ALKBH overexpression in head and neck cancer: potential target for novel anticancer therapy

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作者
Tomaš Pilžys
Michał Marcinkowski
Wojciech Kukwa
Damian Garbicz
Małgorzata Dylewska
Karolina Ferenc
Adam Mieczkowski
Andrzej Kukwa
Ewa Migacz
Dominika Wołosz
Damian Mielecki
Arne Klungland
Jan Piwowarski
Jarosław Poznański
Elżbieta Grzesiuk
机构
[1] Institute of Biochemistry and Biophysics,Department of Otolaryngology
[2] Polish Academy of Sciences,Department of Pathology
[3] Medical University of Warsaw,Department of Microbiology
[4] Veterinary Research Centre and Center for Biomedical Research,undefined
[5] Department of Large Animal Diseases with the Clinic,undefined
[6] Faculty of Veterinary Medicine,undefined
[7] Warsaw University of Life Sciences,undefined
[8] Medical University of Warsaw,undefined
[9] Oslo University Hospital,undefined
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The nine identified human homologues of E. coli AlkB 2-oxoglutarate (2OG) and Fe(II)-dependent dioxygenase, ALKBH1-8 and FTO, display different substrate specificities and diverse biological functions. Here we discovered the combined overexpression of members of the ALKBH family in head and neck squamous cell carcinomas (HNSCC). We found direct correlation of ALKBH3 and FTO expression with primary HNSCC tumor size. We observed unidentified thus far cytoplasmic localization of ALKBH2 and 5 in HNSCC, suggesting abnormal role(s) of ALKBH proteins in cancer. Further, high expression of ALKBHs was observed not only in HNSCC, but also in several cancerous cell lines and silencing ALKBH expression in HeLa cancer cells resulted in dramatically decreased survival. Considering the discovered impact of high expression of ALKBH proteins on HNSCC development, we screened for ALKBH blockers among newly synthetized anthraquinone derivatives and demonstrated their potential to support standard anticancer therapy.
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