Investigator

Elena Díaz-Rodríguez

Profesor Permanente Laboral · Universidad de Salamanca, Bioquímica y Biología Molecular

EDElena Díaz-Rodríg…
Papers(1)
Ocoxin Oral Solution …
Collaborators(1)
Atanasio Pandiella
Institutions(2)
Universidad De Salama…Consejo Superior de I…

Papers

Ocoxin Oral Solution Triggers DNA Damage and Cell Death in Ovarian Cancer

Ovarian cancer is the most fatal of all the reproductive cancers within the female population, mainly due to its late diagnosis that limits surgery and medical treatment. Classically, ovarian cancer therapy has included conventional chemotherapy, and other therapeutic approaches are now being used to treat these patients, but the outcomes of the disease are still poor. Therefore, new strategies are needed to improve life expectancy and life quality of ovarian cancer patients. Considering that, we investigated the effect of the nutritional supplement Ocoxin Oral Solution (OOS) in ovarian cancer models. OOS contains several nutritional supplements, some of them with demonstrated antitumoral action. In vitro studies showed that OOS inhibited the proliferation of several ovarian cancer cell lines, especially of those representative of the endometrioid subtype, in a time- and dose-dependent manner. A fast cell death induction after OOS treatment was observed, and when the molecular mechanisms leading to this effect were investigated, an activation of the DNA damage checkpoint was detected, as shown by activation (phosphorylation) of CHK1 and CHK2 kinases that was followed by the phosphorylation of the target protein histone H2AX. When tested in animal models of ovarian cancer, OOS reduced tumor growth without any observed secondary effects. Moreover, such reduction in tumor proliferation was caused by the induction of DNA damage as corroborated by the in vivo phosphorylation of CHK2 and Histone H2AX. Finally, OOS potentiated the action of carboplatin or olaparib, the standard of care treatments used in ovarian clinics, opening the possibility of including OOS in combination with those standard of care agents in patients with ovarian cancer.

38Works
1Papers
1Collaborators
Ovarian NeoplasmsCell Line, TumorXenograft Model Antitumor Assays

Positions

2021–

Profesor Permanente Laboral

Universidad de Salamanca · Bioquímica y Biología Molecular

2007–

Investigadora

Centro de Investigación del Cáncer

2002–

Investigadora Postdoctoral

Memorial Sloan Kettering Cancer Center

Education

1999

Doctora en Biología

Universidad de Salamanca · Departamento de Microbiología y Genética. Instituto de Microbiología Biooquímica

1992

Licenciada en Biología

Universidad de Salamanca · Facultad de Biología

Country

ES