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Ribosomal protein S11 influences glioma response to TOP2 poisons
Awah, C.U.
;
Chen, L.
;
Bansal, M.
;
Mahajan, A.
;
Winter, J.
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Lad, M.
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Warnke, L.
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Gonzalez-Buendia, E.
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Park, C.
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Zhang, D.
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Feldstein, E.
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Yu, D.
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Zannikou, M.
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Balyasnikova, I.V.
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Martuscello, R.
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Konerman, S.
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Győrffy, B. [Győrffy, Balázs (Onkológia), author] Institute of Enzymology (RCNS); II. Department of Pediatrics (SU / FM / C); Enzim_417 (IMLS)
;
Burdett, K.B.
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Scholtens, D.M.
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Stupp, R.
;
Ahmed, A.
;
Hsu, P.
;
Sonabend, A.M. ✉
English Article (Journal Article) Scientific
Published:
ONCOGENE 0950-9232 1476-5594
39
(27)
pp. 5068-5081
2020
SJR Scopus - Genetics: D1
Identifiers
MTMT: 31359015
DOI:
10.1038/s41388-020-1342-0
WoS:
000539817600002
Scopus:
85086318328
PubMed:
32528131
Topoisomerase II poisons are one of the most common class of chemotherapeutics used in cancer. We and others had shown that a subset of glioblastomas, the most malignant of all primary brain tumors in adults, is responsive to TOP2 poisons. To identify genes that confer susceptibility to this drug in gliomas, we performed a genome-scale CRISPR knockout screen with etoposide. Genes involved in protein synthesis and DNA damage were implicated in etoposide susceptibility. To define potential biomarkers for TOP2 poisons, CRISPR hits were overlapped with genes whose expression correlates with susceptibility to this drug across glioma cell lines, revealing ribosomal protein subunit RPS11, 16, and 18 as putative biomarkers for response to TOP2 poisons. Loss of RPS11 led to resistance to etoposide and doxorubicin and impaired the induction of proapoptotic gene APAF1 following treatment. The expression of these ribosomal subunits was also associated with susceptibility to TOP2 poisons across cell lines from gliomas and multiple other cancers. © 2020, The Author(s), under exclusive licence to Springer Nature Limited.
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2025-04-02 22:00
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