Melanoma antigen family A identified by the bimodality index defines a subset of triple negative breast cancers as candidates for immune response augmentation

Thomas Karn; Lajos Pusztai; Eugen Ruckhäberle; Cornelia Liedtke; Volkmar Müller; Marcus Schmidt; Dirk Metzler; Jing Wang; Kevin R. Coombes; Regine Gätje; Lars Hanker; Christine Solbach; Andre Ahr; Uwe Holtrich; Achim Rody; Manfred Kaufmann

doi:10.1016/j.ejca.2011.06.025

Melanoma antigen family A identified by the bimodality index defines a subset of triple negative breast cancers as candidates for immune response augmentation

Thomas Karn, Lajos Pusztai, Eugen Ruckhäberle, Cornelia Liedtke, Volkmar Müller, Marcus Schmidt, Dirk Metzler, Jing Wang, Kevin R. Coombes, Regine Gätje, Lars Hanker, Christine Solbach, Andre Ahr, Uwe Holtrich, Achim Rody, Manfred Kaufmann

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37 Scopus citations

Abstract

Background: Molecular markers displaying bimodal expression distribution can reveal distinct disease subsets and may serve as prognostic or predictive markers or represent therapeutic targets. Oestrogen (ER) and human epidermal growth factor receptor 2 (HER2) receptors are strongly bimodally expressed genes in breast cancer. Material and methods: We applied a novel method to identify bimodally expressed genes in 394 triple negative breast cancers (TNBC). We identified 133 bimodally expressed probe sets (128 unique genes), 69 of these correlated to previously reported metagenes that define molecular subtypes within TNBC including basal-like, molecular-apocrine, claudin-low and immune cell rich subgroups but 64 probe sets showed no correlation with these features. Results: The single most prominent functional group among these uncorrelated genes was the X chromosome derived Cancer/Testis Antigens (CT-X) including melanoma antigen family A (MAGE-A) and Cancer/Testis Antigens (CTAG). High expression of CT-X genes correlated with worse survival in multivariate analysis (HR 2.02, 95% CI 1.27-3.20; P = 0.003). The only other significant variable was lymph node status. The poor prognosis of patients with high MAGE-A expression was ameliorated by the concomitant high expression of immune cell metagenes (HR 1.87, 95% CI 0.96-3.64; P = 0.060), whereas the same immune metagene had lesser prognostic value in TNBC with low MAGE-A expression. Conclusions: MAGE-A antigen defines a very aggressive subgroup of TNBC; particularly in the absence of immune infiltration in the tumour microenvironment. These observations suggest a therapeutic hypothesis; TNBC with MAGE-A expression may benefit the most from further augmentation of the immune response. Novel immune stimulatory drugs such as (anti-cytotoxic T-lymphocyte antigen-4 CTLA-4) directed therapies provide a realistic opportunity to directly test this hypothesis in the clinic.

Original language	English (US)
Pages (from-to)	12-23
Number of pages	12
Journal	European Journal of Cancer
Volume	48
Issue number	1
DOIs	https://doi.org/10.1016/j.ejca.2011.06.025
State	Published - Jan 2012
Externally published	Yes

Keywords

Bimodal expression
CT-X antigens
Immune therapy
Microarray analysis
Prognostic markers
Subtypes of breast cancer

ASJC Scopus subject areas

Oncology
Cancer Research

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1016/j.ejca.2011.06.025

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Karn, T., Pusztai, L., Ruckhäberle, E., Liedtke, C., Müller, V., Schmidt, M., Metzler, D., Wang, J., Coombes, K. R., Gätje, R., Hanker, L., Solbach, C., Ahr, A., Holtrich, U., Rody, A., & Kaufmann, M. (2012). Melanoma antigen family A identified by the bimodality index defines a subset of triple negative breast cancers as candidates for immune response augmentation. European Journal of Cancer, 48(1), 12-23. https://doi.org/10.1016/j.ejca.2011.06.025

Karn, T, Pusztai, L, Ruckhäberle, E, Liedtke, C, Müller, V, Schmidt, M, Metzler, D, Wang, J, Coombes, KR, Gätje, R, Hanker, L, Solbach, C, Ahr, A, Holtrich, U, Rody, A & Kaufmann, M 2012, 'Melanoma antigen family A identified by the bimodality index defines a subset of triple negative breast cancers as candidates for immune response augmentation', European Journal of Cancer, vol. 48, no. 1, pp. 12-23. https://doi.org/10.1016/j.ejca.2011.06.025

