Enhancement of chemotherapy using oncolytic virotherapy: Mathematical and optimal control analysis

  • Received: 27 March 2018 Accepted: 10 July 2018 Published: 01 December 2018
  • MSC : Primary: 49K15; Secondary: 92B05

  • Oncolytic virotherapy has been emerging as a promising novel cancer treatment which may be further combined with the existing therapeutic modalities to enhance their effects. To investigate how virotherapy could enhance chemotherapy, we propose an ODE based mathematical model describing the interactions between tumour cells, the immune response, and a treatment combination with chemotherapy and oncolytic viruses. Stability analysis of the model with constant chemotherapy treatment rates shows that without any form of treatment, a tumour would grow to its maximum size. It also demonstrates that chemotherapy alone is capable of clearing tumour cells provided that the drug efficacy is greater than the intrinsic tumour growth rate. Furthermore, virotherapy alone may not be able to clear tumour cells from body tissue but would rather enhance chemotherapy if viruses with high viral potency are used. To assess the combined effect of virotherapy and chemotherapy we use the forward sensitivity index to perform a sensitivity analysis, with respect to chemotherapy key parameters, of the virus basic reproductive number and the tumour endemic equilibrium. The results from this sensitivity analysis indicate the existence of a critical dose of chemotherapy above which no further significant reduction in the tumour population can be observed. Numerical simulations show that a successful combinational therapy of the chemotherapeutic drugs and viruses depends mostly on the virus burst size, infection rate, and the amount of drugs supplied. Optimal control analysis was performed, by means of the Pontryagin's maximum principle, to further refine predictions of the model with constant treatment rates by accounting for the treatment costs and sides effects. Results from this analysis suggest that the optimal drug and virus combination correspond to half their maximum tolerated doses. This is in agreement with the results from stability and sensitivity analyses.

    Citation: Joseph Malinzi, Rachid Ouifki, Amina Eladdadi, Delfim F. M. Torres, K. A. Jane White. Enhancement of chemotherapy using oncolytic virotherapy: Mathematical and optimal control analysis[J]. Mathematical Biosciences and Engineering, 2018, 15(6): 1435-1463. doi: 10.3934/mbe.2018066

    Related Papers:

  • Oncolytic virotherapy has been emerging as a promising novel cancer treatment which may be further combined with the existing therapeutic modalities to enhance their effects. To investigate how virotherapy could enhance chemotherapy, we propose an ODE based mathematical model describing the interactions between tumour cells, the immune response, and a treatment combination with chemotherapy and oncolytic viruses. Stability analysis of the model with constant chemotherapy treatment rates shows that without any form of treatment, a tumour would grow to its maximum size. It also demonstrates that chemotherapy alone is capable of clearing tumour cells provided that the drug efficacy is greater than the intrinsic tumour growth rate. Furthermore, virotherapy alone may not be able to clear tumour cells from body tissue but would rather enhance chemotherapy if viruses with high viral potency are used. To assess the combined effect of virotherapy and chemotherapy we use the forward sensitivity index to perform a sensitivity analysis, with respect to chemotherapy key parameters, of the virus basic reproductive number and the tumour endemic equilibrium. The results from this sensitivity analysis indicate the existence of a critical dose of chemotherapy above which no further significant reduction in the tumour population can be observed. Numerical simulations show that a successful combinational therapy of the chemotherapeutic drugs and viruses depends mostly on the virus burst size, infection rate, and the amount of drugs supplied. Optimal control analysis was performed, by means of the Pontryagin's maximum principle, to further refine predictions of the model with constant treatment rates by accounting for the treatment costs and sides effects. Results from this analysis suggest that the optimal drug and virus combination correspond to half their maximum tolerated doses. This is in agreement with the results from stability and sensitivity analyses.


