The mammalian AlkB homologue-3 (AlkBH3) is a member of the dioxygenase family of enzymes that in humans is involved in DNA dealkylation repair. Because of its role in promoting tumor cell proliferation and metastasis of cancer, extensive efforts are being directed in developing selective inhibitors for AlkBH3. Here we report synthesis, screening and evaluation of panel of arylated indenone derivatives as new class of inhibitors of AlkBH3 DNA repair activity. An efficient synthesis of 2,3-diaryl indenones from 2,3-dibromo indenones was achieved via Suzuki-Miyaura cross-coupling. Using a robust quantitative assay, we have obtained an AlkBH3 inhibitor that display specific binding and competitive mode of inhibition against DNA substrate. Finally, we established that this compound could prevent the proliferation of lung cancer cell line and enhance sensitivity to DNA damaging alkylating agent. © 2018 Elsevier Ltd

Anindya Roy

Department of Biotechnology

Faiz Ahmed Khan

Department of Chemistry

Subha Narayan Rath

Department of Biomedical Engineering

R. Nigam

K.R. Babu

T. Ghosh

B. Kumari

D. Akula

P. Das

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IIT Hyderabad

Bioorganic and Medicinal Chemistry

Indenone derivatives as inhibitor of human DNA dealkylation repair enzyme AlkBH3

Journal	Data powered by TypesetBioorganic and Medicinal Chemistry
Publisher	Data powered by TypesetElsevier Ltd
ISSN	09680896