Pharmakokinetische/pharmakodynamische Modelle für Inhalationsanästhetika

Kreuer, Sascha; Bruhn, Jørgen; Wilhelm, Wolfram; Bouillon, Thomas

doi:10.1007/s00101-007-1188-7

Cited by 17 publications

(6 citation statements)

References 120 publications

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“…Multiple studies have shown higher ke0 values for desflurane than for sevoflurane and isoflurane. 42,43 This means that an increase or decrease in Etaa using desflurane will result in a more rapid change in the depth of anesthesia. Bispectral index measurements and ke0 values derived from pharmacokinetic modelling do not provide a full appreciation of inhalational agent equilibration.…”

Section: Alveolar Ventilationmentioning

confidence: 99%

Brief review: Theory and practice of minimal fresh gas flow anesthesia

Brattwall

Warrén-Stomberg

Hesselvik

et al. 2012

Can J Anesth/J Can Anesth

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Section: Alveolar Ventilationmentioning

confidence: 99%

Brief review: Theory and practice of minimal fresh gas flow anesthesia

Brattwall

Warrén-Stomberg

Hesselvik

et al. 2012

Can J Anesth/J Can Anesth

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“…Untuk mengatasi hal tersebut, aliran gas segar (oksigen) harus dapat mencukupi kebutuhan oksigen basal, tidak ada kebocoran pada sirkuit anestesi, dan alat penyerap CO 2 harus berfungsi baik agar konsentrasi CO 2 dalam udara inspirasi tidak melebihi nilai ambang yang diperkenankan sebesar 0,2%. 9 Teknik low flow anesthesia pada penelitian ini mengikuti guideline yang diberikan oleh Foldes 10 atau Virtue, 11 yaitu pada fase awal selama 10-15 menit digunakan FGF yang tinggi. Foldes 10 telah merekomendasikan pengaturan oksigen 2 L/menit dan N 2 O 3 L/menit selama 10 menit untuk menjamin denitrogenisasi yang adekuat.…”

Section: Pembahasanunclassified

“…Terakhir, jika flow diturunkan terlalu cepat ke nilai yang sangat rendah, defisiensi volume gas tidak dapat dihindarkan sehingga dapat mengakibatkan ventilasi yang tidak adekuat. 1,9 Sistem rebreathing dapat dipergunakan dengan cara yang berbeda dan jika digunakan FGF yang sama dengan minute volume pasien maka peran rebreathing akan sia-sia. Hampir sepenuhnya udara yang diekspirasikan akan dilepaskan keluar sistem sebagai kelebihan gas melalui katup APL.…”

Section: Pembahasanunclassified

Perbandingan Nilai SpO2 dan EtCO2 pada Anestesi Umum dengan Teknik Low Flow dan High Flow

Arifin¹,

Andri²

2016

jap

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“…The higher the blood/gas partition coefficient, the more soluble is the anaesthetic in blood compared to air and the more it binds to lipids and proteins in the blood. If an anaesthetic has a high Ostwald coefficient, then a large amount of it will have to be taken up in the body's blood before being passed on to the fatty (lipid) tissues of the brain where it can exert its effect10.…”

mentioning

confidence: 99%

“…The blood/gas partition coefficient is widely used for the PK description of volatile anaesthetics10. However, for PK modelling the coefficient could only be used if the partial pressure in both compartments is at equilibrium.…”

mentioning

confidence: 99%

Two different approaches for pharmacokinetic modeling of exhaled drug concentrations

Kreuer

Hauschild

Fink

et al. 2014

Sci Rep

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Online measurement of drug concentrations in patient's breath is a promising approach for individualized dosage. A direct transfer from breath- to blood-concentrations is not possible. Measured exhaled concentrations are following the blood-concentration with a delay in non-steady-state situations. Therefore, it is necessary to integrate the breath-concentration into a pharmacological model. Two different approaches for pharmacokinetic modelling are presented. Usually a 3-compartment model is used for pharmacokinetic calculations of blood concentrations. This 3-compartment model is extended with a 2-compartment model based on the first compartment of the 3-compartment model and a new lung compartment. The second approach is to calculate a time delay of changes in the concentration of the first compartment to describe the lung-concentration. Exemplarily both approaches are used for modelling of exhaled propofol. Based on time series of exhaled propofol measurements using an ion-mobility-spectrometer every minute for 346 min a correlation of calculated plasma and the breath concentration was used for modelling to deliver R2 = 0.99 interdependencies. Including the time delay modelling approach the new compartment coefficient ke0lung was calculated to ke0lung = 0.27 min−1 with R2 = 0.96. The described models are not limited to propofol. They could be used for any kind of drugs, which are measurable in patient's breath.

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Pharmakokinetische/pharmakodynamische Modelle für Inhalationsanästhetika

Cited by 17 publications

References 120 publications

Brief review: Theory and practice of minimal fresh gas flow anesthesia

Brief review: Theory and practice of minimal fresh gas flow anesthesia

Perbandingan Nilai SpO2 dan EtCO2 pada Anestesi Umum dengan Teknik Low Flow dan High Flow

Two different approaches for pharmacokinetic modeling of exhaled drug concentrations

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