The logic of containing tumors

Viossat, Yannick; Noble, Robert

doi:10.1101/2020.01.22.915355

Cited by 16 publications

(36 citation statements)

References 35 publications

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“…We have shown that high initial tumour cell density, and low initial resistance fractions, maximise the benefit of adaptive therapy, assuming a cure is not possible. This prediction is consistent with previous non-spatial [11,15,16,18,22,33] and spatial theoretical studies [11,19], and experimental evidence in cancer [11] and bacteria [34].…”

Section: Discussionsupporting

confidence: 92%

Spatial structure impacts adaptive therapy by shaping intra-tumoral competition

Strobl

Gallaher

West

et al. 2020

Preprint

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(1) Background: Adaptive therapy aims to tackle cancer drug resistance by leveraging intra-tumoural competition between drug-sensitive and resistant cells. Motivated by promising results in prostate cancer there is growing interest in extending this approach to other cancers. Here we present a theoretical study of intra-tumoural competition during adaptive therapy, to identify under which circumstances it will be superior to aggressive treatment, and how it can be improved through combination treatment; (2) Methods: We study a 2-D, on-lattice, agent-based tumour model. We examine the impact of different micro-environmental factors on the comparison between continuous drug administration and the adaptive schedule pioneered in the first-in-human clinical trial. (3) Results: We show that the degree of crowding, the initial resistance fraction, the presence of possible resistance costs, and the rate of tumour cell turnover are key determinants of the benefit of adaptive therapy. Subsequently, we investigate whether combination with treatments which amplify proliferation or which target cell turnover can prolong tumour control. While the former increases competition, we find that only the latter can robustly improve time to progression; (4) Conclusion: Our work helps to identify selection factors for adaptive therapy and provides stepping stones towards the rational design of multi-drug adaptive regimens.

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Section: Discussionsupporting

confidence: 92%

Spatial structure impacts adaptive therapy by shaping intra-tumoral competition

Strobl

Gallaher

West

et al. 2020

Preprint

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“…). As Hansen et al[8] and Viossat and Noble[32] show, if one accounts for potential de novo resistance acquisition, this high burden can generate situations in which maintaining a pool of sensitive cells can in fact accelerate the emergence of the resistant population. Investigating the risks associated with the higher average tumour burden under adaptive therapy is an important area of future research.…”

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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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“…This criterion was implemented in the first clinical trial of adaptive therapy for castrateresistant prostate cancer (20). Would a less aggressive treatment stop criterion be better as suggested by more recent models (27,28,34)? We simulated a suite of adaptive therapy simulations with a new stopping criterion of 20% reduction to address this question.…”

Section: A Different Treatment-stopping Criterionmentioning

confidence: 99%

“…Strobl et al showed how the turnover rate of cancer cells within the tumor influences benefits derived from adaptive therapy (27). More general and deeper mathematical analysis by Viossat and Noble predict the clinical benefits of tumor containment therapy (28).…”

Section: Introductionmentioning

confidence: 99%

Understanding the potential benefits of adaptive therapy for metastatic melanoma

Kim

Brown

Eroglu

et al. 2020

Preprint

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Adaptive therapy is an evolution-based treatment approach that aims to maintain tumor volume by employing minimum effective drug doses or timed drug holidays. For successful adaptive therapy outcomes, it is critical to find the optimal timing of treatment switch points. Mathematical models are ideal tools to facilitate adaptive therapy dosing and switch time points. We developed two different mathematical models to examine interactions between drug-sensitive and resistant cells in a tumor. The first model assumes genetically fixed drug-sensitive and resistant populations that compete for limited resources. Resistant cell growth is inhibited by sensitive cells. The second model considers phenotypic switching between drug-sensitive and resistant cells. We calibrated each model to fit melanoma patient biomarker changes over time and predicted patient-specific adaptive therapy schedules. Overall, the models predict that adaptive therapy would have delayed time to progression by 6-25 months compared to continuous therapy with dose rates of 6%-74% relative to continuous therapy. We identified predictive factors driving the clinical time gained by adaptive therapy. The first model predicts 6-20 months gained from continuous therapy when the initial population of sensitive cells is large enough, and when the sensitive cells have a large competitive effect on resistant cells. The second model predicts 20-25 months gained from continuous therapy when the switching rate from resistant to sensitive cells is high and the growth rate of sensitive cells is low. This study highlights that there is a range of potential patient specific benefits of adaptive therapy, depending on the underlying mechanism of resistance, and identifies tumor specific parameters that modulate this benefit.

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The logic of containing tumors

Cited by 16 publications

References 35 publications

Spatial structure impacts adaptive therapy by shaping intra-tumoral competition

Spatial structure impacts adaptive therapy by shaping intra-tumoral competition

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

Understanding the potential benefits of adaptive therapy for metastatic melanoma

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