A model-based approach to the in vitro evaluation of anticancer activity Export

@article{citeulike:4255462, abstract = {Abstract Purpose\ \ The use of in vitro screening tests for characterizing the activity of anticancer agents is a standard practice in oncology research and development. In these studies, human A2780 ovarian carcinoma cells cultured in plates are exposed to different concentrations of the compounds for different periods of time. Their anticancer activity is then quantified in terms of EC50 comparing the number of metabolically active cells present in the treated and the control arms at specified time points. The major concern of this methodology is the observed dependency of the EC50 on the experimental design in terms of duration of exposure. This dependency could affect the efficacy ranking of the compounds, causing possible biases especially in the screening phase, when compound selection is the primary purpose of the in vitro analysis. To overcome this problem, the applicability of a modeling approach to these in vitro studies was evaluated. Methods\ \ The model, consisting of a system of ordinary differential equations, represents the growth of tumor cells using a few identifiable and biologically relevant parameters related to cell proliferation dynamics and drug action. In particular, the potency of the compounds can be measured by a unique and drug-specific parameter that is essentially independent of drug concentration and exposure time. Parameter values were estimated using weighted nonlinear least squares. Results\ \ The model was able to adequately describe the growth of tumor cells at different experimental conditions. The approach was validated both on commercial drugs and discovery candidate compounds. In addition, from this model the relationship between EC50 and the exposure time was derived in an analytic form. Conclusions\ \ The proposed approach provides a new tool for predicting and/or simulating cell responses to different treatments with useful indications for optimizing in vitro experimental designs. The estimated potency parameter values obtained from different compounds can be used for an immediate ranking of anticancer activity.}, author = {Del Bene, Francesca and Germani, Massimiliano and De Nicolao, Giuseppe and Magni, Paolo and Re, Claudia and Ballinari, Dario and Rocchetti, Maurizio}, citeulike-article-id = {4255462}, citeulike-linkout-0 = {http://dx.doi.org/10.1007/s00280-008-0798-3}, citeulike-linkout-1 = {http://www.springerlink.com/content/1272p6q121100606}, doi = {10.1007/s00280-008-0798-3}, journal = {Cancer Chemotherapy and Pharmacology}, keywords = {activity, modelization, vitro}, posted-at = {2009-04-02 09:45:03}, priority = {2}, title = {A model-based approach to the in vitro evaluation of anticancer activity}, url = {http://dx.doi.org/10.1007/s00280-008-0798-3} }

TY - JOUR ID - citeulike:4255462 L3 - citeulike-article-id:4255462 N2 - Abstract Purpose  The use of in vitro screening tests for characterizing the activity of anticancer agents is a standard practice in oncology research and development. In these studies, human A2780 ovarian carcinoma cells cultured in plates are exposed to different concentrations of the compounds for different periods of time. Their anticancer activity is then quantified in terms of EC50 comparing the number of metabolically active cells present in the treated and the control arms at specified time points. The major concern of this methodology is the observed dependency of the EC50 on the experimental design in terms of duration of exposure. This dependency could affect the efficacy ranking of the compounds, causing possible biases especially in the screening phase, when compound selection is the primary purpose of the in vitro analysis. To overcome this problem, the applicability of a modeling approach to these in vitro studies was evaluated. Methods  The model, consisting of a system of ordinary differential equations, represents the growth of tumor cells using a few identifiable and biologically relevant parameters related to cell proliferation dynamics and drug action. In particular, the potency of the compounds can be measured by a unique and drug-specific parameter that is essentially independent of drug concentration and exposure time. Parameter values were estimated using weighted nonlinear least squares. Results  The model was able to adequately describe the growth of tumor cells at different experimental conditions. The approach was validated both on commercial drugs and discovery candidate compounds. In addition, from this model the relationship between EC50 and the exposure time was derived in an analytic form. Conclusions  The proposed approach provides a new tool for predicting and/or simulating cell responses to different treatments with useful indications for optimizing in vitro experimental designs. The estimated potency parameter values obtained from different compounds can be used for an immediate ranking of anticancer activity. JF - Cancer Chemotherapy and Pharmacology TI - A model-based approach to the in vitro evaluation of anticancer activity KW - activity KW - modelization KW - vitro AU - Del Bene, Francesca AU - Germani, Massimiliano AU - De Nicolao, Giuseppe AU - Magni, Paolo AU - Re, Claudia AU - Ballinari, Dario AU - Rocchetti, Maurizio UR - http://dx.doi.org/10.1007/s00280-008-0798-3 ER -