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Molecular serum portraits in patients with primary breast cancer predict the development of distant metastases

Anders Carlsson, Christer Wingren, Malin Kristensson, Carsten Rose, Mårten Fernö, Håkan Olsson, Helena Jernström, Sara Ek, Elin Gustavsson, Christian Ingvar, Mattias Ohlsson, Carsten Peterson, and Carl A. K. Borrebaeck
PNAS published ahead of print August 15, 2011 https://doi.org/10.1073/pnas.1103125108
Anders Carlsson
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Christer Wingren
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Malin Kristensson
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Carsten Rose
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Mårten Fernö
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Håkan Olsson
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Helena Jernström
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Sara Ek
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Elin Gustavsson
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Christian Ingvar
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Mattias Ohlsson
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Carsten Peterson
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Carl A. K. Borrebaeck
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  1. Edited* by Larry Gold, SomaLogic, Inc., Boulder, CO, and approved July 20, 2011 (received for review February 24, 2011)

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Abstract

The risk of distant recurrence in breast cancer patients is difficult to assess with current clinical and histopathological parameters, and no validated serum biomarkers currently exist. Using a recently developed recombinant antibody microarray platform containing 135 antibodies against 65 mainly immunoregulatory proteins, we screened 240 sera from 64 patients with primary breast cancer. This unique longitudinal sample material was collected from each patient between 0 and 36 mo after the primary operation. The velocity for each serum protein was determined by comparing the samples collected at the primary operation and then 3–6 mo later. A 21-protein signature was identified, using leave-one-out cross-validation together with a backward elimination strategy in a training cohort. This signature was tested and evaluated subsequently in an independent test cohort (prevalidation). The risk of developing distant recurrence after primary operation could be assessed for each patient, using her molecular portraits. The results from this prevalidation study showed that patients could be classified into high- versus low-risk groups for developing metastatic breast cancer with a receiver operating characteristic area under the curve of 0.85. This risk assessment was not dependent on the type of adjuvant therapy received by the patients. Even more importantly, we demonstrated that this protein signature provided an added value compared with conventional clinical parameters. Consequently, we present here a candidate serum biomarker signature able to classify patients with primary breast cancer according to their risk of developing distant recurrence, with an accuracy outperforming current procedures.

  • affinity proteomics
  • monitoring disease
  • prognosis
  • tumour relaps
  • malignancy

Footnotes

  • ↵1To whom correspondence should be addressed. E-mail: carl.borrebaeck{at}immun.lth.se.
  • Author contributions: C.W., C.R., H.O., and C.A.K.B. designed research; A.C. and M.K. performed research; C.R., M.F., S.E., E.G., and C.I. contributed new reagents/analytic tools; A.C., H.J., M.O., and C.P. analyzed data; and A.C. and C.A.K.B. wrote the paper.

  • Conflict of interest statement: Patent application on the biomarker signature (C.A.K.B. and C.W.).

  • ↵*This Direct Submission article had a prearranged editor.

  • This article contains supporting information online at www.pnas.org/lookup/suppl/doi:10.1073/pnas.1103125108/-/DCSupplemental.

Freely available online through the PNAS open access option.

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Molecular serum portraits in patients with primary breast cancer predict the development of distant metastases
Anders Carlsson, Christer Wingren, Malin Kristensson, Carsten Rose, Mårten Fernö, Håkan Olsson, Helena Jernström, Sara Ek, Elin Gustavsson, Christian Ingvar, Mattias Ohlsson, Carsten Peterson, Carl A. K. Borrebaeck
Proceedings of the National Academy of Sciences Aug 2011, 201103125; DOI: 10.1073/pnas.1103125108

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Molecular serum portraits in patients with primary breast cancer predict the development of distant metastases
Anders Carlsson, Christer Wingren, Malin Kristensson, Carsten Rose, Mårten Fernö, Håkan Olsson, Helena Jernström, Sara Ek, Elin Gustavsson, Christian Ingvar, Mattias Ohlsson, Carsten Peterson, Carl A. K. Borrebaeck
Proceedings of the National Academy of Sciences Aug 2011, 201103125; DOI: 10.1073/pnas.1103125108
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