I.V. Bolus administration of subconvulsive doses of lignocaine to conscious sheep: Myocardial pharmacokinetics

Y. F. Huang; R. N. Upton; W. B. Runciman

doi:10.1093/bja/70.3.326

I.V. Bolus administration of subconvulsive doses of lignocaine to conscious sheep: Myocardial pharmacokinetics

Y. F. Huang, R. N. Upton, W. B. Runciman

Research output: Contribution to journal › Article › peer-review

21 Citations (Scopus)

Abstract

Mass balance principles were used to study the myocardial pharmacokinetics of lignocaine in conscious sheep. After i.v.bolus doses of lignocaine 50, 75 or 100 mg, arterial lignocaine concentrations reached a peak in approximately 16 s and these increased linearly with dose. Coronary sinus concentrations reached a peak between 83 and 129 s and the values showed poor relationships with dose. Net myocardial lignocaine uptake lasted for approximately 60s7-this was much shorter than the reported initial distribution half-life of lignocaine. The maximum rate of uptake was proportional to both the dose and the peak arterial lignocaine concentrations. At 15 min, the myocardial lignocaine concentrations were 46 (SD 22) % of their peak values. Pseudo-equilibrium between blood and myocardial lignocaine concentrations was not observed. It is concluded that, despite the myocardium being very well perfused, lignocaine myocardial concentrations were not well represented by blood lignocaine concentrations for at least 15 min. A greater understanding of the determinants of myocardial drug concentrations is required. (Br. J. Anaesth. 1993; 70: 326-332).

Original language	English
Pages (from-to)	326-332
Number of pages	7
Journal	British Journal of Anaesthesia
Volume	70
Issue number	3
DOIs	https://doi.org/10.1093/bja/70.3.326
Publication status	Published or Issued - Mar 1993
Externally published	Yes

Keywords

Anaesthetics, local: lignocaine Heart drug uptake
Pharmacokinetics

ASJC Scopus subject areas

Anesthesiology and Pain Medicine

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10.1093/bja/70.3.326

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title = "I.V. Bolus administration of subconvulsive doses of lignocaine to conscious sheep: Myocardial pharmacokinetics",

abstract = "Mass balance principles were used to study the myocardial pharmacokinetics of lignocaine in conscious sheep. After i.v.bolus doses of lignocaine 50, 75 or 100 mg, arterial lignocaine concentrations reached a peak in approximately 16 s and these increased linearly with dose. Coronary sinus concentrations reached a peak between 83 and 129 s and the values showed poor relationships with dose. Net myocardial lignocaine uptake lasted for approximately 60s7-this was much shorter than the reported initial distribution half-life of lignocaine. The maximum rate of uptake was proportional to both the dose and the peak arterial lignocaine concentrations. At 15 min, the myocardial lignocaine concentrations were 46 (SD 22) \% of their peak values. Pseudo-equilibrium between blood and myocardial lignocaine concentrations was not observed. It is concluded that, despite the myocardium being very well perfused, lignocaine myocardial concentrations were not well represented by blood lignocaine concentrations for at least 15 min. A greater understanding of the determinants of myocardial drug concentrations is required. (Br. J. Anaesth. 1993; 70: 326-332).",

keywords = "Anaesthetics, local: lignocaine Heart drug uptake, Pharmacokinetics",

author = "Huang, \{Y. F.\} and Upton, \{R. N.\} and Runciman, \{W. B.\}",

note = "Funding Information: This study was supported by a grant from the National Heart Foundation of Australia. The authors thank Professor L. E. Mather for providing research facilities in the Department of Anaesthesia and Intensive Care of Flinders Medical Centre while those at the University of Adelaide were being refurbished, and thank Dr J. P. Plummer for statistical advice. Technical help from Mr K. Smart, Ms E. Henning and Ms C. Adcock was greatly appreciated.",

year = "1993",

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doi = "10.1093/bja/70.3.326",

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TY - JOUR

T1 - I.V. Bolus administration of subconvulsive doses of lignocaine to conscious sheep

T2 - Myocardial pharmacokinetics

AU - Huang, Y. F.

AU - Upton, R. N.

AU - Runciman, W. B.

N1 - Funding Information: This study was supported by a grant from the National Heart Foundation of Australia. The authors thank Professor L. E. Mather for providing research facilities in the Department of Anaesthesia and Intensive Care of Flinders Medical Centre while those at the University of Adelaide were being refurbished, and thank Dr J. P. Plummer for statistical advice. Technical help from Mr K. Smart, Ms E. Henning and Ms C. Adcock was greatly appreciated.

PY - 1993/3

Y1 - 1993/3

N2 - Mass balance principles were used to study the myocardial pharmacokinetics of lignocaine in conscious sheep. After i.v.bolus doses of lignocaine 50, 75 or 100 mg, arterial lignocaine concentrations reached a peak in approximately 16 s and these increased linearly with dose. Coronary sinus concentrations reached a peak between 83 and 129 s and the values showed poor relationships with dose. Net myocardial lignocaine uptake lasted for approximately 60s7-this was much shorter than the reported initial distribution half-life of lignocaine. The maximum rate of uptake was proportional to both the dose and the peak arterial lignocaine concentrations. At 15 min, the myocardial lignocaine concentrations were 46 (SD 22) % of their peak values. Pseudo-equilibrium between blood and myocardial lignocaine concentrations was not observed. It is concluded that, despite the myocardium being very well perfused, lignocaine myocardial concentrations were not well represented by blood lignocaine concentrations for at least 15 min. A greater understanding of the determinants of myocardial drug concentrations is required. (Br. J. Anaesth. 1993; 70: 326-332).

AB - Mass balance principles were used to study the myocardial pharmacokinetics of lignocaine in conscious sheep. After i.v.bolus doses of lignocaine 50, 75 or 100 mg, arterial lignocaine concentrations reached a peak in approximately 16 s and these increased linearly with dose. Coronary sinus concentrations reached a peak between 83 and 129 s and the values showed poor relationships with dose. Net myocardial lignocaine uptake lasted for approximately 60s7-this was much shorter than the reported initial distribution half-life of lignocaine. The maximum rate of uptake was proportional to both the dose and the peak arterial lignocaine concentrations. At 15 min, the myocardial lignocaine concentrations were 46 (SD 22) % of their peak values. Pseudo-equilibrium between blood and myocardial lignocaine concentrations was not observed. It is concluded that, despite the myocardium being very well perfused, lignocaine myocardial concentrations were not well represented by blood lignocaine concentrations for at least 15 min. A greater understanding of the determinants of myocardial drug concentrations is required. (Br. J. Anaesth. 1993; 70: 326-332).

KW - Anaesthetics, local: lignocaine Heart drug uptake

KW - Pharmacokinetics

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ER -

I.V. Bolus administration of subconvulsive doses of lignocaine to conscious sheep: Myocardial pharmacokinetics

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Keywords

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