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Large-scale pharmacogenomics based drug discovery for ITGB3 dependent chemoresistance in mesenchymal lung cancer

Title
Large-scale pharmacogenomics based drug discovery for ITGB3 dependent chemoresistance in mesenchymal lung cancer
Authors
Hong, Soon-KiLee, HaeseungKwon, Ok-SeonSong, Na-YoungLee, Hyo-JuKang, SeungminKim, Jeong-HwanKim, MirangKim, WankyuCha, Hyuk-Jin
Ewha Authors
김완규이해승
SCOPUS Author ID
김완규scopus
Issue Date
2018
Journal Title
MOLECULAR CANCER
ISSN
1476-4598JCR Link
Citation
MOLECULAR CANCER vol. 17
Keywords
ChemoresistanceMesenchymal cancerPharmacogenomicsDrug repurposingBiomarkerITGB3NF-BAtorvastatinSystems pharmacology
Publisher
BMC
Indexed
SCIE; SCOPUS WOS scopus
Document Type
Article
Abstract
Even when targets responsible for chemoresistance are identified, drug development is often hampered due to the poor druggability of these proteins. We systematically analyzed therapy-resistance with a large-scale cancer cell transcriptome and drug-response datasets and predicted the candidate drugs based on the gene expression profile. Our results implicated the epithelial-mesenchymal transition as a common mechanism underlying resistance to chemotherapeutic drugs. Notably, we identified ITGB3, whose expression was abundant in both drug resistance and mesenchymal status, as a promising target to overcome chemoresistance. We also confirmed that depletion of ITGB3 sensitized cancer cells to conventional chemotherapeutic drugs by modulating the NF-B signaling pathway. Considering the poor druggability of ITGB3 and the lack of feasible drugs to directly inhibit this protein, we took an in silico screening for drugs mimicking the transcriptome-level changes caused by knockdown of ITGB3. This approach successfully identified atorvastatin as a novel candidate for drug repurposing, paving an alternative path to drug screening that is applicable to undruggable targets.
DOI
10.1186/s12943-018-0924-8
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자연과학대학 > 생명과학전공 > Journal papers
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