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title = "Melanoma antigen family A identified by the bimodality index defines a subset of triple negative breast cancers as candidates for immune response augmentation",

abstract = "Background: Molecular markers displaying bimodal expression distribution can reveal distinct disease subsets and may serve as prognostic or predictive markers or represent therapeutic targets. Oestrogen (ER) and human epidermal growth factor receptor 2 (HER2) receptors are strongly bimodally expressed genes in breast cancer. Material and methods: We applied a novel method to identify bimodally expressed genes in 394 triple negative breast cancers (TNBC). We identified 133 bimodally expressed probe sets (128 unique genes), 69 of these correlated to previously reported metagenes that define molecular subtypes within TNBC including basal-like, molecular-apocrine, claudin-low and immune cell rich subgroups but 64 probe sets showed no correlation with these features. Results: The single most prominent functional group among these uncorrelated genes was the X chromosome derived Cancer/Testis Antigens (CT-X) including melanoma antigen family A (MAGE-A) and Cancer/Testis Antigens (CTAG). High expression of CT-X genes correlated with worse survival in multivariate analysis (HR 2.02, 95% CI 1.27-3.20; P = 0.003). The only other significant variable was lymph node status. The poor prognosis of patients with high MAGE-A expression was ameliorated by the concomitant high expression of immune cell metagenes (HR 1.87, 95% CI 0.96-3.64; P = 0.060), whereas the same immune metagene had lesser prognostic value in TNBC with low MAGE-A expression. Conclusions: MAGE-A antigen defines a very aggressive subgroup of TNBC; particularly in the absence of immune infiltration in the tumour microenvironment. These observations suggest a therapeutic hypothesis; TNBC with MAGE-A expression may benefit the most from further augmentation of the immune response. Novel immune stimulatory drugs such as (anti-cytotoxic T-lymphocyte antigen-4 CTLA-4) directed therapies provide a realistic opportunity to directly test this hypothesis in the clinic.",

keywords = "Bimodal expression, CT-X antigens, Immune therapy, Microarray analysis, Prognostic markers, Subtypes of breast cancer",

author = "Thomas Karn and Lajos Pusztai and Eugen Ruckh{\"a}berle and Cornelia Liedtke and Volkmar M{\"u}ller and Marcus Schmidt and Dirk Metzler and Jing Wang and Coombes, {Kevin R.} and Regine G{\"a}tje and Lars Hanker and Christine Solbach and Andre Ahr and Uwe Holtrich and Achim Rody and Manfred Kaufmann",

note = "Funding Information: We thank Katherina Kourtis and Samira Adel for expert technical assistance. This work was supported by grants from the the H.W. & J. Hector-Stiftung, Mannheim ; the Margarete Bonifer-Stiftung, Bad Soden ; the BANSS-Stiftung, Biedenkopf ; and the Dr. Robert Pfleger-Stiftung, Bamberg . These foundations had no role in planning of the study and writing of the manuscript. ",

year = "2012",

month = jan,

doi = "10.1016/j.ejca.2011.06.025",

language = "English (US)",

volume = "48",

pages = "12--23",

journal = "European Journal of Cancer",

issn = "0959-8049",

publisher = "Elsevier Limited",

number = "1",

}

TY - JOUR

T1 - Melanoma antigen family A identified by the bimodality index defines a subset of triple negative breast cancers as candidates for immune response augmentation

AU - Karn, Thomas

AU - Pusztai, Lajos

AU - Ruckhäberle, Eugen

AU - Liedtke, Cornelia

AU - Müller, Volkmar

AU - Schmidt, Marcus

AU - Metzler, Dirk

AU - Wang, Jing

AU - Coombes, Kevin R.

AU - Gätje, Regine

AU - Hanker, Lars

AU - Solbach, Christine

AU - Ahr, Andre

AU - Holtrich, Uwe

AU - Rody, Achim

AU - Kaufmann, Manfred

N1 - Funding Information: We thank Katherina Kourtis and Samira Adel for expert technical assistance. This work was supported by grants from the the H.W. & J. Hector-Stiftung, Mannheim ; the Margarete Bonifer-Stiftung, Bad Soden ; the BANSS-Stiftung, Biedenkopf ; and the Dr. Robert Pfleger-Stiftung, Bamberg . These foundations had no role in planning of the study and writing of the manuscript.

