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  • 1
    Electronic Resource
    Electronic Resource
    Springer
    Der Anaesthesist 43 (1994), S. 26-29 
    ISSN: 1432-055X
    Keywords: Schlüsselwörter: Spinalanästhesie – Säuglinge – Adrenalin – Bupivacain – Wirkdauer ; Key words: Spinal anaesthesia – Pre-term infant – Epinephrine – Bupivacaine – Duration
    Source: Springer Online Journal Archives 1860-2000
    Topics: Medicine
    Description / Table of Contents: Abstract. The duration of spinal anaesthesia in infants is short compared to adult patients. When tetracaine is used, the addition of epinephrine significantly prolongs the duration. For bupivacaine, however, the influence of epinephrine on the duration is not clear. We investigated the effects of epinephrine 1: 200 000 added to bupivacaine 0.5% on duration and haemodynamics. Patients and Methods. Ten former pre-term infants with postnatal respiratory problems, scheduled for bilateral inguinal hernia repair, were enrolled in the study after informed parental consent had been obtained. The infants were fasted at least 4 h prior to surgery. If they did not receive i.v. infusions before surgery, a bolus of 10 ml/kg Ringer's acetate was injected after inserting the i.v. cannula, followed by a continuous infusion of 8 ml/kg 2/3 N NaCl with 5% dextrose. Spinal anaesthesia was performed in a sitting position with 0.6 ml bupivacaine 0.5%. Five patients received plain bupivacaine (group I) and five bupivacaine with epinephrine 1: 200 000 (group II). Heart rate registered by ECG and non-invasive blood pressure were recorded prior to positioning the baby for lumbar puncture and 2, 5, 10, and 20 min after injection of bupivacaine. The duration of spinal anaesthesia was defined as the time from injection to the time when the first movements of the legs were observed after stimulation. For testing statistical differences the U test was used between the groups and the Wilcoxon and Wilcox test within the groups. Results (expressed as median and range). Additional epinephrine significantly prolonged the duration of spinal anaesthesia (group II: 95 min [60 – 120] vs group I: 50 min [37 – 85]). Haemodynamic parameters did not differ at any time between or within the groups. In group I, one infant had high spinal anaesthesia with impaired respiration but without cardiovascular effects; after 10 min of assisted ventilation by mask, sufficient respiration as judged by pulse oximetry and clinical observation had returned. The duration of spinal anaesthesia in this child was 60 min. Conclusions. Epinephrine 1: 200 000 significantly prolongs the duration of spinal anaesthesia in former preterm infants. Haemodynamic parameters in this age group remain unchanged during spinal anaesthesia and are not influenced by the addition of epinephrine.
    Notes: Zusammenfassung. Bei 10 ehemaligen Frühgeborenen mit einem Gestationsalter zwischen 38 und 48 Wochen am Operationstag und einem Gewicht zwischen 2,10 und 3,22 kg, die postpartal respiratorische Adaptationsstörungen aufwiesen, wurde nach elterlichem Einverständnis eine Spinalanästhesie mit 0,6 ml Bupivacain 0,5% für eine Leistenhernienoperation durchgeführt. Jeweils 5 Patienten erhielten Bupivacain ohne Adrenalinzusatz (Gruppe I) bzw. mit Adrenalin 1: 200 000=5 µg/ml (Gruppe II). Die Wirkdauer wurde definiert als Zeit von der Injektion bis zur ersten Bewegung der Beine: Die über das EKG registrierte Herzfrequenz und die oszillometrisch gemessenen Blutdruckwerte wurden vor Lagerung zur Lumbalpunktion sowie 2, 5, 10 und 20 min nach der Injektion des Lokalanästhetikums erhoben. Die Wirkdauer einer Spinalanästhesie war im Median in der Gruppe II mit 95 min (60 – 120) signifikant länger als in der Gruppe I mit 50 min (37 – 85). Keine signifikanten Unterschiede zeigten sich bei Herzfrequenz und Blutdruckwerten – weder zwischen den Gruppen noch im zeitlichen Verlauf einer Gruppe.
    Type of Medium: Electronic Resource
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  • 2
    Electronic Resource
    Electronic Resource
    Oxford, UK : Blackwell Publishing Ltd
    Pediatric anesthesia 5 (1995), S. 0 
    ISSN: 1460-9592
    Source: Blackwell Publishing Journal Backfiles 1879-2005
    Topics: Medicine
    Notes: Twenty ASA 1 children, one to six years old, weighing 10–20 kg, scheduled for a combination of general and caudal anaesthesia received at random midazolam 0.2, 0.4, or 0.6 mg·kg−1 or NaCl 0.9% (control group) intranasally. Drug or NaCl 0.9% were administered in one nostril, after inhalation induction of anaesthesia, intubation without relaxant and caudal anaesthesia. Spontaneous respiration was via a circle system and fresh gas flow of 61·min−1 (N2O/O2= 2:1), PEEP 5 cm H2O, endtidal halothane 0.4%.Immediately before and 2, 5, 8, 12, 16, 20, 30, 60 and 120 min after application of the drug 2.5 ml blood was sampled for plasma levels of midazolam. Endtidal CO2, respiratory rate, and oxygen saturation were recorded as long as the children were intubated. Endtidal CO2 and respiratory rate showed no statistical difference between the groups at any time, however, in the group receiving 0.6 mg·kg−1, -endtidal CO2 increased significantly from 5.3 kPa (41 mm Hg) at the start to 5.9 kPa (45.5 mm Hg) after 30 min. Plasma levels of midazolam were detected 2 min after application in 10 of 15 patients. Median peak levels were found between 12 and 16 min. Medians of peak plasma levels showed no statistical difference between the three groups (0.2 mg·kg−1:111 ng·ml−1, 0.4 mg·kg−1:136 ng·ml−1, 0.6 mg·kg−1:277 ng·ml−1). After 30, 60 and 120 min medians of midazolam plasma concentration were significantly higher in the group 0.6 mg·kg−1.
    Type of Medium: Electronic Resource
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