• Reg Anesth Pain Med · May 2002

    Randomized Controlled Trial Comparative Study Clinical Trial

    Preemptive analgesia: no relevant advantage of preoperative compared with postoperative intravenous administration of morphine, ketamine, and clonidine in patients undergoing transperitoneal tumor nephrectomy.

    • Holger Holthusen, Peter Backhaus, Frank Boeminghaus, Maria Breulmann, and Peter Lipfert.
    • Department of Anesthesiology, Heinrich-Heine-University, Duesseldorf, Germany. holthusen@med.uni-duesseldorf.de
    • Reg Anesth Pain Med. 2002 May 1; 27 (3): 249-53.

    Background And ObjectivesPreemptive analgesia often failed in the clinical arena because application of a single intravenously applied drug may not prevent nociceptive input and spinal pain processing sufficiently. We therefore used an intravenous (IV), multireceptor approach and tested the preemptive analgesic effect of the antinociceptive drugs morphine, ketamine, and clonidine given before or immediately after surgery.MethodsA double-blind, randomized, prospective study was performed in 30 patients undergoing transperitoneal tumor nephrectomy (via median laparotomy). Standard general anesthesia procedure without opioids was used. After induction, patients were randomly allocated to receive 150 microg x kg(-1) of morphine, 150 microg x kg(-1) of ketamine, and 5 microg x kg(-1) of clonidine intravenously via a motor-driven pump within 15 minutes, either before or immediately after surgery. Patient-controlled analgesia (PCA) with the opioid piritramide (IV) was used for postoperative analgesia. Postoperative pain at rest and during induced cough was quantified by analgesic requirement and pain scores (visual analog scale [VAS]) within 48 hours.ResultsThere was no significant difference in analgesic requirement of piritramide and pain scores at rest or during induced cough.ConclusionsIn contrast to encouraging observations on the combination of antinociceptive drugs, the multireceptor approach tested here failed to exert a clinically relevant effect.

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