A mathematical approach to differentiate spontaneous and induced evolution to drug resistance during cancer treatment

Greene, James M.; Gevertz, Jana L.; Sontag, Eduardo D.

doi:10.1101/235150

Cited by 19 publications

(39 citation statements)

References 83 publications

(200 reference statements)

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“…This is also the most common way in which the cost is modelled (e.g. [12,13,26]). Note that the factor of 2 in the drug response accounts for the fact that if a cell dies during mitosis not only the potential daughter but also the mother are lost.…”

Section: Mathematical Modelmentioning

confidence: 99%

Turnover modulates the need for a cost of resistance in adaptive therapy

Strobl

West

Viossat

et al. 2020

Preprint

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Control and conquer" -this is the philosophy behind adaptive therapy, which seeks to exploit intra-tumoural competition to avoid, or at least, delay the emergence of therapy resistance in cancer. Motivated by promising results from theoretical, experimental and, most recently, a clinical study in prostate cancer, there is an increasing interest in extending this approach to other cancers. As such, it is urgent to understand the characteristics of a cancer which determine whether it will respond well to adaptive therapy, or not. A plausible candidate for such a selection criterion is the fitness cost of resistance. In this 1 paper, we study a simple competition model between sensitive & resistant cell populations to investigate whether the presence of a cost is a necessary condition for adaptive therapy to extend the time to progression beyond that of a standard-of-care continuous therapy. We find that for tumours close to their environmental carrying capacity such a cost of resistance is not required. However, for tumours growing far from carrying capacity, a cost may be required to see meaningful gains. Notably, we show that in such cases it is important to consider the cell turnover in the tumour and we discuss its role in modulating the impact of a cost of resistance. Overall, our work helps to clarify under which circumstances adaptive therapy may be beneficial, and suggests that turnover may play an unexpectedly important role in the decision making process.

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Section: Mathematical Modelmentioning

confidence: 99%

Turnover modulates the need for a cost of resistance in adaptive therapy

Strobl

West

Viossat

et al. 2020

Preprint

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“…To describe and predict the dynamics of cancer cells in response to treatment, we use a mechanistic model that describes sensitive and resistant cell subpopulations growing, dying, and transitioning from the sensitive, S, to resistant, R, state as a direct result of treatment (17). In this model (Fig 1A), sensitive and resistant cells grow via a logistic growth hypothesis at their own intrinsic growth rates (rS and rR) and a joint carrying capacity (K), which will either take the value of KN for the carrying capacity of the cells in the longitudinal treatment experiment or Kf for the carrying capacity of the cells in the scRNA-seq experiment.…”

Section: Utilizing a Model Of Sensitive And Resistant Subpopulations mentioning

confidence: 99%

“…These models describe cancer cells dynamically growing and responding to drug with differential growth rates and drug sensitivities. Knowledge of these model parameters have enabled the theoretical optimization of treatment protocols (16)(17)(18), and have been applied successfully to prolong tumor control in both mice (12) and patients (14,19).…”

Section: Introductionmentioning

confidence: 99%

Integrating multimodal data sets into a mathematical framework to describe and predict therapeutic resistance in cancer

Johnson

Howard

Morgan

et al. 2020

Preprint

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A significant challenge in the field of biomedicine is the development of methods to integrate the multitude of dispersed data sets into comprehensive frameworks to be used to generate optimal clinical decisions. Recent technological advances in single cell analysis allow for high-dimensional molecular characterization of cells and populations, but to date, few mathematical models have attempted to integrate measurements from the single cell scale with other data types. Here, we present a framework that actionizes static outputs from a machine learning model and leverages these as measurements of state variables in a dynamic mechanistic model of treatment response. We apply this framework to breast cancer cells to integrate single cell transcriptomic data with longitudinal population-size data. We demonstrate that the explicit inclusion of the 1 2 J K L C O D − C O : , O R: DS J T UVWXU OY6

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“…Upon division, both daughter cells inherit mothers' damage level and tolerance level, while the drug absorbed by the mother cell is split into half between both daughter cells (18,38).…”

Section: Individual Cell Dynamicsmentioning

confidence: 99%

“…Feizabadi (17) used mathematical modeling to show that certain chemotherapy strategies are highly unsuccessful, and even damaging to the patient, under the assumption that the drug can induce resistance during the treatment period. Greene et al (18,19) developed mathematical approach to differentiate between spontaneous and induced resistance to drugs and proposed in vitro experiments that can determine weather treatment can induce resistance. The authors also designed optimized treatment protocols that can prolong the time before resistance develops.…”

Section: Introductionmentioning

confidence: 99%

Drug-induced resistance in micrometastases: analysis of spatio-temporal cell lineages

Pérez-Velázquez

Rejniak

2020

Preprint

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AbstractResistance to anti-cancer drugs is a major cause of treatment failure. While several intracellular mechanisms of resistance have been postulated, the role of extrinsic factors in the development of resistance in individual tumor cells is still not fully understood. Here we used a hybrid agent-based model to investigate how sensitive tumor cells develop drug resistance in the heterogeneous tumor microenvironment. We characterized the spatio-temporal evolution of lineages of the resistant cells and examined how resistance at the single-cell level contributes to the overall tumor resistance. We also developed new methods to track tumor cell adaptation, to trace cell viability trajectories and to examine the three-dimensional spatio-temporal lineage trees. Our findings indicate that drug-induced resistance can result from cells adaptation to the changes in drug distribution. Two modes of cell adaptation were identified that coincide with microenvironmental niches—areas sheltered by cell micro-communities (protectorates) or regions with limited drug penetration (refuga or sanctuaries). We also recognized that certain cells gave rise to lineages of resistant cells (precursors of resistance) and pinpointed three temporal periods and spatial locations at which such cells emerged. This supports the hypothesis that tumor micrometastases do not need to harbor cell populations with pre-existing resistance, but that individual tumor cells can adapt and develop resistance induced by the drug during the treatment.

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A mathematical approach to differentiate spontaneous and induced evolution to drug resistance during cancer treatment

Cited by 19 publications

References 83 publications

Turnover modulates the need for a cost of resistance in adaptive therapy

Turnover modulates the need for a cost of resistance in adaptive therapy

Integrating multimodal data sets into a mathematical framework to describe and predict therapeutic resistance in cancer

Drug-induced resistance in micrometastases: analysis of spatio-temporal cell lineages

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