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Expression Profiles of the Individual Genes Corresponding to the Genes Generated by Cytotoxicity Experiments with Bortezomib in Multiple Myeloma

OBJECTIVE: Multiple myeloma (MM) is currently incurable due to refractory disease relapse even under novel anti-myeloma treatment. In silico studies are effective for key decision making during clinicopathological battles against the chronic course of MM. The aim of this present in silico study was...

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Autores principales: Ghasemi, Mehdi, Alpsoy, Semih, Türk, Seyhan, Malkan, Ümit Y., Atakan, Şükrü, Haznedaroğlu, İbrahim C., Güneş, Gürsel, Gündüz, Mehmet, Yılmaz, Burak, Etgül, Sezgin, Aydın, Seda, Aslan, Tuncay, Sayınalp, Nilgün, Aksu, Salih, Demiroğlu, Haluk, Özcebe, Osman İ., Büyükaşık, Yahya, Göker, Hakan
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Galenos Publishing 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5204182/
https://www.ncbi.nlm.nih.gov/pubmed/27095044
http://dx.doi.org/10.4274/tjh.2015.0145
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author Ghasemi, Mehdi
Alpsoy, Semih
Türk, Seyhan
Malkan, Ümit Y.
Atakan, Şükrü
Haznedaroğlu, İbrahim C.
Güneş, Gürsel
Gündüz, Mehmet
Yılmaz, Burak
Etgül, Sezgin
Aydın, Seda
Aslan, Tuncay
Sayınalp, Nilgün
Aksu, Salih
Demiroğlu, Haluk
Özcebe, Osman İ.
Büyükaşık, Yahya
Göker, Hakan
author_facet Ghasemi, Mehdi
Alpsoy, Semih
Türk, Seyhan
Malkan, Ümit Y.
Atakan, Şükrü
Haznedaroğlu, İbrahim C.
Güneş, Gürsel
Gündüz, Mehmet
Yılmaz, Burak
Etgül, Sezgin
Aydın, Seda
Aslan, Tuncay
Sayınalp, Nilgün
Aksu, Salih
Demiroğlu, Haluk
Özcebe, Osman İ.
Büyükaşık, Yahya
Göker, Hakan
author_sort Ghasemi, Mehdi
collection PubMed
description OBJECTIVE: Multiple myeloma (MM) is currently incurable due to refractory disease relapse even under novel anti-myeloma treatment. In silico studies are effective for key decision making during clinicopathological battles against the chronic course of MM. The aim of this present in silico study was to identify individual genes whose expression profiles match that of the one generated by cytotoxicity experiments for bortezomib. MATERIALS AND METHODS: We used an in silico literature mining approach to identify potential biomarkers by creating a summarized set of metadata derived from relevant information. The E-MTAB-783 dataset containing expression data from 789 cancer cell lines including 8 myeloma cell lines with drug screening data from the Wellcome Trust Sanger Institute database obtained from ArrayExpress was “Robust Multi-array analysis” normalized using GeneSpring v.12.5. Drug toxicity data were obtained from the Genomics of Drug Sensitivity in Cancer project. In order to identify individual genes whose expression profiles matched that of the one generated by cytotoxicity experiments for bortezomib, we used a linear regression-based approach, where we searched for statistically significant correlations between gene expression values and IC50 data. The intersections of the genes were identified in 8 cell lines and used for further analysis. RESULTS: Our linear regression model identified 73 genes and some genes expression levels were found to very closely correlated with bortezomib IC50 values. When all 73 genes were used in a hierarchical cluster analysis, two major clusters of cells representing relatively sensitive and resistant cells could be identified. Pathway and molecular function analysis of all the significant genes was also investigated, as well as the genes involved in pathways. CONCLUSION: The findings of our present in silico study could be important not only for the understanding of the genomics of MM but also for the better arrangement of the targeted anti-myeloma therapies, such as bortezomib.
