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@article{1506137, author = {Gomes, Sara and Raimundo, Liliana Sofia Gomes and Soares, Joana and Loureiro, Joana B. and Leao, Mariana and Nogueira Ramos Rocha, Helena Isabel and Monteiro, Madalena N. and Lemos, Agostinho and Moreira, Joana and Pinto, Madalena and Chlapek, Petr and Veselská, Renata and Sousa, Emília and Saraiva, Lucília}, article_location = {County Clare}, article_number = {4}, doi = {http://dx.doi.org/10.1016/j.canlet.2019.01.014}, keywords = {p73; Carbaldehydic xanthone; Anticancer therapy}, language = {eng}, issn = {0304-3835}, journal = {Cancer Letters}, title = {New inhibitor of the TAp73 interaction with MDM2 and mutant p53 with promising antitumor activity against neuroblastoma}, url = {https://www.sciencedirect.com/science/article/pii/S0304383519300266}, volume = {446}, year = {2019} }
TY - JOUR ID - 1506137 AU - Gomes, Sara - Raimundo, Liliana Sofia Gomes - Soares, Joana - Loureiro, Joana B. - Leao, Mariana - Nogueira Ramos Rocha, Helena Isabel - Monteiro, Madalena N. - Lemos, Agostinho - Moreira, Joana - Pinto, Madalena - Chlapek, Petr - Veselská, Renata - Sousa, Emília - Saraiva, Lucília PY - 2019 TI - New inhibitor of the TAp73 interaction with MDM2 and mutant p53 with promising antitumor activity against neuroblastoma JF - Cancer Letters VL - 446 IS - 4 SP - 90-102 EP - 90-102 PB - ELSEVIER IRELAND LTD SN - 03043835 KW - p73 KW - Carbaldehydic xanthone KW - Anticancer therapy UR - https://www.sciencedirect.com/science/article/pii/S0304383519300266 L2 - https://www.sciencedirect.com/science/article/pii/S0304383519300266 N2 - TAp73 is a key tumor suppressor protein, regulating the transcription of unique and shared p53 target genes with crucial roles in tumorigenesis and therapeutic response. As such, in tumors with impaired p53 signaling, like neuroblastoma, TAp73 activation represents an encouraging strategy, alternative to p53 activation, to suppress tumor growth and chemoresistance. In this work, we report a new TAp73-activating agent, the 1-carbaldehyde-3,4-dimethoxyxanthone (LEM2), with potent antitumor activity. Notably, LEM2 was able to release TAp73 from its interaction with both MDM2 and mutant p53, enhancing TAp73 transcriptional activity, cell cycle arrest, and apoptosis in p53-null and mutant p53-expressing tumor cells. Importantly, LEM2 displayed potent antitumor activity against patient-derived neuroblastoma cells, consistent with an activation of the TAp73 pathway. Additionally, potent synergistic effects were obtained for the combination of LEM2 with doxorubicin and cisplatin in patient-derived neuroblastoma cells. Collectively, besides its relevant contribution to the advance of TAp73 pharmacology, LEM2 may pave the way to improved therapeutic alternatives against neuroblastoma. ER -
GOMES, Sara, Liliana Sofia Gomes RAIMUNDO, Joana SOARES, Joana B. LOUREIRO, Mariana LEAO, Helena Isabel NOGUEIRA RAMOS ROCHA, Madalena N. MONTEIRO, Agostinho LEMOS, Joana MOREIRA, Madalena PINTO, Petr CHLAPEK, Renata VESELSKÁ, Emília SOUSA and Lucília SARAIVA. New inhibitor of the TAp73 interaction with MDM2 and mutant p53 with promising antitumor activity against neuroblastoma. \textit{Cancer Letters}. County Clare: ELSEVIER IRELAND LTD, 2019, vol.~446, No~4, p.~90-102. ISSN~0304-3835. Available from: https://dx.doi.org/10.1016/j.canlet.2019.01.014.
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