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DOI: 10.3414/ME12-01-0076
A Negative Feedback Model for a Mechanism Based Description of Longitudinal Observations
Application for Bone Turnover BiomarkersPublication History
received:
16 August 2012
accepted:
29 April 2013
Publication Date:
20 January 2018 (online)
Summary
In modern medicine the diagnosis and prognosis of an abnormal metabolic condition is based on blood borne measurements involving one or more biomarker.
Objective: This paper reports the development of a minimal negative feedback model for the description of longitudinal biomarkers concentrations for treatment of osteoporosis in postmenopausal women.
Methods: Literature data were obtained from double-blind, placebo-controlled clinical trial over three years. There were four treatment groups: 1) Placebo, 2) Alendro -nate, 3) Conjugated Estrogen, and/or 4) Combination therapy. The negative feedback model consists of a biomarker and a companion controller. By considering the above basal biomarker values it is shown that the dynamics can be described by a second order differential equation without the involvement of biomarker production rate. The second order differential equation is also analogous to classical negative feedback servomechanism model with two parameters ωn and ξ. It was assumed that the rate constants defining the negative feedback model were equal which would set ξ to 0.707 with only ωn to be estimated.
Results: ωn was estimated for both lumbar spine bone mineral density (BMD) and bone-specific alkaline phosphatase (BAP) in four treatments groups. The t½ of BMD and BAP were estimated at 26.8 (0.30) and 9.4 (0.30) days respectively.
Conclusions: The negative feedback model of BMD supports the mechanism whereby Conjugated Estrogen and Alendronate decrease the clearance rate constant of BMD analogous to increased apoptosis of osteoclasts. The linked negative feedback models facilitate a mechanism based prediction of BMD using the concentrations of the bone turnover marker BAP.
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References
- 1 Colledge NR, Walker BR, Ralston SH. Davidson’s Principles and Practice of Medicine. Churchill Livingstone 2010.
- 2 Schmidt S, Post TM, Boroujerdi MA, van Kesteren S, Ploeger BA, Della Pasqua OE. et al. In: Kimko HC, Peck CC. (eds). Clinical trial simulations. 1st edn.. New York: Springer; 2010: 437-459.
- 3 Umpleby AM, Boroujerdi MA, Brown PM, Carson ER, Sonksen PH. The effect of metabolic control on leucine metabolism in type 1 (insulin-dependent) diabetic patients. Diabetologia 1986; 29: 131-141.
- 4 Danhof M, Alvan G, Dahl SG, Kuhlmann J, Paintaud G. Mechanism-based pharmacokinetic-pharmacodynamic modeling - a new classification of biomarkers. Pharm Res 2005; 22: 1432-1437.
- 5 Cobelli C, Man CD, Sparacino G, Magni L, De Nicolao G, Kovatchev BP. Diabetes: Models, Signals, and Control. IEEE Rev Biomed Eng 2009; 2: 54-96.
- 6 Veldhuis JD, Johnson ML. A Review and Appraisal of Deconvolution Methods to Evaluate in vivo Neuroendocrine Secretory Events. J Neuroendocrinol 1990; 2: 755-771.
- 7 Cnaan A, Laird NM, Slasor P. Using the general linear mixed model to analyse unbalanced repeated measures and longitudinal data. Stat Med 1997; 16: 2349-2380.
- 8 De Stavola BL, Nitsch D, dos Santos Silva I, McCormack V, Hardy R, Mann V. et al. Statistical issues in life course epidemiology. Am J Epidemiol 2006; 163: 84-96.
- 9 Komarova SV, Smith RJ, Dixon SJ, Sims SM, Wahl LM. Mathematical model predicts a critical role for osteoclast autocrine regulation in the control of bone remodeling. Bone 2003; 33 (02) 206-215.
- 10 Frost HM. Bone’s mechanostat: a 2003 update. Anat Rec A Discov Mol Cell Evol Biol 2003; 275 (02) 1081-1101.
- 11 Pivonka P, Zimak J, Smith DW, Gardiner BS, Dunstan CR, Sims NA. et al. Theoretical investigation of the role of the RANK-RANKL-OPG system in bone remodeling. J Theor Biol 2005; 262: 306-316.
- 12 Lemaire V, Tobin FL, Greller LD, Cho CR, Suva LJ. Modeling the interactions between osteoblast and osteoclast activities in bone remodeling. J Theor Biol 2004; 229: 293-309.
- 13 Pivonka P, Komarova SV. Mathematical modeling in bone biology: from intracellular signaling to tissue mechanics. Bone 2010; 47: 181-189.
- 14 Greenspan SL, Emkey RD, Bone HG, Weiss SR, Bell NH, Downs RW. et al. Significant differential effects of alendronate, estrogen, or combination therapy on the rate of bone loss after discontinuation of treatment of postmenopausal osteoporosis. A randomized, double-blind, placebo-controlled trial. Ann Intern Med 2002; 137: 875-883.
- 15 Visvanathan M, Breit M, Pfeifer B, Baumgartner C, Modre-Osprian R, Tilg B. DMSP - Database for Modeling Signaling Pathways. Combining biological and mathematical modeling knowledge for pathways. Methods Inf Med 2008; 47 (02) 140-148.
- 16 Ackerman E, Rosevear JW, McGuckin WF. A Mathematical Model of the Glucose-tolerance test. Phys Med Biol 1964; 9: 203-213.
- 17 Healey M. Principles of Automatic Control. London: Hodder and Stoughton; 1967.
- 18 R: A Language and Environment for Statistical Computing (computer program) 2011.
- 19 Dennis JE. Numerical Methods for Unconstrained Optimization and Nonlinear Equations. Englewood Cliffs, NJ: Prentice-Hall; 1983.
- 20 Soeraert K, Petzoldt T, Setzer W. Solving Differential Equations in R: Package deSolve. Journal of Statistical Software 2010; 33: 1-25.
- 21 Parfitt AM, Mundy GR, Roodman GD, Hughes DE, Boyce BF. A new model for the regulation of bone resorption, with particular reference to the effects of bisphosphonates. J Bone Miner Res 1996; 11: 150-159.
- 22 Posen S, Grunstein HS. Turnover rate of skeletal alkaline phosphatase in humans. Clin Chem 1982; 28: 153-154.
- 23 Luckman SP, Coxon FP, Ebetino FH, Russell RG, Rogers MJ. Heterocycle-containing bisphosphonates cause apoptosis and inhibit bone resorption by preventing protein prenylation: evidence from structure-activity relationships in J774 macrophages. J Bone Miner Res 1998; 13: 1668-1678.
- 24 Marincola FM. Translational Medicine: A two-way road. J Transl Med 2003; 1 (01) 1
- 25 Kulikowski CA, Kulikowski CW. Biomedical and health informatics in translational medicine. Methods Inf Med 2009; 48 (01) 4-10.