Concentrations of vatinoxan and xylazine in plasma, cerebrospinal fluid and brain tissue following intravenous administration in sheep

Magdy Adam; Jere Linden; Marja Raekallio; Ahmed Abu-Shahba; Bettina Mannerström; Riitta Seppänen-Kaijansinkko; Anna Meller; Kati Salla

doi:10.1016/j.vaa.2021.08.003

Concentrations of vatinoxan and xylazine in plasma, cerebrospinal fluid and brain tissue following intravenous administration in sheep

Magdy Adam, Jere Linden, Marja Raekallio, Ahmed Abu-Shahba, Bettina Mannerström, Riitta Seppänen-Kaijansinkko, Anna Meller, Kati Salla

Forskningsoutput: Tidskriftsbidrag › Artikel › Vetenskaplig › Peer review

Sammanfattning

Objectives To investigate the extent of vatinoxan distribution into sheep brain, and whether vatinoxan influences brain concentrations of xylazine; and to examine the utility of cerebrospinal fluid (CSF) as a surrogate of brain tissue concentrations for vatinoxan and xylazine.

Study design Randomised, blinded, experimental study.

Animals A total of 14 adult female sheep.

Methods Sheep were randomly allocated into two equal groups and premeditated with either intravenous (IV) vatinoxan (750 mu g kg(-1), VX) or saline (SX) administered 10 minutes before IV xylazine (500 mu g kg(-1)). Sedation was subjectively assessed at selected intervals before and after treatments. At 10 minutes after xylazine administration, a venous blood sample was collected and the sheep were immediately euthanised with IV pentobarbital (100 mg kg(-1)). Plasma, CSF and brain tissues were harvested, and concentrations of vatinoxan and xylazine were quantified using liquid chromatography-tandem mass spectrometry. Drug ratios were then calculated and the data were analysed as appropriate.

Results The brain-to-plasma and CSF-to-plasma ratios of vatinoxan were 0.06 +/- 0.013 and 0.05 +/- 0.01 (mean +/- standard deviation), respectively. Xylazine brain concentrations were not significantly different (835 +/- 262 versus 1029 +/- 297 ng g(-1) in groups VX and SX, respectively) and were approximately 15-fold higher than those in plasma. The CSF-to-brain ratio of vatinoxan was 0.8 +/- 0.2, whereas xylazine concentrations in the brain were approximately 17-fold greater than those in CSF, with and without vatinoxan.

Conclusions and clinical relevance Vatinoxan did not significantly affect sedation with xylazine or the concentrations of xylazine in the brain. CSF is not a good predictor of xylazine concentrations in the brain, whereas vatinoxan concentrations were concordant between the brain and CSF, using the dosages in this study.

Originalspråk	engelska
Tidskrift	Veterinary Anaesthesia and Analgesia
Volym	48
Nummer	6
Sidor (från-till)	900-905
Antal sidor	6
ISSN	1467-2987
DOI	https://doi.org/10.1016/j.vaa.2021.08.003
Status	Publicerad - nov. 2021
MoE-publikationstyp	A1 Tidskriftsartikel-refererad

Vetenskapsgrenar

413 Veterinärvetenskap

Åtkomst av dokument

10.1016/j.vaa.2021.08.003

PIIS146729872100204XSlutlig publicerad version, 312 KBLicens: CC BY

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@article{766293f1e90245ed96b39f29d34f2340,

title = "Concentrations of vatinoxan and xylazine in plasma, cerebrospinal fluid and brain tissue following intravenous administration in sheep",

abstract = "Objectives To investigate the extent of vatinoxan distribution into sheep brain, and whether vatinoxan influences brain concentrations of xylazine; and to examine the utility of cerebrospinal fluid (CSF) as a surrogate of brain tissue concentrations for vatinoxan and xylazine.Study design Randomised, blinded, experimental study.Animals A total of 14 adult female sheep.Methods Sheep were randomly allocated into two equal groups and premeditated with either intravenous (IV) vatinoxan (750 mu g kg(-1), VX) or saline (SX) administered 10 minutes before IV xylazine (500 mu g kg(-1)). Sedation was subjectively assessed at selected intervals before and after treatments. At 10 minutes after xylazine administration, a venous blood sample was collected and the sheep were immediately euthanised with IV pentobarbital (100 mg kg(-1)). Plasma, CSF and brain tissues were harvested, and concentrations of vatinoxan and xylazine were quantified using liquid chromatography-tandem mass spectrometry. Drug ratios were then calculated and the data were analysed as appropriate.Results The brain-to-plasma and CSF-to-plasma ratios of vatinoxan were 0.06 +/- 0.013 and 0.05 +/- 0.01 (mean +/- standard deviation), respectively. Xylazine brain concentrations were not significantly different (835 +/- 262 versus 1029 +/- 297 ng g(-1) in groups VX and SX, respectively) and were approximately 15-fold higher than those in plasma. The CSF-to-brain ratio of vatinoxan was 0.8 +/- 0.2, whereas xylazine concentrations in the brain were approximately 17-fold greater than those in CSF, with and without vatinoxan.Conclusions and clinical relevance Vatinoxan did not significantly affect sedation with xylazine or the concentrations of xylazine in the brain. CSF is not a good predictor of xylazine concentrations in the brain, whereas vatinoxan concentrations were concordant between the brain and CSF, using the dosages in this study.",

keywords = "BRADYCARDIA, CSF, DEXMEDETOMIDINE-INDUCED SEDATION, EFFICACY, L-659,066, MEDETOMIDINE, MK-467, PERIPHERAL ALPHA(2)-ADRENOCEPTOR ANTAGONIST, PHARMACOKINETICS, SURROGATE, brain tissue, cerebrospinal fluid, sheep, vatinoxan, xylazine, 413 Veterinary science",

author = "Magdy Adam and Jere Linden and Marja Raekallio and Ahmed Abu-Shahba and Bettina Mannerstr{\"o}m and Riitta Sepp{\"a}nen-Kaijansinkko and Anna Meller and Kati Salla",

year = "2021",

month = nov,

doi = "10.1016/j.vaa.2021.08.003",

language = "English",

volume = "48",

pages = "900--905",

journal = "Veterinary Anaesthesia and Analgesia",

issn = "1467-2987",

publisher = "Elsevier Scientific Publ. Co",

number = "6",

}

TY - JOUR

T1 - Concentrations of vatinoxan and xylazine in plasma, cerebrospinal fluid and brain tissue following intravenous administration in sheep

