Human cancer cell line microRNAs associated with in vitro sensitivity to paclitaxel

Paclitaxel is a mainstay of treatment for many solid tumors, and frequently, clinical outcome is influenced by paclitaxel sensitivity. Despite this, our understanding of the molecular basis of paclitaxel response is incomplete. Recently, it has been shown that microRNAs (miRNAs) influence messenger...

Descripción completa

Detalles Bibliográficos
Autores principales: CHEN, NING, CHON, HYE SOOK, XIONG, YIN, MARCHION, DOUGLAS C., JUDSON, PATRICIA L., HAKAM, ARDESHIR, GONZALEZ-BOSQUET, JESUS, PERMUTH-WEY, JENNIFER, WENHAM, ROBERT M., APTE, SACHIN M., CHENG, JIN Q., SELLERS, THOMAS A., LANCASTER, JOHNATHAN M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: D.A. Spandidos 2014
Materias:
Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3981115/
https://www.ncbi.nlm.nih.gov/pubmed/24220856
http://dx.doi.org/10.3892/or.2013.2847
_version_ 1782310981037195264
author CHEN, NING
CHON, HYE SOOK
XIONG, YIN
MARCHION, DOUGLAS C.
JUDSON, PATRICIA L.
HAKAM, ARDESHIR
GONZALEZ-BOSQUET, JESUS
PERMUTH-WEY, JENNIFER
WENHAM, ROBERT M.
APTE, SACHIN M.
CHENG, JIN Q.
SELLERS, THOMAS A.
LANCASTER, JOHNATHAN M.
author_facet CHEN, NING
CHON, HYE SOOK
XIONG, YIN
MARCHION, DOUGLAS C.
JUDSON, PATRICIA L.
HAKAM, ARDESHIR
GONZALEZ-BOSQUET, JESUS
PERMUTH-WEY, JENNIFER
WENHAM, ROBERT M.
APTE, SACHIN M.
CHENG, JIN Q.
SELLERS, THOMAS A.
LANCASTER, JOHNATHAN M.
author_sort CHEN, NING
collection PubMed
description Paclitaxel is a mainstay of treatment for many solid tumors, and frequently, clinical outcome is influenced by paclitaxel sensitivity. Despite this, our understanding of the molecular basis of paclitaxel response is incomplete. Recently, it has been shown that microRNAs (miRNAs) influence messenger RNA (mRNA) transcriptional control and can contribute to human carcinogenesis. In the present study, our objective was to identify miRNAs associated with cancer cell line response to paclitaxel and to evaluate these miRNAs as therapeutic targets to increase paclitaxel sensitivity. We measured the expression of 335 unique miRNAs in 40 human cancer cell lines selected from the NCI panel. We then integrated miRNA expression data with publicly available paclitaxel-sensitivity (GI(50)) data for each of the 40 cell lines to identify miRNAs associated with paclitaxel sensitivity. Ovarian cancer cell lines with differential miRNA expression and paclitaxel sensitivity were transiently transfected with miRNA precursors and inhibitors, and the effects on in vitro cell paclitaxel sensitivity were evaluated. Pearson’s correlation identified 2 miRNAs (miR-367 and miR-30a-5p) associated with the NCI40 cell line in vitro paclitaxel response (P<0.0003). Ovarian cancer cells were selected based on the association between paclitaxel sensitivity and miR-367/miR-30a-5p expression. Overexpression of miR-367 in the paclitaxel-sensitive cells [PA1; IC(50), 1.69 nM, high miR-367 (2.997), low miR-30a-5p (−0.323)] further increased paclitaxel sensitivity, whereas miR-367 depletion decreased paclitaxel sensitivity. In contrast, overexpression and depletion of miR-30a-5p in the paclitaxel-resistant cells [OVCAR4; IC(50), 17.8 nM, low miR-367 (−0.640), high miR-30a-5p (3.270)] decreased and increased paclitaxel sensitivity, respectively. We identified and successfully targeted miRNAs associated with human cancer cell line response to paclitaxel. Our strategy of integrating in vitro miRNA expression and drug sensitivity data may not only aid in the characterization of determinants of drug response but also in the identification of novel therapeutic targets to increase activity of existing therapeutics.
format Online
Article
Text
id pubmed-3981115
institution National Center for Biotechnology Information
language English
publishDate 2014
publisher D.A. Spandidos
record_format MEDLINE/PubMed
spelling pubmed-39811152014-04-09 Human cancer cell line microRNAs associated with in vitro sensitivity to paclitaxel CHEN, NING CHON, HYE SOOK XIONG, YIN MARCHION, DOUGLAS C. JUDSON, PATRICIA L. HAKAM, ARDESHIR GONZALEZ-BOSQUET, JESUS PERMUTH-WEY, JENNIFER WENHAM, ROBERT M. APTE, SACHIN M. CHENG, JIN Q. SELLERS, THOMAS A. LANCASTER, JOHNATHAN M. Oncol Rep Articles Paclitaxel is a mainstay of treatment for many solid tumors, and frequently, clinical outcome is influenced by paclitaxel sensitivity. Despite this, our understanding of the molecular basis of paclitaxel response is incomplete. Recently, it has been shown that microRNAs (miRNAs) influence messenger RNA (mRNA) transcriptional control and can