Literature DB >> 2614681

The unit impulse response procedure for the pharmacokinetic evaluation of drug entry into the central nervous system.

J B van Bree1, A V Baljet, A van Geyt, A G de Boer, M Danhof, D D Breimer.   

Abstract

The unit impulse response theory has been adapted to characterize the transport profile of drugs into the central nervous system (CNS). From the obtained input function, the cumulative plasma volume (V) cleared by transport into the CNS in time can be calculated. Simulation studies demonstrated that transport governed by passive diffusion resulted in a linear relationship between V and time, while the slope of the line, the blood-brain barrier (BBB) clearance, proved to be an adequate and model independent parameter to characterize drug transport into the CNS. The error in the result of the numerical procedure could be limited to less than 10% of the theoretically predicted value. Superposition of 5 or 10% random noise on simulated data did not result in significant differences between the calculated and theoretically predicted clearance values. Simulations of carrier-mediated transport resulted in nonlinear transport curves; the degree of nonlinearity, and thus the detectability, was dependent on the initial degree of saturation of the system, the rate of desaturation, as caused by drug elimination processes and the noise level on the data. In vivo experiments in the rat were performed, using atenolol, acetaminophen, and antipyrine as model drugs. Linear transport relationships were obtained for all drugs, indicating that transport was dependent on passive diffusion or a low affinity carrier system. BBB-clearance values were 7 +/- 1 microliters/min for atenolol, 63 +/- 7 microliters/min for acetaminophen and 316 +/- 25 microliters/min for antipyrine. These experiments validate the applicability of the presented technique in in vivo studies.

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Year:  1989        PMID: 2614681     DOI: 10.1007/bf01061457

Source DB:  PubMed          Journal:  J Pharmacokinet Biopharm        ISSN: 0090-466X


  24 in total

1.  The importance of dissociaton constant and lipid-solubility in influencing the passage of drugs into the cerebrospinal fluid.

Authors:  B B BRODIE; H KURZ; L S SCHANKER
Journal:  J Pharmacol Exp Ther       Date:  1960-09       Impact factor: 4.030

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Journal:  J Physiol       Date:  1976-02       Impact factor: 5.182

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Authors:  E Preston; N Haas
Journal:  J Neurosci Res       Date:  1986       Impact factor: 4.164

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Authors:  T W Latson; W C Hunter; D Burkhoff; K Sagawa
Journal:  Am J Physiol       Date:  1986-12

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Authors:  E A Bering
Journal:  Fed Proc       Date:  1974-09

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Authors:  W H Oldendorf
Journal:  Proc Soc Exp Biol Med       Date:  1974-12

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Authors:  W H Oldendorf
Journal:  Brain Res       Date:  1970-12-01       Impact factor: 3.252

8.  Blood-brain barrier: endogenous modulation by adrenal-cortical function.

Authors:  J B Long; J W Holaday
Journal:  Science       Date:  1985-03-29       Impact factor: 47.728

9.  Distributed model for drug delivery to CSF and brain tissue.

Authors:  J M Collins; R L Dedrick
Journal:  Am J Physiol       Date:  1983-09

10.  Carotid artery injection technique: bounds for bolus mixing by plasma and by brain.

Authors:  W M Pardridge; E M Landaw; L P Miller; L D Braun; W H Oldendorf
Journal:  J Cereb Blood Flow Metab       Date:  1985-12       Impact factor: 6.200

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  14 in total

Review 1.  Drug transport across the blood-brain barrier. II. Experimental techniques to study drug transport.

Authors:  J B Van Bree; A G De Boer; M Danhof; D D Breimer
Journal:  Pharm Weekbl Sci       Date:  1992-12-11

2.  Estimation of amobarbital plasma-effect site equilibration kinetics. Relevance of polyexponential conductance functions.

Authors:  J W Mandema; P Veng-Pedersen; M Danhof
Journal:  J Pharmacokinet Biopharm       Date:  1991-12

Review 3.  Delivering peptides to the central nervous system: dilemmas and strategies.

Authors:  W A Banks; A J Kastin; C M Barrera
Journal:  Pharm Res       Date:  1991-11       Impact factor: 4.200

4.  Transport of desglycinamide-arginine vasopressin across the blood-brain barrier in rats as evaluated by the unit impulse response methodology.

Authors:  J B van Bree; S Tio; A G de Boer; M Danhof; J C Verhoef; D D Breimer
Journal:  Pharm Res       Date:  1990-03       Impact factor: 4.200

5.  The use of microdialysis for the study of drug kinetics: some methodological considerations illustrated with antipyrine in rat frontal cortex.

Authors:  P N Patsalos; W T Abed; M S Alavijeh; M T O'Connell
Journal:  Br J Pharmacol       Date:  1995-06       Impact factor: 8.739

6.  In vitro and in vivo transport of zidovudine (AZT) across the blood-brain barrier and the effect of transport inhibitors.

Authors:  R Masereeuw; U Jaehde; M W Langemeijer; A G de Boer; D D Breimer
Journal:  Pharm Res       Date:  1994-02       Impact factor: 4.200

7.  Application of intracerebral microdialysis to study regional distribution kinetics of drugs in rat brain.

Authors:  E C de Lange; M R Bouw; J W Mandema; M Danhof; A G de Boer; D D Breimer
Journal:  Br J Pharmacol       Date:  1995-11       Impact factor: 8.739

8.  The use of intracerebral microdialysis to determine changes in blood-brain barrier transport characteristics.

Authors:  E C de Lange; M B Hesselink; M Danhof; A G de Boer; D D Breimer
Journal:  Pharm Res       Date:  1995-01       Impact factor: 4.200

9.  Paracetamol plasma and cerebrospinal fluid pharmacokinetics in children.

Authors:  B J Anderson; N H Holford; G A Woollard; P L Chan
Journal:  Br J Clin Pharmacol       Date:  1998-09       Impact factor: 4.335

Review 10.  Physiologically based pharmacokinetic modeling to investigate regional brain distribution kinetics in rats.

Authors:  Joost Westerhout; Bart Ploeger; Jean Smeets; Meindert Danhof; Elizabeth C M de Lange
Journal:  AAPS J       Date:  2012-05-17       Impact factor: 4.009

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