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Modeling breast cancer proliferation, drug synergies, and alternating therapies.


ABSTRACT: Estrogen receptor positive (ER+) breast cancer is responsive to a number of targeted therapies used clinically. Unfortunately, the continuous application of targeted therapy often results in resistance, driving the consideration of combination and alternating therapies. Toward this end, we developed a mathematical model that can simulate various mono, combination, and alternating therapies for ER + breast cancer cells at different doses over long time scales. The model is used to look for optimal drug combinations and predicts a significant synergism between Cdk4/6 inhibitors in combination with the anti-estrogen fulvestrant, which may help explain the clinical success of adding Cdk4/6 inhibitors to anti-estrogen therapy. Furthermore, the model is used to optimize an alternating treatment protocol so it works as well as monotherapy while using less total drug dose.

SUBMITTER: He W 

PROVIDER: S-EPMC10206440 | biostudies-literature | 2023 May

REPOSITORIES: biostudies-literature

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Modeling breast cancer proliferation, drug synergies, and alternating therapies.

He Wei W   Demas Diane M DM   Shajahan-Haq Ayesha N AN   Baumann William T WT  

iScience 20230423 5


Estrogen receptor positive (ER+) breast cancer is responsive to a number of targeted therapies used clinically. Unfortunately, the continuous application of targeted therapy often results in resistance, driving the consideration of combination and alternating therapies. Toward this end, we developed a mathematical model that can simulate various mono, combination, and alternating therapies for ER + breast cancer cells at different doses over long time scales. The model is used to look for optima  ...[more]

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