A posttranslational modification in histones as prognostic/predictive marker in Estrogen-Positive Breast Cancer

Lobo, S.; Fontes-Sousa, M.; Salta, S.; Lopes, P.; Lobo, J.; Sousa, S.; Henrique, R.; Jerónimo, C.

doi:10.1016/j.pbj.2017.07.116

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Aim: This work aims to evaluate H3K27me3 expression in luminal-like breast tumors, using immunohistochemistry assay, to assess the prognostic value of this epigenetic alterations in estrogen positive breast cancer (BrC).

Introduction: BrC is the second most incident cancer worldwide. In Portugal, in 2012, BrC was simultaneously the leading cancer in incidence and mortality in women.1 Around 70% of all BrC are hormone-receptor positive, that is the major part of breast tumors is luminal-like.2 H3K27m3 is a gene repression marker3,4 and is associated with gene silencing, playing a crucial role in cell proliferation and differentiation.3 H3K27me3 may have some clinical value in several types of cancer since it can be used as a biomarker. This histone modification has been associated with poor prognosis of some BrC subtypes.5

Methods: It was used a cohort of BrC patients of the Portuguese Oncology Institution of Porto (IPO-Porto), diagnosed between 1994 and 2002. A total of 102 luminal-like tumor cases were assessed by immunohistochemistry, to H3K27me3 expression. To verify the prognostic value of H3K27me3 levels, Cox regression with a log rank test was performed for both disease-specific and disease-free survival.

Results: Through the result analysis, it was established that only tumor grade (p=0.021) was significant associated with disease-specific survival. Nevertheless, both luminal subtype (p=0.016) and H3K27me3 expression (p=0.012) were significantly associated with disease-free survival. Indeed, H3K27me3 high expression is associated with higher recurrence risk, especially in Luminal A.

Conclusion: We could confirm the prognostic value of H3K27me3 expression in luminal A subtype BrC patients. Therefore, higher H3K27me3 expression in luminal A tumors is associated with a greater probability of recurrence.

However, studies in larger cohorts are mandatory to validate its clinical utility.

Acknowledgements: This study was funded by a grant of the Research Centre of Portuguese Oncology Institute of Porto (CI-IPOP-74-2016).

References

[1]

J.S.I. Ferlay, M. Ervik, R. Dikshit, S. Eser, C. Mathers, M. Rebelo, et al.

GLOBOCAN 2012 v1.0, cancer incidence and mortality worldwide: IARC CancerBase No. 11.

International Agency for Research on Cancer, (2013),

[2]

E. Senkus, S. Kyriakides, S. Ohno, F. Penault-Llorca, P. Poortmans, E. Rutgers, et al.

Primary breast cancer: ESMO Clinical Practice Guidelines for diagnosis, treatment and follow-up.

Ann Oncol, 26 (2015),

http://dx.doi.org/10.1093/annonc/mdv383 | Medline

v8-30

[3]

A. Chase, N.C. Cross.

Aberrations of EZH2 in cancer.

Clin Cancer Res, 17 (2011), pp. 2613-2618

http://dx.doi.org/10.1158/1078-0432.CCR-10-2156 | Medline

[4]

K.H. Yoo, L. Hennighausen.

EZH2 methyltransferase and H3K27 methylation in breast cancer.

Int J Biol Sci, 8 (2012), pp. 59-65

Medline

[5]

A. Hayashi, N. Yamauchi, J. Shibahara, H. Kimura, T. Morikawa, S. Ishikawa, et al.

Concurrent activation of acetylation and tri-methylation of H3K27 in a subset of hepatocellular carcinoma with aggressive behavior.

PLoS ONE, 9 (2014), pp. e91330

http://dx.doi.org/10.1371/journal.pone.0091330 | Medline

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