koers, A, Lacy, K, Josephs, DH, Takhar, P, Geh, JLC, Healy, C, Harries, M, Acland, KM, Rudman, SM , Beavil, RL , Blower, PJ , Beavil, AJ , Gould, HJ , Spicer, J , Nestle, FO & Karagiannis, SN 2011, 'Monitoring the Systemic Human Memory B Cell Compartment of Melanoma Patients for Anti-Tumor IgG Antibodies', PL o S One , vol. 6, no. 4, e19330. https://doi.org/10.1371/journal.pone.0019330

TY - JOUR

T1 - Monitoring the Systemic Human Memory B Cell Compartment of Melanoma Patients for Anti-Tumor IgG Antibodies

AU - Gilbert, Amy E.

AU - Karagiannis, Panagiotis

AU - Dodev, Tihomir

AU - Koers, Alexander

AU - Lacy, Katie

AU - Josephs, Debra H.

AU - Takhar, Pooja

AU - Geh, Jenny L. C.

AU - Healy, Ciaran

AU - Harries, Mark

AU - Acland, Katharine M.

AU - Rudman, Sarah M.

AU - Beavil, Rebecca L.

AU - Blower, Philip J.

AU - Beavil, Andrew J.

AU - Gould, Hannah J.

AU - Spicer, James

AU - Nestle, Frank O.

AU - Karagiannis, Sophia N

PY - 2011

Y1 - 2011

N2 - 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.

AB - 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.

U2 - 10.1371/journal.pone.0019330

DO - 10.1371/journal.pone.0019330

M3 - Article

SN - 1932-6203

VL - 6

JO - PL o S One

JF - PL o S One

IS - 4

M1 - e19330

ER -

Monitoring the Systemic Human Memory B Cell Compartment of Melanoma Patients for Anti-Tumor IgG Antibodies

Abstract

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