The Impact of Cell Density and Mutations in a Model of Multidrug Resistance in Solid Tumors

Greene, James M.; Lavi, Orit; Gottesman, Michael M.; Levy, Doron

doi:10.1007/s11538-014-9936-8

Cited by 42 publications

(48 citation statements)

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“…Mathematical modeling studies in particular have been used to explore both broad and detailed aspects of cancer drug resistance, as reviewed in [43,7,25]. The fundamental question of how the presence of drug resistant cells influences tumor dynamics and treatment outcomes has been thoroughly explored in mathematical models under a wide variety of assumptions [14,37,39,47,58,40,23,24,70,16,45,60,63,4,22,33,44,52,65,3,32,80,13,26,29,46,49,51,57,59,77,18,68,1,9,10,20]. Cancer models have also been utilized to assess how various underlying mechanisms contribute to the resistant phenotype [80,13,59,18,20], and to calculate the probability that drug resistance emerges within a specified time frame, be it before or during cancer treatment …”

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confidence: 99%

“…As examples, pre-existing BCR-ABL kinase domain mutations confer resistance to the tyrosine kinase inhibitor imatinib in chronic myeloid leukemia patients [66,36], and pre-existing MEK1 mutations confer resistance to BRAF inhibitors in melanoma patients [8]. Many mathematical models have considered how the presence of preexisting resistant cells impact cancer progression and treatment [37,39,58,40,23,24,70,16,60,63,4,22,44,3,32,80,29,49,57,59,77,68,9,10].On the other hand, acquired drug resistance broadly describes the case in which drug resistance develops during the course of therapy from a population of cells that were initially drug sensitive [34]. The term "acquired resistance" is really an umbrella term for two distinct phenomena, which complicates the study of acquired resistance.…”

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confidence: 99%

“…On the one hand there is resistance that is randomly acquired during the course of treatment, be it due to random genetic mutations or stochastic non-genetic phenotype switching [65]. This spontaneous form of acquired resistance has been considered in many mathematical models [14,39,47,58,40,23,24,45,4,22,33,44,52,32,80,26,46,51,57,10]. On the other hand, drug resistance can be induced (caused) by the drug itself [62,61,69,65,64].…”

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

Greene

Gevertz

Sontag

2017

Preprint

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Resistance to chemotherapy is a major impediment to the successful treatment of cancer. Classically, resistance has been thought to arise primarily through random genetic mutations, after which mutated cells expand via Darwinian selection. However, recent experimental evidence suggests that the progression to drug resistance need not occur randomly, but instead may be induced by the therapeutic agent itself. This process of resistance induction can be a result of genetic changes, or can occur through epigenetic alterations that cause otherwise drug-sensitive cancer cells to undergo phenotype switching. This relatively novel notion of resistance further complicates the already challenging task of designing treatment protocols that minimize the risk of developing drug resistance. In an effort to better understand resistance to treatment, we have developed a mathematical modeling framework that incorporates both random and drug-induced resistance. Our model demonstrates that the ability (or lack thereof) of a drug to induce resistance can result in qualitatively different responses to the same drug dose and delivery schedule. The importance of induced resistance in treatment response led us to ask if, in our model, one can determine the resistance induction rate of a drug for a given treatment protocol. Not only could we prove that the induction parameter in our model is theoretically identifiable, we have also proposed a possible in vitro protocol which could potentially be used to determine a treatment's propensity to induce resistance. (which was not peer-reviewed) is the author/funder, who has granted bioRxiv a license to display the preprint in perpetuity.The copyright holder for this preprint . http://dx.doi.org/10.1101/235150 doi: bioRxiv preprint first posted online Dec. 15, 2017; Tumor resistance to chemotherapy and targeted drugs is a major cause of treatment failure. Both molecular and microenvironmental factors have been implicated in the development of drug resistance [34]. As an example of molecular resistance, the upregulation of drug efflux transporters can prevent sufficiently high intracellular drug accumulation, limiting treatment efficacy [31]. Other molecular causes of drug resistance include modification of drug targets, enhanced DNA damage repair mechanisms, dysregulation of apoptotic pathways, and the presence of cancer stem cells [31,17,34,78,81]. The irregular tumor vasculature which results in inconsistent drug distribution and hypoxia is an example of a microenvironmental factor that impacts drug resistance [76]. Other characteristics of the tumor microenvironment that influence drug resistance include regions of acidity, immune cell infiltration and activation, and the tumor stroma [27,76,56,15,34,55].Research continues to shed light on the multitude of factors that contribute to cancer drug resistance. Mathematical modeling studies in particular have been used to explore both broad and detailed aspects of cancer drug resistance, as reviewed in [43,7,25]. The fundamental ques...

