Abstract
The physiome is the quantitative description of the functioning organism in normal and pathophysiological states. The human physiome can be regarded as the virtual human. It is built upon the morphome, the quantitative description of anatomical structure, chemical and biochemical composition, and material properties of an intact organism, including its genome, proteome, cell, tissue, and organ structures up to those of the whole intact being. The Physiome Project is a multicentric integrated program to design, develop, implement, test and document, archive and disseminate quantitative information, and integrative models of the functional behavior of molecules, organelles, cells, tissues, organs, and intact organisms from bacteria to man. A fundamental and major feature of the project is the databasing of experimental observations for retrieval and evaluation. Technologies allowing many groups to work together are being rapidly developed. Internet II will facilitate this immensely. When problems are huge and complex, a particular working group can be expert in only a small part of the overall project. The strategies to be worked out must therefore include how to pull models composed of many submodules together even when the expertise in each is scattered amongst diverse institutions. The technologies of bioinformatics will contribute greatly to this effort. Developing and implementing code for large-scale systems has many problems. Most of the submodules are complex, requiring consideration of spatial and temporal events and processes. Submodules have to be linked to one another in a way that preserves mass balance and gives an accurate representation of variables in nonlinear complex biochemical networks with many signaling and controlling pathways. Microcompartmentalization vitiates the use of simplified model structures. The stiffness of the systems of equations is computationally costly. Faster computation is needed when using models as thinking tools and for iterative data analysis. Perhaps the most serious problem is the current lack of definitive information on kinetics and dynamics of systems, due in part to the almost total lack of databased observations, but also because, though we are nearly drowning in new information being published each day, either the information required for the modeling cannot be found or has never been obtained. “Simple” things like tissue composition, material properties, and mechanical behavior of cells and tissues are not generally available. The development of comprehensive models of biological systems is a key to pharmaceutics and drug design, for the models will become gradually better predictors of the results of interventions, both genomic and pharmaceutic. Good models will be useful in predicting the side effects and long term effects of drugs and toxins, and when the models are really good, to predict where genomic intervention will be effective and where the multiple redundancies in our biological systems will render a proposed intervention useless. The Physiome Project will provide the integrating scientific basis for the Genes to Health initiative, and make physiological genomics a reality applicable to whole organisms, from bacteria to man. © 2000 Biomedical Engineering Society.
PAC00: 8710+e
This is a preview of subscription content, log in via an institution to check access.
Similar content being viewed by others
References
Bassingthwaighte, J. B., and H. Reuter. Calcium movements and excitation-contraction coupling in cardiac cells. In: Elec-trical Phenomena in the Heart, edited by W. C. DeMello. New York: Academic, 1972, pp. 353-395.
Bassingthwaighte, J. B., R. B. King, and S. A. Roger. Fractal nature of regional myocardial blood flow heterogeneity. Circ. Res. 65:578-590, 1989.
Bassingthwaighte, J. B., C. Y. Wang, and I. S. Chan. Blood-tissue exchange via transport and transformation by endothe-lial cells. Circ. Res. 65:997-1020, 1989.
Bassingthwaighte, J. B., L. S. Liebovitch, and B. J. West. Fractal Physiology. New York: Oxford University Press, 1994, p. 364.
Bassingthwaighte, J. B. and D. A. Beard. Fractal 15 O-water washout from the heart. Circ. Res. 77:1212-1221, 1995.
Bassingthwaighte, J. B., C. A. Goresky, and J. H. Linehan, Editors. Whole Organ Approaches to Cellular Metabolism. 1057 Strategies for the Physiome Project.Capillary Permeation, Cellular Uptake and Product Forma-tion. New York: Springer, 1998, p. 575.
Beadle, G. W. and E. L. Tatum. Genetic control of biochemi-cal reactions in Neurospora. Proc. Natl. Acad. Sci. U.S.A. 27:499-506, 1941.
