B.A. Loughnan scite author profile

B.A. Loughnan

5Publications

85Citation Statements Received

41Citation Statements Given

How they've been cited

216

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Affiliations

Northwick Park Hospital, Royal London Hospital, St Mark's Hospital

Publications

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Randomized controlled comparison of epidural bupivacaine versus pethidine for analgesia in labour

Loughnan

Carli

Romney

et al. 2000

British Journal of Anaesthesia

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We compared the incidence of Caesarean delivery in nulliparous women randomized to receive epidural analgesia with those randomized to intramuscular (i.m.) pethidine. On admission to the delivery suite in established labour, 802 nulliparae had already agreed to be randomized with respect to their first analgesia. One hundred and eighty-eight women required either no analgesia or 50% nitrous oxide in oxygen (Entonox) only. Of the remaining 614 women, 310 were randomly allocated to receive i.m. pethidine up to 300 mg and 304 to receive epidural bupivacaine. Labour management was standardized according to the criteria for active management of labour. The intention-to-treat analysis showed similar Caesarean section rates in those randomized to epidural (12%) or pethidine analgesia (13%). The difference in Caesarean rate was -1.1% with 95% confidence intervals from -6.3% to +4.1%. The normal vaginal delivery rates were similar (epidural, 59%; pethidine, 61%).

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Speed of onset of regional analgesia in labour: a comparison of the epidural and spinal routes

Nickells¹,

Vaughan²,

Lillywhite³

et al. 2000

Anaesthesia

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SummaryThis study compares the speed of onset of effective analgesia in two randomly assigned groups of patients requesting analgesia in labour. Patients in the combined spinal-epidural group (n ¼ 69) were given a subarachnoid injection of 1.5 ml containing bupivacaine 2.5 mg and fentanyl 25 mg for initiation of analgesia. Patients in the epidural group (n ¼ 73) were given an epidural injection of 10 ml containing bupivacaine 12.5 mg and fentanyl 50 mg. Mean (SD) onset times to the first pain-free contraction were 10.0 (5.7) min in the combined spinal-epidural group and 12.1 (6.5) min in the epidural group (p ¼ 0.054). Patients in the combined spinal-epidural group suffered a higher incidence of motor weakness and proprioceptive deficit than those in the epidural group (p ¼ 0.01). The incidence of technique failure and side-effects was similar in the two groups. It is our contention that the statistically nonsignificant difference in onset times does not justify the additional potential for side-effects and the extra cost of the equipment involved in the combined spinal-epidural technique.

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Speed of Onset of Regional Analgesia in Labour: A Comparison of the Epidural and Spinal Routes

Nickells

Vaughan

Lillywhite

et al. 2000

Obstetrical & Gynecological Survey

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Effects of Halothane on Motor Evoked Potential Recorded in the Extradural Space

Loughnan¹,

Anderson

Hetreed

et al. 1989

British Journal of Anaesthesia

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We studied the effects of supplementing nitrous oxide-oxygen anaesthesia with halothane (1 MAC end-tidal concentration) on the motor evoked potential recorded in the extradural space of eight patients before corrective surgery for idiopathic adolescent scoliosis. The motor cortex was stimulated electrically through the scalp. An additional eight patients in whom anaesthesia was supplemented with an infusion of propofol acted as a control group. Halothane had no significant effect on the amplitude or latency of the motor evoked potential. We conclude that halothane is unlikely to alter the interpretation of motor evoked potentials recorded extradurally during scoliosis surgery.

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Nalbuphine for obstetric analgesia

et al. 1987

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B.A. Loughnan

Randomized controlled comparison of epidural bupivacaine versus pethidine for analgesia in labour

Speed of onset of regional analgesia in labour: a comparison of the epidural and spinal routes

Speed of Onset of Regional Analgesia in Labour: A Comparison of the Epidural and Spinal Routes

Effects of Halothane on Motor Evoked Potential Recorded in the Extradural Space

Nalbuphine for obstetric analgesia

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