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Cited 126 time in webofscience Cited 125 time in scopus
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Pharmacogenomic landscape of patient-derived tumor cells informs precision oncology therapy

Authors
Lee, Jin-KuLiu, ZhaoqiSa, Jason K.Shin, SangWang, JiguangBordyuh, MykolaCho, HeejinElliott, OliverChu, TimothyChoi, Seung WonRosenbloom, Daniel I. S.Lee, In-HeeShin, Yong JaeKang, Hyun JuKim, DonggeonKim, Sun YoungSim, Moon-HeeKim, JusunLee, TaehyangSeo, Yun JeeShin, HyemiLee, MijeongKim, Sung HeonKwon, Yong-JunOh, Jeong-WooSong, MinsukKim, MisukKong, Doo-SikChoi, Jung WonSeol, Ho JunLee, Jung-IlKim, Seung TaePark, Joon OhKim, Kyoung-MeeSong, Sang-YongLee, Jeong-WonKim, Hee-CheolLee, Jeong EonChoi, Min GewSeo, Sung WookShim, Young MogZo, Jae IllJeong, Byong ChangYoon, YeupRyu, Gyu HaKim, Nayoung K. D.Bae, Joon SeolPark, Woong-YangLee, JeongwuVerhaak, Roel G. W.Iavarone, AntonioLee, JeeyunRabadan, RaulNam, Do-Hyun
Issue Date
Oct-2018
Publisher
Nature Publishing Group
Citation
Nature Genetics, v.50, no.10, pp 1399 - +
Indexed
SCI
SCIE
SCOPUS
Journal Title
Nature Genetics
Volume
50
Number
10
Start Page
1399
End Page
+
URI
https://scholarworks.korea.ac.kr/kumedicine/handle/2020.sw.kumedicine/3060
DOI
10.1038/s41588-018-0209-6
ISSN
1061-4036
1546-1718
Abstract
Outcomes of anticancer therapy vary dramatically among patients due to diverse genetic and molecular backgrounds, highlighting extensive intertumoral heterogeneity. The fundamental tenet of precision oncology defines molecular characterization of tumors to guide optimal patient-tailored therapy. Towards this goal, we have established a compilation of pharmacological landscapes of 462 patient-derived tumor cells (PDCs) across 14 cancer types, together with genomic and transcriptomic profiling in 385 of these tumors. Compared with the traditional long-term cultured cancer cell line models, PDCs recapitulate the molecular properties and biology of the diseases more precisely. Here, we provide insights into dynamic pharmacogenomic associations, including molecular determinants that elicit therapeutic resistance to EGFR inhibitors, and the potential repurposing of ibrutinib (currently used in hematological malignancies) for EGFR-specific therapy in gliomas. Lastly, we present a potential implementation of PDC-derived drug sensitivities for the prediction of clinical response to targeted therapeutics using retrospective clinical studies.
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