676 research outputs found

    Optimal Controlled Trajectories for a Mathematical Model of Anti-Angiogenic Therapy in Cancer

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    Abstract-Anti-angiogenic therapy is a novel treatment approach in cancer therapy that aims at preventing a tumor from developing a network of blood vessels and capillaries that it needs for its supply of nutrients to further its growth. In this paper, a mathematical model for anti-angiogenic treatment that is based on a biologically validated model by Hahnfeldt, Panigrahy, Folkman and Hlatky is considered. Using geometric methods from optimal control theory, in [20] a full solution was given for the problem of scheduling an a priori given amount of anti-angiogenic agents when dosage and effectiveness of the agent are identified. The anchor piece of the optimal synthesis is an order 1 singular arc whose control saturates. In this paper the structure of this optimal synthesis near the saturation point is developed in detail

    A Review of Mathematical Models for the Formation of\ud Vascular Networks

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    Mainly two mechanisms are involved in the formation of blood vasculature: vasculogenesis and angiogenesis. The former consists of the formation of a capillary-like network from either a dispersed or a monolayered population of endothelial cells, reproducible also in vitro by specific experimental assays. The latter consists of the sprouting of new vessels from an existing capillary or post-capillary venule. Similar phenomena are also involved in the formation of the lymphatic system through a process generally called lymphangiogenesis.\ud \ud A number of mathematical approaches have analysed these phenomena. This paper reviews the different modelling procedures, with a special emphasis on their ability to reproduce the biological system and to predict measured quantities which describe the overall processes. A comparison between the different methods is also made, highlighting their specific features

    Tumor Growth Control by TP-LPV-LMI Based Controller

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    Deterministic and stochastic study for a microscopic angiogenesis model: applications to the Lewis lung carcinoma

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    Angiogenesis modelling is an important tool to understand the underlying mechanisms yielding tumour growth. Nevertheless, there is usually a gap between models and experimental data. We propose a model based on the intrinsic microscopic reactions defining the angiogenesis process to link experimental data with previous macroscopic models. The microscopic characterisation can describe the macroscopic behaviour of the tumour, which stability analysis reveals a set of predicted tumour states involving different morphologies. Additionally, the microscopic description also gives a framework to study the intrinsic stochasticity of the reactive system through the resulting Langevin equation. To follow the goal of the paper, we use available experimental information on the Lewis lung carcinoma to infer meaningful parameters for the model that are able to describe the different stages of the tumour growth. Finally we explore the predictive capabilities of the fitted model by showing that fluctuations are determinant for the survival of the tumour during the first week and that available treatments can give raise to new stable tumour dormant states with a reduced vascular network

    Optimisation of cancer drug treatments using cell population dynamics

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    International audienceCancer is primarily a disease of the physiological control on cell population proliferation. Tissue proliferation relies on the cell division cycle: one cell becomes two after a sequence of molecular events that are physiologically controlled at each step of the cycle at so-called checkpoints, in particular at transitions between phases of the cycle [105]. Tissue proliferation is the main physiological process occurring in development and later in maintaining the permanence of the organism in adults, at that late stage mainly in fast renewing tissues such as bone marrow, gut and skin
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