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PK/PD model

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Goutelle, S.; Maurin, M.; Rougier, F.; Barbaut, X.; Bourguignon, L.; Ducher, M.; Maire, P. (2008). "The Hill equation: A review of its capabilities in pharmacological modelling".
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Aarons, L.; Karlsson, M. O.; Mentré, F.; Rombout, F.; Steimer, J. L.; van Peer, A.; COST B15 Experts (May 2001). "Role of modelling and simulation in Phase I drug development".
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Hahn, J. O.; Khosravi, S.; Dumont, G. A.; Ansermino, J. M. (2011). "Two-stage vs mixed-effect approach to pharmacodynamic modeling of propofol in children using state entropy".
69:. However, if a delay is observed between the drug administration and the drug effect, a temporal dissociation needs to be taken into account and more complex models exist: 324:
Pharmaceutical Biotechnology: Fundamentals and Applications. Crommelin, Daan; Meibohm, Bernd; Sindelar, Robert. Third Edition. Informa Healthcare USA. 2008.
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Central to PK/PD models is the concentration-effect or exposure-response relationship. A variety of PK/PD modeling approaches exist to describe
243:"Basic Concepts in Population Modeling, Simulation, and Model-Based Drug Development: Part 3-Introduction to Pharmacodynamic Modeling Methods" 526:
Karlsson, Mats O.; Anehall, Therese; Friberg, Lena E.; Henningsson, Anja; Kloft, Charlotte; Sandström, Marie; Xie, Rujia (2005-03-01).
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Derendorf, H.; Meibohm, B. (1999). "Modeling of pharmacokinetic/pharmacodynamic (PK/PD) relationships: Concepts and perspectives".
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PK/PD modeling has its importance at each step of the drug development and it has shown its usefulness in many diseases. The
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Mager, Donald E.; Wyska, Elzbieta; Jusko, William J. (2003-05-01). "Diversity of Mechanism-Based Pharmacodynamic Models".
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Meibohm, B.; Derendorf, H. (October 1997). "Basic concepts of pharmacokinetic/pharmacodynamic (PK/PD) modelling".
62: 93: 66: 17: 675: 34:) (alternatively abbreviated as PKPD or PK-PD modeling) is a technique that combines the two classical 50:
that allows the description of the time course of effect intensity in response to administration of a
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also provides guidances for Industry to recommend how exposure-response studies should be performed.
47: 65:. PK/PD relationships can be described by simple equations such as linear model, Emax model or 471: 577:"Exposure-Response Relationships — Study Design, Data Analysis, and Regulatory Applications" 632: 491:
Rajman, Iris (2008-04-01). "PK/PD modelling and simulations: utility in drug development".
8: 544: 527: 46:. It integrates a pharmacokinetic and a pharmacodynamic model component into one set of 411: 378: 267: 242: 223: 180: 137: 447: 620: 557: 549: 508: 459: 451: 416: 398: 359: 351: 307: 299: 272: 215: 172: 168: 129: 125: 227: 141: 539: 500: 443: 406: 390: 343: 262: 254: 207: 184: 164: 121: 85: 43: 39: 504: 55: 616: 211: 659: 553: 455: 402: 355: 303: 612: 561: 528:"Pharmacokinetic/Pharmacodynamic Modelling in Oncological Drug Development" 512: 463: 363: 276: 219: 176: 133: 35: 420: 311: 347: 258: 394: 379:"Comparison of Four Basic Models of Indirect Pharmacodynamic Responses" 377:
Dayneka, Natalie L.; Garg, Varun; Jusko, William J. (August 1993).
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International Journal of Clinical Pharmacology and Therapeutics
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Index

PK/PD models
pharmacologic
pharmacokinetics
pharmacodynamics
mathematical expressions
drug
pharmacometrics
exposure-response relationships
sigmoid Emax model
Complex response
Food and Drug Administration
doi
10.1111/j.1460-9592.2011.03584.x
PMID
21518104
S2CID
23414752
doi
10.1111/j.1472-8206.2008.00633.x
PMID
19049668
S2CID
4979109
doi
10.1023/A:1011907920641
PMID
10100300
S2CID
23165736
"Basic Concepts in Population Modeling, Simulation, and Model-Based Drug Development: Part 3-Introduction to Pharmacodynamic Modeling Methods"

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