contribute to human carcinogenesis. In the present study, our objective was to identify miRNAs associated with cancer cell line response to paclitaxel and to evaluate these miRNAs as therapeutic targets to increase paclitaxel sensitivity. We measured the expression of 335 unique miRNAs in 40 human cancer cell lines selected from the NCI panel. We then integrated miRNA expression data with publicly available paclitaxel-sensitivity (GI(50)) data for each of the 40 cell lines to identify miRNAs associated with paclitaxel sensitivity. Ovarian cancer cell lines with differential miRNA expression and paclitaxel sensitivity were transiently transfected with miRNA precursors and inhibitors, and the effects on in vitro cell paclitaxel sensitivity were evaluated. Pearson’s correlation identified 2 miRNAs (miR-367 and miR-30a-5p) associated with the NCI40 cell line in vitro paclitaxel response (P<0.0003). Ovarian cancer cells were selected based on the association between paclitaxel sensitivity and miR-367/miR-30a-5p expression. Overexpression of miR-367 in the paclitaxel-sensitive cells [PA1; IC(50), 1.69 nM, high miR-367 (2.997), low miR-30a-5p (−0.323)] further increased paclitaxel sensitivity, whereas miR-367 depletion decreased paclitaxel sensitivity. In contrast, overexpression and depletion of miR-30a-5p in the paclitaxel-resistant cells [OVCAR4; IC(50), 17.8 nM, low miR-367 (−0.640), high miR-30a-5p (3.270)] decreased and increased paclitaxel sensitivity, respectively. We identified and successfully targeted miRNAs associated with human cancer cell line response to paclitaxel. Our strategy of integrating in vitro miRNA expression and drug sensitivity data may not only aid in the characterization of determinants of drug response but also in the identification of novel therapeutic targets to increase activity of existing therapeutics. D.A. Spandidos 2014-01 2013-11-13 /pmc/articles/PMC3981115/ /pubmed/24220856 http://dx.doi.org/10.3892/or.2013.2847 Text en Copyright © 2014, Spandidos Publications http://creativecommons.org/licenses/by/3.0 This is an open-access article licensed under a Creative Commons Attribution-NonCommercial 3.0 Unported License. The article may be redistributed, reproduced, and reused for non-commercial purposes, provided the original source is properly cited.
spellingShingle Articles
CHEN, NING
CHON, HYE SOOK
XIONG, YIN
MARCHION, DOUGLAS C.
JUDSON, PATRICIA L.
HAKAM, ARDESHIR
GONZALEZ-BOSQUET, JESUS
PERMUTH-WEY, JENNIFER
WENHAM, ROBERT M.
APTE, SACHIN M.
CHENG, JIN Q.
SELLERS, THOMAS A.
LANCASTER, JOHNATHAN M.
Human cancer cell line microRNAs associated with in vitro sensitivity to paclitaxel
title Human cancer cell line microRNAs associated with in vitro sensitivity to paclitaxel
title_full Human cancer cell line microRNAs associated with in vitro sensitivity to paclitaxel
title_fullStr Human cancer cell line microRNAs associated with in vitro sensitivity to paclitaxel
title_full_unstemmed Human cancer cell line microRNAs associated with in vitro sensitivity to paclitaxel
title_short Human cancer cell line microRNAs associated with in vitro sensitivity to paclitaxel
title_sort human cancer cell line micrornas associated with in vitro sensitivity to paclitaxel
topic Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3981115/
https://www.ncbi.nlm.nih.gov/pubmed/24220856
http://dx.doi.org/10.3892/or.2013.2847
work_keys_str_mv AT chenning humancancercelllinemicrornasassociatedwithinvitrosensitivitytopaclitaxel
AT chonhyesook humancancercelllinemicrornasassociatedwithinvitrosensitivitytopaclitaxel
AT xiongyin humancancercelllinemicrornasassociatedwithinvitrosensitivitytopaclitaxel
AT marchiondouglasc humancancercelllinemicrornasassociatedwithinvitrosensitivitytopaclitaxel
AT judsonpatricial humancancercelllinemicrornasassociatedwithinvitrosensitivitytopaclitaxel
AT hakamardeshir humancancercelllinemicrornasassociatedwithinvitrosensitivitytopaclitaxel
AT gonzalezbosquetjesus humancancercelllinemicrornasassociatedwithinvitrosensitivitytopaclitaxel
AT permuthweyjennifer humancancercelllinemicrornasassociatedwithinvitrosensitivitytopaclitaxel
AT wenhamrobertm humancancercelllinemicrornasassociatedwithinvitrosensitivitytopaclitaxel
AT aptesachinm humancancercelllinemicrornasassociatedwithinvitrosensitivitytopaclitaxel
AT chengjinq humancancercelllinemicrornasassociatedwithinvitrosensitivitytopaclitaxel
AT sellersthomasa humancancercelllinemicrornasassociatedwithinvitrosensitivitytopaclitaxel
AT lancasterjohnathanm humancancercelllinemicrornasassociatedwithinvitrosensitivitytopaclitaxel

Ejemplares similares