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    [1] [M. Agarwal and A. S. Bhadauria, Mathematical modeling and analysis of tumor therapy with oncolytic virus, Journal of Applied Mathematics, 2 (2011), 131-140.
    [2] [T. Agrawal, M. Saleem and S. Sahu, Optimal control of the dynamics of a tumor growth model with hollings' type-Ⅱ functional response, Computational and Applied Mathematics, 33 (2014), 591-606.
    [3] [ M. Alonso, C. Gomez-Manzano, H. Jiang, N. B. Bekele, Y. Piao, W. K. A. Yung, R. Alemany and J. Fueyo, Combination of the oncolytic adenovirus icovir-5 with chemotherapy provides enhanced anti-glioma effect in vivo, Journal of Cancer Gene Therapy, 14 (2007), 756-761.
    [4] [ Z. Bajzer, T. Carr, K. Josic, S. J. Russell and D. Dingli, Modeling of cancer virotherapy with recombinant measles viruses, Journal of Theoretical Biology, 252 (2008), 109-122.
    [5] [M. Bartkowski, S. Bridges, P. Came, H. Eggers, P. Fischer, H. Friedmann, M. Green, C. Gurgo, J. Hay, B. D. Korant et al., Chemotherapy of viral infections, vol. 61, Springer Science & Business Media, 2012.
    [6] [S. Benzekry, C. Lamont, A. Beheshti, A. Tracz and J. M. L. Ebos, Classical mathematical models for description and prediction of experimental tumor growth, PLoS Comput Biol, 10 (2014), e1003800.
    [7] [M. Bertau, E. Mosekilde and H. V. Westerhoff, Biosimulation in Drug Development, John Wiley & Sons, 2008.
    [8] [ E. Binz and L. M. Ulrich, Chemovirotherapy: Combining chemotherapeutic treatment with oncolytic virotherapy, Oncolytic Virotherapy, 4 (2015), 39-48.
    [9] [ C. Bollard and H. HeslopS, T cells for viral infections after allogeneic hematopoietic stem cell transplant, Blood, 127 (2016), 3331-3340.
    [10] [G. J. Bostol and S. Patil, Carboplatin in clinical stage Ⅰ seminoma: too much and too little at the same time, Journal of Clinical Oncology, 29 (2011), 949-952.
    [11] [ T. D. Brock, The Emergence of Bacterial Genetics, Cold Spring Harbor Laboratory Press Cold Spring Harbor, New York, 1990.
    [12] [R. W. Carlson and B. I. Sikic, Continuous infusion or bolus injection in cancer chemotherapy, Annals of Internal Medicine, 99 (1983), 823-833.
    [13] [J. Crivelli, J. Földes, P. Kim and J. Wares, A mathematical model for cell cycle-specific cancer virotherapy, Journal of Biological Dynamics, 6 (2012), 104-120.
    [14] [ S. Dasari and P. Tchounwou, Cisplatin in cancer therapy: Molecular mechanisms of action, European Journal of Pharmacology, 740 (2014), 364-378.
    [15] [R. J. de Boer, Modeling Population Dynamics: A Graphical Approach, Utrecht University, 2018.
    [16] [ L. de Pillis, K. R. Fister, W. Gu, C. Collins, M. Daub, D. Gross, J. Moore and B. Preskill, Mathematical model creation for cancer chemo-immunotherapy, Journal of Computational and Mathematical Methods in Medicine, 10 (2009), 165-184.
    [17] [ W. Fleming and R. Rishel, Deterministic and Stochastic Optimal Control, vol. 1, Springer-Verlag, Berlin-New York, 1975.
    [18] [ E. Frei III and G. P. Canellos, Dose: a critical factor in cancer chemotherapy, The American Journal of Medicine, 69 (1980), 585-594.
    [19] [ T. Gajewski, H. Schreiber and Y. Fu, Innate and adaptive immune cells in the tumor microenvironment, Nature Immunology, 14 (2013), 1014-1022.
    [20] [ K. Garber, China approves world's first oncolytic virus therapy for cancer treatment, Journal of the National Cancer Institute, 98 (2006), 298-300.
    [21] [ V. Groh, J. Wu, C. Yee and T. Spies, Tumour-derived soluble MIC ligands impair expression of nkg2d and t-cell activation, Journal of Nature, 419 (2002), 734-738.
    [22] [ A. Howells, G. Marelli, N. Lemoine and Y. Wang, Oncolytic viruses-interaction of virus and tumor cells in the battle to eliminate cancer, Frontiers in Oncology, 7 (2017), 195.
    [23] [ E. Kelly and S. J. Russel, History of oncolytic viruses: Genesis to genetic engineering, Journal of Molecular Therapy, 15 (2007), 651-659.
    [24] [ S. Khajanchi and S. Banerjee, Stability and bifurcation analysis of delay induced tumor immune interaction model, Applied Mathematics and Computation, 248 (2014), 652-671.
    [25] [ D. Kirschner and J. Panetta, Modeling immunotherapy of the tumor-immune interaction, Journal of Mathematical Biology, 37 (1998), 235-252.
    [26] [ A. Konstorum, A. Vella, A. Adler and R. Laubenbacher, Addressing current challenges in cancer immunotherapy with mathematical and computational modeling, The Royal Society Interface, (2017), 146902.
    [27] [ D. Le, J. Miller and V. Ganusov, Mathematical modeling provides kinetic details of the human immune response to vaccination, Frontiers in Cellular and Infection Microbiology, 7 (2015), 00177.
    [28] [ T. C. Liau, E. Galanis and D. Kirn, Clinical trial results with oncolytic virotherapy: A century of promise, a decade of progress, Journal of Nature Clinical Practice Oncology, 4 (2007), 101-117.
