ketamine Flashcards
what is ketamine
phencyclidine derivative
uses of ketamine
- induction of general anaesthesia,
-as an analgesic agent
-@ subanaesthetic dose- 0.2-0.5mg/kg
-to provide analgesia and sedation for short procedures,
-as an adjunct in epidural anaesthesia
- management of severe asthma.
main mechanism of ketamine
-interaction with the phencyclidine binding site at the N-methyl-D-aspartate (NMDA) receptor, resulting in non- competitive antagonism of L-glutamate (a major excitatory neurotransmitter in
the central nervous system).
-Ketamine also has local anaesthetic properties in high doses (sodium channel blockade) along with interaction at opioid, monoaminergic, muscarinic and nicotinic receptors.
-typically causes dissociative anaesthesia and has a number of benefits, including analgesic properties, maintenance of airway tone and spontaneous ventilation with cardiovascular stability.
major drawback of ketamine
as an anaesthetic agent
association with emergence reactions, delirium, hallucinations and vivid dreams.
pharmacokinetics of ketamine
-a chiral centre with two optical stereoisomers: R- and S-ketamine.
-S-ketamine is the more potent enantiomer, with fewer side effects, shorter recovery time and greater affinity for the NMDA receptor
-The pKa of ketamine is 7.5.
-Ketamine is highly lipid soluble (up to 10 times more soluble than thiopentone) and penetrates the blood–brain barrier rapidly.
-Peak plasma-occur within 1 minute after IV administration and within 5 minutes after IM injection.
-PPB- Ketamine is not significantly bound to plasma proteins and leaves the blood rapidly to be distributed into tissues.
-Initially, ketamine is distributed to highly perfused tissues such as the brain, where the peak concentration may be 4 or 5 times that present in plasma.
- ketamine-induced increases in cerebral blood flow could facilitate delivery of drug and thus enhance rapid achievement of high brain concentrations
-Subsequently, ketamine is redistributed from the brain and other highly perfused tissues to less well-perfused tissues, the release of which results in late psychodynamic effects after emergence.
-Ketamine has a high hepatic clearance rate (1 L per minute) and a large Vd (3 L/kg), resulting in an elimination half-time of 2 to 3 hours.
-The high hepatic extraction ratio suggests that alterations in hepatic blood flow could influence ketamine’s clearance rate.
Metabolism
-metabolized extensively by hepatic microsomal enzymes.
-demethylation of ketamine by
cytochrome P450 enzymes to form norketamine and subsequently hydroxynorketamine
-active metabolite-norketamine is one-fifth to one-third as potent as ketamine
-contribute to prolonged effects of ketamine (analgesia), especially with repeated doses or a continuous IV infusion
can develop tolerance and dependence
-Accelerated metabolism of ketamine as a result of enzyme induction
-occurs in patients receiving repeated doses of this drug.