AU - Adam, Magdy

AU - Linden, Jere

AU - Raekallio, Marja

AU - Abu-Shahba, Ahmed

AU - Mannerström, Bettina

AU - Seppänen-Kaijansinkko, Riitta

AU - Meller, Anna

AU - Salla, Kati

PY - 2021/11

Y1 - 2021/11

N2 - Objectives To investigate the extent of vatinoxan distribution into sheep brain, and whether vatinoxan influences brain concentrations of xylazine; and to examine the utility of cerebrospinal fluid (CSF) as a surrogate of brain tissue concentrations for vatinoxan and xylazine.Study design Randomised, blinded, experimental study.Animals A total of 14 adult female sheep.Methods Sheep were randomly allocated into two equal groups and premeditated with either intravenous (IV) vatinoxan (750 mu g kg(-1), VX) or saline (SX) administered 10 minutes before IV xylazine (500 mu g kg(-1)). Sedation was subjectively assessed at selected intervals before and after treatments. At 10 minutes after xylazine administration, a venous blood sample was collected and the sheep were immediately euthanised with IV pentobarbital (100 mg kg(-1)). Plasma, CSF and brain tissues were harvested, and concentrations of vatinoxan and xylazine were quantified using liquid chromatography-tandem mass spectrometry. Drug ratios were then calculated and the data were analysed as appropriate.Results The brain-to-plasma and CSF-to-plasma ratios of vatinoxan were 0.06 +/- 0.013 and 0.05 +/- 0.01 (mean +/- standard deviation), respectively. Xylazine brain concentrations were not significantly different (835 +/- 262 versus 1029 +/- 297 ng g(-1) in groups VX and SX, respectively) and were approximately 15-fold higher than those in plasma. The CSF-to-brain ratio of vatinoxan was 0.8 +/- 0.2, whereas xylazine concentrations in the brain were approximately 17-fold greater than those in CSF, with and without vatinoxan.Conclusions and clinical relevance Vatinoxan did not significantly affect sedation with xylazine or the concentrations of xylazine in the brain. CSF is not a good predictor of xylazine concentrations in the brain, whereas vatinoxan concentrations were concordant between the brain and CSF, using the dosages in this study.

AB - Objectives To investigate the extent of vatinoxan distribution into sheep brain, and whether vatinoxan influences brain concentrations of xylazine; and to examine the utility of cerebrospinal fluid (CSF) as a surrogate of brain tissue concentrations for vatinoxan and xylazine.Study design Randomised, blinded, experimental study.Animals A total of 14 adult female sheep.Methods Sheep were randomly allocated into two equal groups and premeditated with either intravenous (IV) vatinoxan (750 mu g kg(-1), VX) or saline (SX) administered 10 minutes before IV xylazine (500 mu g kg(-1)). Sedation was subjectively assessed at selected intervals before and after treatments. At 10 minutes after xylazine administration, a venous blood sample was collected and the sheep were immediately euthanised with IV pentobarbital (100 mg kg(-1)). Plasma, CSF and brain tissues were harvested, and concentrations of vatinoxan and xylazine were quantified using liquid chromatography-tandem mass spectrometry. Drug ratios were then calculated and the data were analysed as appropriate.Results The brain-to-plasma and CSF-to-plasma ratios of vatinoxan were 0.06 +/- 0.013 and 0.05 +/- 0.01 (mean +/- standard deviation), respectively. Xylazine brain concentrations were not significantly different (835 +/- 262 versus 1029 +/- 297 ng g(-1) in groups VX and SX, respectively) and were approximately 15-fold higher than those in plasma. The CSF-to-brain ratio of vatinoxan was 0.8 +/- 0.2, whereas xylazine concentrations in the brain were approximately 17-fold greater than those in CSF, with and without vatinoxan.Conclusions and clinical relevance Vatinoxan did not significantly affect sedation with xylazine or the concentrations of xylazine in the brain. CSF is not a good predictor of xylazine concentrations in the brain, whereas vatinoxan concentrations were concordant between the brain and CSF, using the dosages in this study.

KW - BRADYCARDIA

KW - CSF

KW - DEXMEDETOMIDINE-INDUCED SEDATION

KW - EFFICACY

KW - L-659,066

KW - MEDETOMIDINE

KW - MK-467

KW - PERIPHERAL ALPHA(2)-ADRENOCEPTOR ANTAGONIST

KW - PHARMACOKINETICS

KW - SURROGATE

KW - brain tissue

KW - cerebrospinal fluid

KW - sheep

KW - vatinoxan

KW - xylazine

KW - 413 Veterinary science

U2 - 10.1016/j.vaa.2021.08.003

DO - 10.1016/j.vaa.2021.08.003

M3 - Article

VL - 48

SP - 900

EP - 905

JO - Veterinary Anaesthesia and Analgesia

JF - Veterinary Anaesthesia and Analgesia

SN - 1467-2987

IS - 6

ER -