    [29] [ W. Liu and H. I. Freedman, A mathematical model of vascular tumor treatment by chemotherapy, Journal of Mathematical and Computer Modelling, 42 (2005), 1089-1112.
    [30] [ J. Malinzi, A. Eladdadi and P. Sibanda, Modelling the spatiotemporal dynamics of chemovirotherapy cancer treatment, Journal of Biological Dynamics, 11 (2017), 244-274.
    [31] [ J. Malinzi, P. Sibanda and H. Mambili-Mamoboundou, Analysis of virotherapy in solid tumor invasion, Journal of Mathematical Biosciences, 263 (2015), 102-110.
    [32] [ S. Nayar, P. Dasgupta and C. Galustian, Extending the lifespan and efficacies of immune cells used in adoptive transfer for cancer immunotherapies-a review, Oncoimmunology, 4 (2015), e1002720.
    [33] [ A. Nguyen, L. Ho and Y. Wan, Chemotherapy and oncolytic virotherapy: Advanced tactics in the war against cancer, Frontiers in Oncology, 4 (2014), 00145.
    [34] [ A. S. Novozhilov, F. S. Berezovskaya, E. V. Koonin and G. P. Karev, Mathematical modeling of tumor therapy with oncolytic viruses: regimes with complete tumor elimination within the framework of deterministic models, Biology Direct, 1 (2006), 1-18.
    [35] [ R. T. D. Oliver, G. M. Mead, G. J. Rustin, J. S. Gordon, J. K. Joffe, N. Aass, R. Coleman, P. P. R. Gabe and S. P. Stenning, Randomized trial of carboplatin versus radiotherapy for stage Ⅰ seminoma: mature results on relapse and contralateral testis cancer rates in MRC TE19/EORTC 30982 study (ISRCTN27163214), Journal of Clinical Oncology, 29 (2011), 957-962.
    [36] [ P. K. Ottolino, J. S. Diallo, B. D. Lichty, J. C. Bell and J. A. McCart, Intelligent design: combination therapy with oncolytic viruses, Journal of Molecular Therapy, 18 (2010), 251-263.
    [37] [ R. Ouifki and G. Witten, A model of HIV-1 infection with HAART therapy and intracellular delays, Discrete and Continous Dynamical Systems Series B, 8 (2007), 229-240.
    [38] [S. T. R. Pinho, H. I. Freedman and F. K. Nani, A chemotherapy model for the treatment of cancer with metastasis, Journal of Mathematical and Computer Modelling, 36 (2002), 773-803.
    [39] [ S. T. R. Pinho, D. S. Rodrigues and P. F. A. Mancera, A mathematical model of chemotherapy response to tumour growth, Canadian Applied Math Quarterly, 19 (2011), 369-384.
    [40] [ S. Pinho, R. A. F. S. Bacelar and H. Freedman, A mathematical model for the effect of antiangiogenic therapy in the treatment of cancer tumours by chemotherapy, Nonlinear Analysis: Real World Applications, 14 (2013), 815-828.
    [41] [ L. Pontryagin, Mathematical Theory of Optimal Processes, CRC Press, 1987.
    [42] [ K. Relph, H. Pandha, G. Simpson, A. Melcher and K. Harrington, Cancer immunotherapy via combining oncolytic virotherapy with chemotherapy: recent advances, Oncolytic Virotherapy, 2016 (2016), 1-13.
    [43] [ S. J. Russel, K. W. Pengl and J. C. Bell, Oncolytic virotherapy, Journal of Nature Biotechnology, 30 (2012), 658-670.
    [44] [ B. J. Schroers, Ordinary Differential Equations: A Practical Guide, Cambridge University Press, 2011.
    [45] [ J. S. Spratt, J. S. Meyer and J. A. Spratt, Rates of growth of human solid neoplasms: Part i, Journal of Surgical Oncology, 60 (1995), 137-146.
    [46] [ H. Thieme, Mathematics in Population Biology, Princeton University Press, 2003.
    [47] [ J. P. Tian, The replicability of oncolytic virus: defining conditions in tumor virotherapy, Journal of Mathematical Biosciences and Engineering, 8 (2011), 841-860.
    [48] [ S. D. Undevia, A. G. Gomez and M. J. Ratain, Pharmacokinetic variability of anticancer agents, Nature Reviews Cancer, 5 (2005), 447-458.
    [49] [ G. Ungerechts, M. E. Frenzke, K. C. Yaiw, T. Miest, P. B. Johnston and R. Cattaneo, Mantle cell lymphoma salvage regimen: Synergy between a reprogrammed oncolytic virus and two chemotherapeutics, Gene Therapy, 17 (2010), 1506-1516.
    [50] [ J. R. Usher, Some mathematical models for cancer chemotherapy, Journal of Computers & Mathematics with Applications, 28 (1994), 73-80.
    [51] [ US Food and Drug Administration and others, FDA approves first-of-its-kind product for the treatment of melanoma. press release. october 27, 2015.
    [52] [ P. van den Driessche and J. Watmough, Reproduction numbers and sub-threshold endemic equilibria for compartmental models of disease transmission, Mathematical Biosciences, 180(2002), 29-48.
    [53] [Y. Wang, J. P. Tian and J. Wei, Lytic cycle: A defining process in oncolytic virotherapy, Journal of Applied Mathematical Modelling, 37 (2013), 5962-5978.
    [54] [ D. Wodarz, Viruses as antitumor weapons defining conditions for tumor remission, Journal of Cancer Research, 61 (2001), 3501-3507.
    [55] [ M. Yoshimori, H. Ookura, Y. Shimada, T. Yoshida, N. Okazaki, M. Yoshino and D. Saito, continuous infusion of anti-cancer drug with balloon infusors, Gan to Kagaku Ryoho. Cancer & Chemotherapy, 15 (1988), 3121-3125.
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