CAR T cell therapy in B-cell acute lymphoblastic leukaemia: Insights from mathematical models

León-Triana, Odelaisy; Sabir, Soukaina; Calvo, Gabriel F.; Belmonte-Beitia, Juan; Chulián, Salvador; Martínez-Rubio, Álvaro; Rosa, María; Pérez‐Martínez, Antonio; Ramírez-Orellana, Manuel; Pérez-Garcı́a, Vı́ctor M.

doi:10.1101/2020.03.18.20038257

Cited by 4 publications

(10 citation statements)

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“…The maximum mitotic rate ρ C and ρC, related to the stimulation effect of the T cells by the interaction with the targets (CD 19 + or tumour antigen), will depend on the properties of the CAR-T product. These parameters will be taken in the range 0.2-0.9 day −1 according to the values reported in other models [26,37] and in agreement with the fact that stimulated CAR-T cells can perform a few mitotic divisions per day. For current CAR-T products the mean lifetime τ C of activated CAR T cells is in the range of 1-4 weeks [38].…”

Section: Parameter Estimationmentioning

confidence: 98%

“…Eqs. (2a-2b) describe the off-tumour interaction between CAR-T and B cells as in previous works [26] term represents natural cell death, where τ C is the activated CAR-T lifespan. Finally, the term −kC represents the traffic of CAR-T cells to brain areas having active GBM cells, where 0 < k < 1 is the average fraction of CAR-T cells crossing the blood-brain barrier (BBB) and infiltrating the tumour site.…”

Section: Modelling Car-t Cells Targetting On-tumour and Off-tumour Anmentioning

confidence: 99%

“…We will assume that in dual therapy, CAR-T cells are injected after lymphoid depletion treatment to promote expansion of CAR-T by stimulation with B cells as usual. We set the initial number of B lymphocytes to be 2.5 ×10 10 to account for the effect of this treatment [26].…”

Section: Parameter Estimationmentioning

confidence: 99%

“…To do so, we neglected the immune suppression term, that is not present in leukaemias and the parameters related to the type of cancer were chosen as in Ref. [26]. We obtained values of g T and g B around 1-2 ×10 10 cell.…”

Section: Parameter Estimationmentioning

confidence: 99%

“…Mathematical modelling has the potential to help in finding optimal administration protocols, provide a deeper understanding of the dynamics, help in the design of clinical trials and more [19,20]. Some recent mathematical modelling studies have been performed studying different aspects of CAR-T cell therapies [21][22][23][24][25][26][27][28]. In this paper we study in-silico, using a mathematical model, the response of a solid tumour to a dual CAR-T product targeting both CD19 and a tumour-associated antigen.…”

Section: Introductionmentioning

confidence: 99%

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Dual-Target Car-Ts With on- and off-Tumour Activity May Override Immune Suppression in Solid Cancers: A Mathematical Proof of Concept

León-Triana¹,

Pérez‐Martínez²,

Ramírez-Orellana³

et al. 2020

Preprint

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Chimeric antigen receptor (CAR)-T cell-based therapies have achieved substantial successes against B-cell malignancies, what has led to a growing scientific and clinical interest on extending their use to solid cancers. However, results for solid tumours have been limited up to now, in part due to the immuno-suppressive tumour microenvironment, that is able to inactivate CAR-T cell clones. In this paper we put forward a mathematical model describing the competition of CAR-T and tumour cells, accounting for their immunosuppressive capabilities. Using the mathematical model, we show that the use of large numbers of CAR-T cells targeting the solid tumour antigens could overcome the cancer immunosuppressive potential. To achieve such high levels of CAR-T cells we propose and study computationaly, the manufacture and injection of CAR-T cells targeting two antigens: CD19 and a tumour-associated antigen. We study in-silico the resulting dynamics of the disease after the injection of this product and find that the expansion of the CAR-T cell population in the blood and lymphopoietic organs could lead to the massive generation of an army of CAR-T cells targetting the solid tumour, and potentially overcoming its inmune suppression capabilities. That strategy could benefit from the combination with PD-1 inhibitors and of low tumour loads. Our computational results provide a theoretical support for the treatment of different types of solid tumours using T-cells engineered with combination treatments of dual CARs with on- and off-tumour activity and anti-PD1 drugs after completion of classical cytoreductive treatments.

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Section: Parameter Estimationmentioning

confidence: 98%

Section: Modelling Car-t Cells Targetting On-tumour and Off-tumour Anmentioning

confidence: 99%

Section: Parameter Estimationmentioning

confidence: 99%

Section: Parameter Estimationmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Dual-Target Car-Ts With on- and off-Tumour Activity May Override Immune Suppression in Solid Cancers: A Mathematical Proof of Concept

León-Triana¹,

Pérez‐Martínez²,

Ramírez-Orellana³

et al. 2020

Preprint

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The Growth Laws of Brain Metastases

Ocaña-Tienda

Pérez-Beteta

Molina-García

et al. 2022

Preprint

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Tumor growth is the result of the interplay of complex biological processes in a huge number of individual cells in a changing environment. Effective simple mathematical laws have been shown to describe tumor growth in vitro, or in animal models with bounded-growth dynamics accurately. However, results for human cancers in patients are scarce. The study mined a dataset of 1133 brain metastases (BMs) with longitudinal imaging follow-up, treated with radiosurgery (SRS) to find growth laws for untreated BMs, relapsing treated BMs, and radiation necrosis (RN). Untreated BMs showed sustained growth acceleration, most likely related to the underlying evolutionary dynam- ics. Relapsing BM growth was slower, most probably due to a reduction in tumor heterogeneity after SRS, which may limit the evolutionary possibilities of the tumor. RN lesions had significantly larger growth exponents than relapsing BMs, providing a way to differentiate them from true pro- gression. This may help in solving a problem of clinical relevance, since the first condition may resolve spontaneously, and not require further work-up, while the second requires therapeutic action.

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Dynamical properties of feedback signalling in B lymphopoiesis: A mathematical modelling approach

Chulián,

Martínez-Rubio,

Marciniak-Czochra

et al. 2020

Preprint

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Haematopoiesis is the process of generation of blood cells. Lymphopoiesis generates lymphocytes, the cells in charge of the adaptive immune response. Disruptions of this process are associated with diseases like leukaemia, which is especially incident in children. The characteristics of self-regulation of this process make them suitable for a mathematical study.In this paper we develop mathematical models of lymphopoiesis using currently available data. We do this by drawing inspiration from existing structured models of cell lineage development and integrating them with paediatric bone marrow data, with special focus on regulatory mechanisms. A formal analysis of the models is carried out, giving steady states and their stability conditions. We use this analysis to obtain biologically relevant regions of the parameter space and to understand the dynamical behaviour of B-cell renovation. Finally, we

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CAR T cell therapy in B-cell acute lymphoblastic leukaemia: Insights from mathematical models

Cited by 4 publications

References 50 publications

Dual-Target Car-Ts With on- and off-Tumour Activity May Override Immune Suppression in Solid Cancers: A Mathematical Proof of Concept

Dual-Target Car-Ts With on- and off-Tumour Activity May Override Immune Suppression in Solid Cancers: A Mathematical Proof of Concept

The Growth Laws of Brain Metastases

Dynamical properties of feedback signalling in B lymphopoiesis: A mathematical modelling approach

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