Beard, D. and J. B. Bassingthwaighte. Advection and diffu-sion of substances in biological tissues with complex vascular networks. Ann. Biomed. Eng. 28:253-268, 2000.
Beard, D. A. and J. B. Bassingthwaighte. Fractal nature of myocardial blood flow described by a whole-organ model of arterial network. J. Vasc. Res. 37:282-296, 2000.
Beeler, Jr., G. W. and H. Reuter. Reconstruction of the action potential of ventricular myocardial fibers. J. Physiol. (Lon-don) 268:177-210, 1977.
Blinks, J. R., R. Rudel, and S. R. Taylor. Calcium transients in isolated amphibian skeletal muscle fibers: detection with aequorin. J. Physiol. (London) 277:291-323, 1978.
Boyd, C. A. R. and D. Noble. The Logic of Life: The Chal-lenge of Integrative Physiology. New York: Oxford Univer-sity Press, 1993, p. 226.
Caldwell, J. H., G. V. Martin, G. M. Raymond, and J. B. Bassingthwaighte. Regional myocardial flow and capillary permeability-surface area products are nearly proportional. Am. J. Phys. 267 ~Heart Circ. Physiol. 36!:H654-H666, 1994.
Ch'en, F. F., R. D. Vaughan-Jones, K. Clarke, and D. Noble. Modeling myocardial ischaemia and reperfusion. Prog. Bio-phys. Mol. Biol. 69:515-538, 1998.
Cowley, Jr., A. W., M. Stoll, A. S. Greene, M. L. Kaldunski, R. J. Roman, P. J. Tonellato, N. J. Schork, P. Dumas, and H. J. Jacob. Genetically defined risk of salt sensitivity in an intercross of Brown Norway and Dahl S rats. Physiological Genomics 2:107-115, 2000.
DiFrancesco, D. and D. Noble. A model of cardiac electrical activity incorporating ionic pumps and concentration changes. Philos. Trans. R. Soc. London, Ser. B 307:353-398, 1985.
Gillis, H.L. and K. R. Lutchen. How heterogeneous broncho-constriction affects ventilation and pressure distributions in human lungs: a morphometric model. Ann. Biomed. Eng. 27:14-22, 1999.
Gillis, H. L. and K. R. Lutchen. Airway remodeling in asthma amplifies the heterogeneous smooth muscle shorten-ing causing hyperresponsiveness. J. Appl. Physiol. 86:2001-2012, 1999.
Glass, L., P. Hunter, and A. McCulloch. Theory of Heart: Biomechanics, Biophysics, and Nonlinear Dynamics of Car-diac Function. New York: Springer, 1991, p. 611.
Guyton, A. C., T. G. Coleman, and H. J. Granger. Circula-tion: overall regulation. Annu. Rev. Physiol. 34:13-46, 1972.
Hodgkin, A. L. and B. Katz. The effect of sodium ions on the electrical activity of the giant axon of the squid. J. Physiol. (London) 108:37-77, 1949.
Hodgkin, A. L. and A. F. Huxley. A quantitative description of membrane current and its application to conduction and excitation in nerve. J. Physiol. (London) 117:500-544, 1952.
Jafri, M. S., J. J. Rice, and R. L. Winslow. Cardiac Ca 21 dynamics: The roles of ryanodine receptor adaptation and sarcoplasmic reticulum load. Biophys. J. 74:1149-1168, 1998.
Jalife, J., J. M. Davidenko, and D. C. Michaels. A new perspective on the mechanisms of arrhythmias and sudden cardiac death: Spiral waves of excitation in heart muscle. J. Cardiovasc. Electrophysiol. 2:S133-S152, 1991.
Kassab, G. S., C. A. Rider, N. J. Tang, and Y. B. Fung. Morphometry of pig coronary arterial trees. Am. J. Physiol. 265 (Heart Circ. Physiol. 34):H350-H365, 1993.
