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DNA repair and cholesterol-mediated drug efflux induce dose-dependent chemoresistance in nutrient-deprived neuroblastoma cells

Authors
Chae, Soo YeonNam, DowoonHyeon, Do YoungHong, AreumLee, Timothy DainKim, SujinIm, DongjoonHong, JiwonKang, ChaewonLee, Ji WonHwang, DaeheeLee, Sang-WonKim, Hugh, I
Issue Date
23-Apr-2021
Publisher
CELL PRESS
Keywords
Cancer; Molecular Biology; Proteomics
Citation
ISCIENCE, v.24, no.4
Indexed
SCIE
SCOPUS
Journal Title
ISCIENCE
Volume
24
Number
4
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/128208
DOI
10.1016/j.isci.2021.102325
ISSN
2589-0042
Abstract
Neuroblastoma is a solid, heterogeneous pediatric tumor. Chemotherapy is widely used to treat neuroblastoma. However, dose-dependent responses and chemoresistance mechanisms of neuroblastoma cells to anticancer drugs remain challenging. Here, we investigated the dose-dependent effects of topotecan on human neuroblastoma cells (SK-N-SH, SH-SY5Y, and SK-N-BE) under various nutrient supply conditions. Serum-starved human neuroblastoma cells showed reduced toxicity. Their survival rate increased upon treatment with a high concentration (1 mu M) of topotecan. Quantitative profiling of global and phosphoproteome identified 12,959 proteins and 48,812 phosphosites, respectively, from SK-N-SH cells. Network analysis revealed that topotecan upregulated DNA repair and cholesterol-mediated topotecan efflux, resulting in topotecan resistance. Results of DNA damage assay, cell cycle, and quantitative analyses of membrane cholesterol supported the validity of these resistance factors and their applicability to all neuroblastoma cells. Our results provide amodel for high dose-dependent chemoresistance in neuroblastoma cells that could enable a patient-dependent chemotherapy screening strategy.
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