Consequences of cell-to-cell P-glycoprotein transfer on acquired multidrug resistance in breast cancer: a cell population dynamics model
Jennifer Pasquier, Pierre Magal, C\'eline Boulang\'e-Lecomte, Glenn, Webb, Frank Le Foll

TL;DR
This study combines experimental and mathematical modeling approaches to investigate how intercellular transfer of P-glycoprotein contributes to the spread of multidrug resistance in breast cancer cell populations, impacting treatment strategies.
Contribution
It provides the first combined experimental and mathematical analysis of P-gp transfer dynamics and its role in extragenetic multidrug resistance in breast cancer cells.
Findings
P-gp transfer occurs between resistant and sensitive cells.
P-gp distribution reorganizes over time in co-cultures.
Transfer rate depends on P-gp expression gradients.
Abstract
Cancer is a proliferation disease affecting a genetically unstable cell population, in which molecular alterations can be somatically inherited by genetic, epigenetic or extragenetic transmission processes, leading to a cooperation of neoplastic cells within tumoral tissue. The efflux protein P-glycoprotein (P gp) is overexpressed in many cancer cells and has known capacity to confer multidrug resistance to cytotoxic therapies. Recently, cell-to-cell P-gp transfers have been shown. Herein, we combine experimental evidence and a mathematical model to examine the consequences of an intercellular P-gp trafficking in the extragenetic transfer of multidrug resistance from resistant to sensitive cell subpopulations. We report cell-to-cell transfers of functional P-gp in co-cultures of a P-gp overexpressing human breast cancer MCF-7 cell variant, selected for its resistance towards…
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Taxonomy
TopicsDrug Transport and Resistance Mechanisms · Nanoparticle-Based Drug Delivery · Cancer therapeutics and mechanisms