PY - 2012/1

Y1 - 2012/1

N2 - Background: Molecular markers displaying bimodal expression distribution can reveal distinct disease subsets and may serve as prognostic or predictive markers or represent therapeutic targets. Oestrogen (ER) and human epidermal growth factor receptor 2 (HER2) receptors are strongly bimodally expressed genes in breast cancer. Material and methods: We applied a novel method to identify bimodally expressed genes in 394 triple negative breast cancers (TNBC). We identified 133 bimodally expressed probe sets (128 unique genes), 69 of these correlated to previously reported metagenes that define molecular subtypes within TNBC including basal-like, molecular-apocrine, claudin-low and immune cell rich subgroups but 64 probe sets showed no correlation with these features. Results: The single most prominent functional group among these uncorrelated genes was the X chromosome derived Cancer/Testis Antigens (CT-X) including melanoma antigen family A (MAGE-A) and Cancer/Testis Antigens (CTAG). High expression of CT-X genes correlated with worse survival in multivariate analysis (HR 2.02, 95% CI 1.27-3.20; P = 0.003). The only other significant variable was lymph node status. The poor prognosis of patients with high MAGE-A expression was ameliorated by the concomitant high expression of immune cell metagenes (HR 1.87, 95% CI 0.96-3.64; P = 0.060), whereas the same immune metagene had lesser prognostic value in TNBC with low MAGE-A expression. Conclusions: MAGE-A antigen defines a very aggressive subgroup of TNBC; particularly in the absence of immune infiltration in the tumour microenvironment. These observations suggest a therapeutic hypothesis; TNBC with MAGE-A expression may benefit the most from further augmentation of the immune response. Novel immune stimulatory drugs such as (anti-cytotoxic T-lymphocyte antigen-4 CTLA-4) directed therapies provide a realistic opportunity to directly test this hypothesis in the clinic.

AB - Background: Molecular markers displaying bimodal expression distribution can reveal distinct disease subsets and may serve as prognostic or predictive markers or represent therapeutic targets. Oestrogen (ER) and human epidermal growth factor receptor 2 (HER2) receptors are strongly bimodally expressed genes in breast cancer. Material and methods: We applied a novel method to identify bimodally expressed genes in 394 triple negative breast cancers (TNBC). We identified 133 bimodally expressed probe sets (128 unique genes), 69 of these correlated to previously reported metagenes that define molecular subtypes within TNBC including basal-like, molecular-apocrine, claudin-low and immune cell rich subgroups but 64 probe sets showed no correlation with these features. Results: The single most prominent functional group among these uncorrelated genes was the X chromosome derived Cancer/Testis Antigens (CT-X) including melanoma antigen family A (MAGE-A) and Cancer/Testis Antigens (CTAG). High expression of CT-X genes correlated with worse survival in multivariate analysis (HR 2.02, 95% CI 1.27-3.20; P = 0.003). The only other significant variable was lymph node status. The poor prognosis of patients with high MAGE-A expression was ameliorated by the concomitant high expression of immune cell metagenes (HR 1.87, 95% CI 0.96-3.64; P = 0.060), whereas the same immune metagene had lesser prognostic value in TNBC with low MAGE-A expression. Conclusions: MAGE-A antigen defines a very aggressive subgroup of TNBC; particularly in the absence of immune infiltration in the tumour microenvironment. These observations suggest a therapeutic hypothesis; TNBC with MAGE-A expression may benefit the most from further augmentation of the immune response. Novel immune stimulatory drugs such as (anti-cytotoxic T-lymphocyte antigen-4 CTLA-4) directed therapies provide a realistic opportunity to directly test this hypothesis in the clinic.

KW - Bimodal expression

KW - CT-X antigens

KW - Immune therapy

KW - Microarray analysis

KW - Prognostic markers

KW - Subtypes of breast cancer

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Melanoma antigen family A identified by the bimodality index defines a subset of triple negative breast cancers as candidates for immune response augmentation

Abstract

Keywords

ASJC Scopus subject areas

UN SDGs

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