Issue 1, 2017
From the journal:

MedChemComm

Phenotype-based variation as a biomarker of sensitivity to molecularly targeted therapy in melanoma

Kerem M. Senses, ORCID logo a   Mehdi Ghasemi,a   Muhammad W. Akbar,a   Murat Isbilen,a   Anna L. Fallacara,b   Shoshana Frankenburg,c   Silvia Schenone,d   Michal Lotem,c   Maurizio Bottab  and  Ali O. Gure*a  

* Corresponding authors

a Department of Molecular Biology and Genetics, Bilkent University, 06800 Ankara, Turkey
E-mail: agure@bilkent.edu.tr

b Department of Biotechnology, Chemistry and Pharmacy, University of Siena, 53100 Siena, Italy

c Sharett Institute of Oncology, Hadassah Hebrew University Hospital, Ein Karem Campus, 91120 Jerusalem, Israel

d Department of Pharmacy, University of Genoa, 16132 Genoa, Italy

Abstract

Transcriptomic phenotypes defined for melanoma have been reported to correlate with sensitivity to various drugs. In this study, we aimed to define a minimal signature that could be used to distinguish melanoma sub-types in vitro, and to determine suitable drugs by which these sub-types can be targeted. By using primary melanoma cell lines, as well as commercially available melanoma cell lines, we find that the evaluation of MLANA and INHBA expression is as capable as one based on a combined analysis performed with genes for stemness, EMT and invasion/proliferation, in identifying melanoma subtypes that differ in their sensitivity to molecularly targeted drugs. Using this approach, we find that 75% of melanoma cell lines can be treated with either the MEK inhibitor AZD6244 or the HSP90 inhibitor 17AAG.

Graphical abstract: Phenotype-based variation as a biomarker of sensitivity to molecularly targeted therapy in melanoma

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Article information

DOI
https://doi.org/10.1039/C6MD00466K
Article type
Research Article
Submitted
15 Aug 2016
Accepted
11 Oct 2016
First published
27 Oct 2016

Med. Chem. Commun., 2017,8, 88-95

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Phenotype-based variation as a biomarker of sensitivity to molecularly targeted therapy in melanoma

K. M. Senses, M. Ghasemi, M. W. Akbar, M. Isbilen, A. L. Fallacara, S. Frankenburg, S. Schenone, M. Lotem, M. Botta and A. O. Gure, Med. Chem. Commun., 2017, 8, 88 DOI: 10.1039/C6MD00466K

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