Koshland, Jr., D. E. Switches, thresholds and ultrasensitivity. TIBS 12:225-229, 1987.
Koshland, Jr., D. E. The era of pathway quantification. Sci-ence 280:852-853, 1998.
LeGrice, I. J., B. H. Smaill, L. Z. Chai, S. G. Edgar, J. B. Gavin, and P. J. Hunter. Laminar structure of the heart: Ventricular myocyte arrangement and connective tissue ar-chitecture in the dog. Am. J. Physiol. 269 (Heart Circ. Physiol. 38):H571-H582, 1995.
Luo, C.H. and Y. Rudy. A dynamic model of the cardiac ventricular action potential I. Simulations of ionic currents and concentration changes. Circ. Res. 74:1071-1096, 1994.
Luo, C. H. and Y. Rudy. A dynamic model of the cardiac ventricular action potential: II: Afterdepolarizations, triggered activity, and potentiation. Circ. Res. 74:1097-1113, 1994.
McCulloch, A., J. B. Bassingthwaighte, P. Hunter, and D. Noble. Computational Biology of the Heart: From Structure to Function Progress in Biophysics and Molecular Biology New York: Elsevier, 1998, Vol. 69, pp. 151-572.
Montani, J. P., T. H. Adair, R. L. Summers, T. G. Coleman, and A. C. Guyton. A simulation support system for solving large physiological models on microcomputers. Int. J. Bio-Med. Comput. 24:41-54, 1989.
Noble, D. and R. W. Tsien. Outward membrane currents activated in the plateau range of potentials in cardiac Purkinje fibers. J. Physiol. (London) 200:205-231, 1969.
Platt, J. R.. Strong inference. Science 146:347-353, 1964.
Ringer, S.. A further contribution regarding the influence of the different constituents of the blood on the contraction of the heart. J. Physiol. (London) 4:29-42, 1883.
Schomburg, D., M. Saltzmann, and D. Stephen. Enzyme Handbook. Berlin: Springer, 1990.
Vetter, F. J. and A. D. McCulloch. Three-dimensional analy-sis of regional cardiac function: a model of rabbit ventricular anatomy. Prog. Biophys. Mol. Biol. 69:157-183, 1998.
Vetter, F. J. and A. D. McCulloch. Three-dimensional stress and strain in passive rabbit left ventricle: A model study. Ann. Biomed. Eng. 28:781, 2000.
Weidmann, S.. The electrical constants of Purkinje fibers. J. Physiol. (London) 118:348-360, 1952.
Wilson, E. O. Consilience: The Unity of Knowledge.New York: Alfred A. Knopf, 1998, p. 332.
Winslow, R. L., J. Rice, S. Jafri, E. Marba´n, and B. O'Rourke. Mechanisms of altered excitation-contraction cou-pling in canine tachycardia-induced heart failure, II: Model studies. Circ. Res. 84:571-586, 1999.
Winslow, R. L., D. F. Scollan, A. Holmes, C. K. Yung, J. Zhang, and M. S. Jafri. Electrophysical modeling of cardiac ventricular function: From cell to organ. Ann. Biomed. Eng. 2:119-155, 2000.
Wood, E. H., R. L. Heppner, and S. Weidmann. Inotropic effects of electric currents. I. Positive and negative effects of constant electric currents or current pulses applied during cardiac action or potentials. II. Hypotheses: calcium move-ments, excitation-contraction coupling and inotropic effects. Circ. Res. 24:409-445, 1969.
Zamir, M. and H. Chee. Segment analysis of human coronaryarteries. Blood 24:76-84, 1987.
Author information
Authors and Affiliations
Rights and permissions
About this article
Cite this article
Bassingthwaighte, J.B. Strategies for the Physiome Project. Annals of Biomedical Engineering 28, 1043–1058 (2000). https://doi.org/10.1114/1.1313771
Issue Date:
DOI: https://doi.org/10.1114/1.1313771