<i>ESR1</i> mutations: Pièce de résistance

Berry Button; Ben Ho Park

doi:10.1016/j.gendis.2016.03.005

Genes & Diseases 2016, 3(2): 124-129 https://doi.org/10.1016/j.gendis.2016.03.005

Review Article |

Open Access | Issue | Published: 19 April 2016

ESR1 mutations: Pièce de résistance

Show Author's Information Hide Author's Information Berry Button^{^a^,^c}, Ben Ho Park^{^a^,^b^,^,^d}(

)

The Sidney Kimmel Comprehensive Cancer Center, The Johns Hopkins University School of Medicine, Baltimore, MD, United States

Department of Chemical and Biomolecular Engineering, The Whiting School of Engineering, The Johns Hopkins University, Baltimore, MD, United States

^c 1650 Orleans Street, CRBI, Room 116, Baltimore, MD 21287, United States.

Peer review under responsibility of Chongqing Medical University.

^d 1650 Orleans Street, CRBI, Room 151, Baltimore, MD 21287, United States.

Keywords:

Mutation, Breast cancer, Plasma, Estrogen receptor, Circulating tumor DNA, ESR1

Cite this article:

Button B, Park BH. ESR1 mutations: Pièce de résistance. Genes & Diseases, 2016, 3(2): 124-129. https://doi.org/10.1016/j.gendis.2016.03.005

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Abstract About this article

Abstract

Estrogen and estrogen receptor-alpha (ER) signaling are important factors in the pathogenesis and treatment of ER-positive breast cancers. Therefore targeted therapies against ER, known as endocrine therapies, are widely used in the treatment of ER-positive breast cancers. While these therapies have shown great success, de novo and acquired resistance are common. The approach to the problem of endocrine therapy resistance is two-fold: identify the mechanisms of resistance and develop alternative treatments to overcome these mechanisms. This review focuses on the progress and integration of these two aspects of resolving endocrine therapy resistance in ER-positive breast cancer patients.

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Publication history

Received: 07 February 2016

Accepted: 29 March 2016

Published: 19 April 2016

Issue date: June 2016

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Acknowledgements

This work was supported by: The Avon Foundation (BHP) and the Canney Foundation. We would also like to thank and acknowledge the support of National Institutes of Health P30 CA006973, the Sandy Garcia Charitable Foundation, the Commonwealth Foundation, the Santa Fe Foundation, the Marcie Ellen Foundation, The Helen Golde Trust and The Robin Page/Lebor Foundation.

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This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).