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

Greene

Gevertz

Sontag

2017

Preprint

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“…Quite recently, continuous models structured according to a phenotypic trait and based on integrodifferential equations, are common in ecology and are based on Darwinian selection principles, applied to the problem of emergence-and its overcoming by combinations of cytotoxic and cytostatic drugs-of drug resistant subpopulations in cancer cell populations, have been proposed [57,71,77]. They offer the advantage of allowing the possibility to represent slow evolution, according to the expression of a phenotype rather than by jumps due to pointwise mutations, of a cancer cell population, a feature which makes them amenable to represent epigenetic modifications on which drug-induced drug resistance is likely to rely when it is reversible.…”

Section: Taking Drug Resistance Into Accountmentioning

confidence: 99%

Deterministic Mathematical Modelling for Cancer Chronotherapeutics: Cell Population Dynamics and Treatment Optimization

Clairambault¹

2014

Mathematical Oncology 2013

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In this short review paper, I will present the mathematical models that have been designed in the frame of continuous deterministic cell population dynamics that aim at optimization of cancer treatments using chronotherapeutics. Many authors have dealt with chronobiology of cancer, less with continuous mathematical models and even less with the declared aim to optimize chronotherapeutics. The biological and theoretical bases for these models are sketched, started from a historical viewpoint, and the main theoretical results are presented, with biological suggestions to account for them. Chronotherapeutics that leads to therapeutic optimization with the constraint of limiting unwanted toxicity of anticancer drugs towards healthy cell populations is put in a medical perspective together with the other main pitfall of cancer therapeutics, for which optimization procedures should have little to do with circadian biology, i.e., emergence of drug resistance in cancer cell populations, which is amenable to the use of other sorts of models, that are briefly mentioned.

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“…Many models have studied some of the key phenomena involved from the theoretical point of view (See, e.g., the review by Lorz et al (2013) or Lavi et al (2013), Greene et al (2014) and references therein).…”

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Transfer of Drug Resistance Characteristics Between Cancer Cell Subpopulations: A Study Using Simple Mathematical Models

Durán

Podolski-Renić²,

Álvarez-Arenas

et al. 2016

Bull Math Biol

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Resistance to chemotherapy is a major cause of cancer treatment failure. The processes of resistance induction and selection of resistant cells (due to the over-expression of the membrane transporter P-glycoprotein, P-gp) are well documented in the literature, and a number of mathematical models have been developed. However, another process of transfer of resistant characteristics is less well known and has received little attention in the mathematical literature. In this paper, we discuss the potential of simple mathematical models to describe the process of resistance transfer, specifically P-gp transfer, in mixtures of resistant and sensitive tumor cell populations. Two different biological hypotheses for P-gp transfer are explored: (1) exchange through physical cell-cell connections and (2) through microvessicles released to the culture medium. Two models are developed which fit very well the observed population growth dynamics. The potential and limitations of these simple "global" models to describe the aforementioned biological processes involved are discussed on the basis of the results obtained.

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The Impact of Cell Density and Mutations in a Model of Multidrug Resistance in Solid Tumors

Cited by 42 publications

References 45 publications

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

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

Deterministic Mathematical Modelling for Cancer Chronotherapeutics: Cell Population Dynamics and Treatment Optimization

Transfer of Drug Resistance Characteristics Between Cancer Cell Subpopulations: A Study Using Simple Mathematical Models

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