A systematic review of genes involved in the inverse resistance relationship between cisplatin and paclitaxel chemotherapy: role of BRCA1

Article

Stordal, B. and Davey, R. 2009. A systematic review of genes involved in the inverse resistance relationship between cisplatin and paclitaxel chemotherapy: role of BRCA1. Current Cancer Drug Targets. 9 (3), pp. 354-365. https://doi.org/10.2174/156800909788166592
TypeArticle
TitleA systematic review of genes involved in the inverse resistance relationship between cisplatin and paclitaxel chemotherapy: role of BRCA1
AuthorsStordal, B. and Davey, R.
Abstract

A systematic review of cell models of acquired drug resistance not involving genetic manipulation showed that 80% of cell models had an inverse resistance relationship between cisplatin and paclitaxel. Here we systematically review genetically modified cell lines in which the inverse cisplatin/paclitaxel resistance phenotype has resulted. This will form a short list of genes which may play a role in the mechanism of the inverse resistance relationship as well as act as potential markers for monitoring the development of resistance in the clinical treatment of cancer. The literature search revealed 91 genetically modified cell lines which report toxicity or viability/apoptosis data for cisplatin and paclitaxel relative to their parental cell lines. This resulted in 26 genes being associated with the inverse cisplatin/paclitaxel phenotype. The gene with the highest number of genetically modified cell lines associated with the inverse resistance relationship was BRCA1 and this gene is discussed in detail with reference to chemotherapy response in cell lines and in the clinical treatment of breast, ovarian and lung cancer. Other genes associated with the inverse resistance phenotype included dihydrodiol dehydrogenase (DDH) and P-glycoprotein. Genes which caused cross resistance or cross sensitivity between cisplatin and paclitaxel were also examined, the majority of these genes were apoptosis associated genes which may be useful for predicting cross resistance. We propose that BRCA1 should be the first of a panel of cellular markers to predict the inverse cisplatin/paclitaxel resistance phenotype.

KeywordsBRCA1; cisplatin; paclitaxel; resistance; sensitivity; genetically modified cell lines
Research GroupBiomarkers for Cancer group
JournalCurrent Cancer Drug Targets
ISSN1568-0096
Electronic1873-5576
Publication dates
Print01 May 2009
Publication process dates
Deposited08 Jan 2016
Accepted19 Jan 2009
Output statusPublished
Accepted author manuscript
Copyright Statement

The Accepted author manuscript is included in the Middlesex University Research Repository as permitted by the publisher's self-archiving policy.
The published manuscript is available at EurekaSelect via https://www.eurekaselect.com/article/14041

Digital Object Identifier (DOI)https://doi.org/10.2174/156800909788166592
PubMed ID19442054
Web of Science identifierWOS:000266994100009
LanguageEnglish
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