| Literature DB >> 33075425 |
Jayoung Song1, Jinha Yu1, Lak Shin Jeong1, Sang Kook Lee2.
Abstract
Most nucleoside anticancer drugs show a primary resistance to p53-deficient or p53-mutated cancer cells and are limited in the clinic to the treatment of hematological malignancies. However, 2'-fluoro-4'-seleno-ara-C (F-Se-Ara-C), a new generation of cytarabine (Ara-C) analogs, exhibited potent antitumor activity against the p53-deficient prostate cancer cell line PC-3. The distinct activity of F-Se-Ara-C was achieved by targeting the synthetic lethal interaction between p53 and mitogen-activated protein kinase-activated protein kinase-2 (MK2). MK2 is a checkpoint effector for DNA damage responses to drive cell cycle arrest and DNA repair in p53-deficient cancer cells. Therefore, targeting MK2 may be an effective therapeutic strategy that induces apoptosis for cancers deficient in p53. F-Se-Ara-C effectively induced anti-prostate cancer activity in vitro and in vivo by inhibition of MK2 activation in p53-deficient prostate cancer cells. Moreover, combining F-Se-Ara-C with cabozantinib, an anticancer drug currently in clinical use, induced synergistic antitumor activity in p53-deficient prostate cancer cells. Taken together, these data show that F-Se-Ara-C may become great anticancer drug candidate with its unique mechanism of action for overcoming the apoptotic resistance of p53-deficient cells by targeting the synthetic lethal interaction.Entities:
Keywords: A nucleoside analog F–Se-Ara-C; Mitogen-activated protein kinase-activated protein kinase-2 (MK2) inhibition; Mitotic catastrophe; Synthetic lethality; p53-deficient cancer cells
Year: 2020 PMID: 33075425 DOI: 10.1016/j.canlet.2020.10.003
Source DB: PubMed Journal: Cancer Lett ISSN: 0304-3835 Impact factor: 8.679