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Cardiopulmonary Effects of Carfentanil in Dama Gazelles (Gazella dama)

Sixteen (10 female, six male) captive-born dama gazelles (Gazella dama) weighing 48 ± 10 kg ($\overline{x}$± SD) were used to evaluate the cardiopulmonary effects of i.m. carfentanil and to validate the use of pulse oximetry in immobilized gazelles. Carfentanil (18.4 ± 2.2 μg/kg i.m.) produced rapid...

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Published in:Journal of zoo and wildlife medicine 1997-06, Vol.28 (2), p.166-170
Main Authors: Schumacher, Juergen, Heard, Darryl J., Young, Lee, Citino, Scott B.
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Language:English
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Heard, Darryl J.
Young, Lee
Citino, Scott B.
description Sixteen (10 female, six male) captive-born dama gazelles (Gazella dama) weighing 48 ± 10 kg ($\overline{x}$± SD) were used to evaluate the cardiopulmonary effects of i.m. carfentanil and to validate the use of pulse oximetry in immobilized gazelles. Carfentanil (18.4 ± 2.2 μg/kg i.m.) produced rapid induction (6 ± 3 min), moderate muscle relaxation, and a significant (P &lt 0.05) decrease in heart rate (87 ± 12 beats/min) beginning 5 min following induction and continuing throughout the immobilization period. A decrease in respiratory rates began 15 min following induction (11 ± 4 breaths/min). Systemic hypertension was present throughout the immobilization period. Arterial blood gas analysis, performed at 10, 20, and 30 min after induction, showed PaCO₂ and PaO₂ values within normal limits. Arterial blood oxygen saturation (SaO₂) was &lt95% 10 min after induction. Relative arterial oxygen saturation (SpO₂) values indicated by pulse oximetry were generally lower than SaO₂ values but reliably demonstrated trends in arterial oxygen saturation as confirmed by arterial blood gas analysis. Periods of hypoxemia were usually indicated by the pulse oximeter reading and confirmed by SaO₂ measurements. There was an increase in creatine phosphokinase values (88 ± 53 U/L to 109 ± 48 U/L) at 30 min postimmobilization. Naltrexone reversal (1.8 ± 0.3 mg/kg, half i.v. and half s.c.) was rapid and uneventful, and time to standing was 2 ± 1 min.
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Carfentanil (18.4 ± 2.2 μg/kg i.m.) produced rapid induction (6 ± 3 min), moderate muscle relaxation, and a significant (P &amp;lt 0.05) decrease in heart rate (87 ± 12 beats/min) beginning 5 min following induction and continuing throughout the immobilization period. A decrease in respiratory rates began 15 min following induction (11 ± 4 breaths/min). Systemic hypertension was present throughout the immobilization period. Arterial blood gas analysis, performed at 10, 20, and 30 min after induction, showed PaCO₂ and PaO₂ values within normal limits. Arterial blood oxygen saturation (SaO₂) was &amp;lt95% 10 min after induction. Relative arterial oxygen saturation (SpO₂) values indicated by pulse oximetry were generally lower than SaO₂ values but reliably demonstrated trends in arterial oxygen saturation as confirmed by arterial blood gas analysis. Periods of hypoxemia were usually indicated by the pulse oximeter reading and confirmed by SaO₂ measurements. There was an increase in creatine phosphokinase values (88 ± 53 U/L to 109 ± 48 U/L) at 30 min postimmobilization. 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Carfentanil (18.4 ± 2.2 μg/kg i.m.) produced rapid induction (6 ± 3 min), moderate muscle relaxation, and a significant (P &amp;lt 0.05) decrease in heart rate (87 ± 12 beats/min) beginning 5 min following induction and continuing throughout the immobilization period. A decrease in respiratory rates began 15 min following induction (11 ± 4 breaths/min). Systemic hypertension was present throughout the immobilization period. Arterial blood gas analysis, performed at 10, 20, and 30 min after induction, showed PaCO₂ and PaO₂ values within normal limits. Arterial blood oxygen saturation (SaO₂) was &amp;lt95% 10 min after induction. Relative arterial oxygen saturation (SpO₂) values indicated by pulse oximetry were generally lower than SaO₂ values but reliably demonstrated trends in arterial oxygen saturation as confirmed by arterial blood gas analysis. Periods of hypoxemia were usually indicated by the pulse oximeter reading and confirmed by SaO₂ measurements. There was an increase in creatine phosphokinase values (88 ± 53 U/L to 109 ± 48 U/L) at 30 min postimmobilization. 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There was an increase in creatine phosphokinase values (88 ± 53 U/L to 109 ± 48 U/L) at 30 min postimmobilization. Naltrexone reversal (1.8 ± 0.3 mg/kg, half i.v. and half s.c.) was rapid and uneventful, and time to standing was 2 ± 1 min.</abstract><cop>United States</cop><pub>American Association of Zoo Veterinarians</pub><pmid>9279405</pmid><tpages>5</tpages></addata></record>
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ispartof Journal of zoo and wildlife medicine, 1997-06, Vol.28 (2), p.166-170
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subjects Analgesics, Opioid - antagonists & inhibitors
Analgesics, Opioid - pharmacology
Animals
Animals, Zoo
Antelopes - physiology
Blood
Blood gas analysis
Blood Gas Analysis - veterinary
Blood Pressure - drug effects
Carbon Dioxide - blood
Female
Fentanyl - analogs & derivatives
Fentanyl - antagonists & inhibitors
Fentanyl - pharmacology
Gazelles
Heart rate
Heart Rate - drug effects
Hemoglobins
Immobilization
Male
Naltrexone - pharmacology
Narcotic Antagonists - pharmacology
Oximetry - veterinary
Oxygen
Oxygen - blood
Pregnancy
Pulse oximetry
Reproducibility of Results
Respiration - drug effects
Respiratory rate
Veterinary medicine
Zoos
title Cardiopulmonary Effects of Carfentanil in Dama Gazelles (Gazella dama)
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