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spelling pubmed-52041822017-01-06 Expression Profiles of the Individual Genes Corresponding to the Genes Generated by Cytotoxicity Experiments with Bortezomib in Multiple Myeloma Ghasemi, Mehdi Alpsoy, Semih Türk, Seyhan Malkan, Ümit Y. Atakan, Şükrü Haznedaroğlu, İbrahim C. Güneş, Gürsel Gündüz, Mehmet Yılmaz, Burak Etgül, Sezgin Aydın, Seda Aslan, Tuncay Sayınalp, Nilgün Aksu, Salih Demiroğlu, Haluk Özcebe, Osman İ. Büyükaşık, Yahya Göker, Hakan Turk J Haematol Research Article OBJECTIVE: Multiple myeloma (MM) is currently incurable due to refractory disease relapse even under novel anti-myeloma treatment. In silico studies are effective for key decision making during clinicopathological battles against the chronic course of MM. The aim of this present in silico study was to identify individual genes whose expression profiles match that of the one generated by cytotoxicity experiments for bortezomib. MATERIALS AND METHODS: We used an in silico literature mining approach to identify potential biomarkers by creating a summarized set of metadata derived from relevant information. The E-MTAB-783 dataset containing expression data from 789 cancer cell lines including 8 myeloma cell lines with drug screening data from the Wellcome Trust Sanger Institute database obtained from ArrayExpress was “Robust Multi-array analysis” normalized using GeneSpring v.12.5. Drug toxicity data were obtained from the Genomics of Drug Sensitivity in Cancer project. In order to identify individual genes whose expression profiles matched that of the one generated by cytotoxicity experiments for bortezomib, we used a linear regression-based approach, where we searched for statistically significant correlations between gene expression values and IC50 data. The intersections of the genes were identified in 8 cell lines and used for further analysis. RESULTS: Our linear regression model identified 73 genes and some genes expression levels were found to very closely correlated with bortezomib IC50 values. When all 73 genes were used in a hierarchical cluster analysis, two major clusters of cells representing relatively sensitive and resistant cells could be identified. Pathway and molecular function analysis of all the significant genes was also investigated, as well as the genes involved in pathways. CONCLUSION: The findings of our present in silico study could be important not only for the understanding of the genomics of MM but also for the better arrangement of the targeted anti-myeloma therapies, such as bortezomib. Galenos Publishing 2016-12 2016-12-01 /pmc/articles/PMC5204182/ /pubmed/27095044 http://dx.doi.org/10.4274/tjh.2015.0145 Text en © Turkish Journal of Hematology, Published by Galenos Publishing. http://creativecommons.org/licenses/by/2.5/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Ghasemi, Mehdi
Alpsoy, Semih
Türk, Seyhan
Malkan, Ümit Y.
Atakan, Şükrü
Haznedaroğlu, İbrahim C.
Güneş, Gürsel
Gündüz, Mehmet
Yılmaz, Burak
Etgül, Sezgin
Aydın, Seda
Aslan, Tuncay
Sayınalp, Nilgün
Aksu, Salih
Demiroğlu, Haluk
Özcebe, Osman İ.
Büyükaşık, Yahya
Göker, Hakan
Expression Profiles of the Individual Genes Corresponding to the Genes Generated by Cytotoxicity Experiments with Bortezomib in Multiple Myeloma
title Expression Profiles of the Individual Genes Corresponding to the Genes Generated by Cytotoxicity Experiments with Bortezomib in Multiple Myeloma
title_full Expression Profiles of the Individual Genes Corresponding to the Genes Generated by Cytotoxicity Experiments with Bortezomib in Multiple Myeloma
title_fullStr Expression Profiles of the Individual Genes Corresponding to the Genes Generated by Cytotoxicity Experiments with Bortezomib in Multiple Myeloma
title_full_unstemmed Expression Profiles of the Individual Genes Corresponding to the Genes Generated by Cytotoxicity Experiments with Bortezomib in Multiple Myeloma
title_short Expression Profiles of the Individual Genes Corresponding to the Genes Generated by Cytotoxicity Experiments with Bortezomib in Multiple Myeloma
title_sort expression profiles of the individual genes corresponding to the genes generated by cytotoxicity experiments with bortezomib in multiple myeloma
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5204182/
https://www.ncbi.nlm.nih.gov/pubmed/27095044
http://dx.doi.org/10.4274/tjh.2015.0145
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