Your search keyword '"Senra, Joana M"' showing total 3 results

1. Preclinical testing of an Atr inhibitor demonstrates improved response to standard therapies for esophageal cancer.

Author

Leszczynska, Katarzyna B., Dobrynin, Greg, Leslie, Rhea E., Ient, Jonathan, Boumelha, Adam J., Senra, Joana M., Hawkins, Maria A., Maughan, Tim, Mukherjee, Somnath, and Hammond, Ester M.

Subjects

*TREATMENT of esophageal cancer, *CHEMORADIOTHERAPY, *CISPLATIN, *CARBOPLATIN, *CELL lines, *THERAPEUTICS

Abstract

Background and purpose Esophageal cancer has a persistently low 5-year survival rate and has recently been classified as a cancer of unmet need by Cancer Research UK. Consequently, new approaches to therapy are urgently required. Here, we tested the hypothesis that an ATR inhibitor, VX-970, used in combination with standard therapies for esophageal cancer could improve treatment outcome. Material and methods Using esophageal cancer cell lines we evaluated the efficacy of combining VX-970 with cisplatin and carboplatin in vitro and with radiation in vitro and in vivo . Radiation experiments were also carried out in hypoxic conditions to mimic the tumor microenvironment. Results Combining VX-970 with cisplatin, carboplatin and radiation increased tumor cell kill in vitro . A significant tumor growth delay was observed when VX-970 was combined with radiotherapy in vivo . Conclusions VX-970 is an effective chemo/radiosensitizer which could be readily integrated in the current treatment paradigm to improve the treatment response in esophageal cancer and we plan to test it prospectively in the forthcoming phase I dose escalation safety study combining the ATR inhibitor VX-970 with chemoradiotherapy in esophageal cancer (EudraCT number: 2015-003965-27). [ABSTRACT FROM AUTHOR]

Published

2016

2. HIF-1α-independent hypoxia-induced rapid PTK6 stabilization is associated with increased motility and invasion.

Author

Pires, Isabel M., Blokland, Nina J. G., Broos, Agnieke W. T., Poujade, Flore-Anne, Senra, Joana M., Eccles, Suzanne A., Span, Paul N., Harvey, Amanda J., and Hammond, Ester M.

Published

2014

3. Replication Stress and Chromatin Context Link ATM Activation to a Role in DNA Replication.

Author

Olcina, Monica?M., Foskolou, Iosifina?P., Anbalagan, Selvakumar, Senra, Joana?M., Pires, Isabel?M., Jiang, Yanyan, Ryan, Anderson?J., and Hammond, Ester?M.

Subjects

*DNA replication, *CHROMATIN, *DNA damage, *CARCINOGENESIS, *HETEROCHROMATIC genes, *HYPOXIA-inducible factors

Abstract

Summary: ATM-mediated signaling in response to DNA damage is a barrier to tumorigenesis. Here we asked whether replication stress could also contribute to ATM signaling. We demonstrate that, in the absence of DNA damage, ATM responds to replication stress in a hypoxia-induced heterochromatin-like context. In certain hypoxic conditions, replication stress occurs in the absence of detectable DNA damage. Hypoxia also induces H3K9me3, a histone modification associated with gene repression and heterochromatin. Hypoxia-induced replication stress together with increased H3K9me3 leads to ATM activation. Importantly, ATM prevents the accumulation of DNA damage in hypoxia. Most significantly, we describe a stress-specific role for ATM in maintaining DNA replication rates in a background of increased H3K9me3. Furthermore, the ATM-mediated response to oncogene-induced replication stress is enhanced in hypoxic conditions. Together, these data indicate that hypoxia plays a critical role in the activation of the DNA damage response, therefore contributing to this barrier to tumorigenesis. [Copyright &y& Elsevier]

Published

2013