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  • 10/2/5:25:01

    時(shí)間:2024-09-25 22:16:06 醫(yī)學(xué)畢業(yè)論文 我要投稿
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    10/2/20075:25:01

    畢業(yè)論文

    M53.doc 1 10/2/20075:25:01 PM
    Comparative clinical pharmacology of dexmedetomidine
    Akira Asada, MD
    Professor and Chair
    Department of Anesthesiology and Intensive Care Medicine
    Osaka City University Medical School
    Drugs used for sedation include analgesics such as opioids, sedatives such
    as propofol and midazolam, or neuroleptics. All of these agents have
    adverse consequences, such as respiratory depression, delirium, lack of
    orientation and cooperation, hypotension, tolerance and abuse potential. A
    new agent, dexmedetomidine was approved for sedation in the intensive
    care unit in Japan in 2004. Dexmedetomidine is an alpha-2 agonist that acts
    on the locus ceruleus/norepinephrine axis, providing non-REM sleep,
    sedation, anxiolysis without respiratory depression. The agent produces
    both sedative and analgesic properties through the effects on the alpha-2
    receptors in the brain and spinal cord.
    Many papers have been published to show the neuroprotective role of the
    agent to improve neurological outcome. The agent produced a
    dose-dependent reduction in neuronal injury provoked by oxygen-glucose
    deprivation in glial-neuronal cultures derived from rats. The agent usually
    causes a decrease in heart rate, and blood pressure as a result of a centrally
    mediated reduction in sympathetic tone. The reduction may have a
    beneficial effect on the heart.
    The agent can facilitate the extubation process by attenuating the
    hemodynamic responses without respiratory depression. Another novel
    advantage of the agent is to make a sedated patient aroused easily to
    demonstrate normal cognitive ability. Therefore, a neurological assessment
    could be done whenever required. The duration for mechanical ventilation
    and days for hospital stay would be reduced by the agent.
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