Pharmacology Comprehensive Study Guide: Section 2

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GABAA receptors are ligand-gated ion channels, more specifically members of the...

"Cys-loop" superfamily that also includes nicotinic acetylcholine (nAChR), glycine, and serotonin type 3 (5-hydroxytryptamine type 3, or 5-HT3) receptors. Each of these receptors is formed as a pentameric combination of transmembrane protein subunits.

Tactile evaluation of double burst stimulation may be better to differentiate...

"fade" than TOF

Myasthenia Gav(MG), the most common and well studied postsynaptic neuromuscular transmission disorder, is caused by antibody-mediated reduction in the number of functioning...

"postsynaptic" AChRs. This complement-mediated destruction is caused by a variety of actions including antibodies directed against the AChR.

Lambert-Eaton myasthenic syndrome (LEMS) is an acquired...

"presynaptic" disorder of neuromuscular transmission caused by autoantibodies directed against voltage-gated Ca2 + channels in the motor nerve terminal resulting in down-regulation by endocytosis.

When given in very high doses, thiopental can even exhibit...

"zero order kinetics," wherein metabolic capacity is saturated, grossly prolonging the duration of action.

Antagonism of nondepolarizing neuromuscular blockade by acetylcholinesterase inhibitors depends primarily on five factors:

(1) Depth of the blockade when reversal is attempted (2) Anticholinesterase used (3) Dose administered (4) Rate of spontaneous clearance of the neuromuscular blocker from plasma (5) Choice of anesthetic drugs and the depth of anesthesia

There are three main classes of α2 agonists:

(1) Phenylethylates (α-methyl DOPA, guanabenz) (2) Imidazolines (clonidine, dexmedetomidine, mivazerol) (3) Oxaloazepines

Anticholinesterase drugs are classified according to the mechanism by which they inhibit the activity of acetylcholinesterase:

(a) Reversible inhibition (b) Formation of carbamyl esters (c) "Irreversible" inactivation by organophosphates

Edrophonium is used to:

(a) antagonize the effects of nondepolarizing neuromuscular-blocking drugs b) diagnose and assess therapy of myasthenia gravis and cholinergic crisis (c) evaluate the presence of dual blockade produced by succinylcholine.

PROPOFOL (Diprivan): Dose

**Base on LBW (IBW + 20%) *Induction: 1-2.5mg/kg, Pedi: 2.5-3.5mg/kg *Infusion: 25-200 mcg/kg/hr

Endogenous Ligand: Mu (μ)

**Endorphins *β-Endorphin *Endomorphin

Endogenous Ligand: Delta (δ)

**Enkephalins *Leu-enkephalin *Met-enkephalin

ALFENTANIL (Alfenta): MOA

**G Protein-Coupled Receptor *Inhibits the activity of adenylate cyclase *Mu agonist *Kappa agonist *Delta agonist *Serotonin Reuptake Inhibitor

MORPHINE: MOA

**G Protein-Coupled Receptor *Mu agonist *Delta agonist *Kappa agonist *Inhibits the activity of adenylate cyclase

HYDROMORPHONE (Dilaudid): MOA

**G Protein-Coupled Receptor *Mu agonist *Kappa agonist *Delta agonist *Inhibits the activity of adenylate cyclase

METHADONE (Dolophine): MOA

**G Protein-Coupled Receptor *Mu agonist *Kappa agonist *Delta agonist *NMDA Antagonist *Serotonin Reuptake Inhibitor *Norepinephrine Reuptake Inhibitor *Inhibits the activity of adenylate cyclase

FENTANYL (Sublimaze): MOA

**G Protein-Coupled Receptor *Mu agonist *Kappa agonist *Delta agonist *Serotonin Reuptake Inhibitor *Inhibits the activity of adenylate cyclase

REMIFENTANIL (Ultiva): MOA

**G Protein-Coupled Receptor *Mu agonist *Kappa agonist *Delta agonist *Serotonin Reuptake Inhibitor *Inhibits the activity of adenylate cyclase

SUFENTANIL (Sufenta): MOA

**G Protein-Coupled Receptor *Mu agonist *Kappa agonist *Delta agonist *Serotonin Reuptake Inhibitor *Inhibits the activity of adenylate cyclase

MEPERIDINE (Demerol): MOA

**G Protein-Coupled Receptor *Mu agonist *Kappa agonist *Delta agonist *mACh Antagonist *Alpha2b agonist (possibly) *Sodium Channel Antagonist *Serotonin Reuptake Inhibitor *Inhibits the activity of adenylate cyclase

NALBUPHINE (Nubain): MOA

**G Protein-Coupled Receptor *Mu antagonist *Kappa partial-agonist *Delta Agonist

NALOXONE (Narcan): MOA

**G Protein-Coupled Receptor *Mu antagonist (high) *Delta antagonist (moderate) *Kappa antagonist (moderate) *Inhibits the activity of adenylate cyclase

BUTORPHANOL (Stadol): MOA

**G Protein-Coupled Receptor *Partial Kappa agonist *Competitive Kappa antagonist *Partial Mu agonist *Competitive Mu antagonist

CODEINE: MOA

**G Protein-Coupled Receptor *Prodrug *Mu agonist *Kappa agonist *Delta agonist *Inhibits the activity of adenylate cyclase

HYDROCODONE: MOA

**G Protein-Coupled Receptor *Prodrug *Mu agonist *Kappa agonist *Delta agonist *Inhibits the activity of adenylate cyclase

OXYCODONE: MOA

**G Protein-Coupled Receptor *Prodrug *Mu agonist *Kappa2b agonist *Delta agonist *Inhibits the activity of adenylate cyclase

BUPRENORPHINE (Buprenex, Subutex, Suboxone, Butrans): MOA

**G-Protein Coupled Recepter *Inhibits the activity of adenylate cyclase *Partial μ-opioid agonist displaying high affinity for and slow dissociation from the μ-opioid receptor *Considered to be a partial Mu agonist (e.g., has limited intrinsic activity) and accordingly can display antagonism when used in conjunction with a full agonist *Kappa Antagonist *Delta Antagonist

TRAMADOL (Ultram): MOA

**G-Protein Coupled Recepter *Inhibits the activity of adenylate cyclase *Supplied as a racemic mixture *Mu agonist (M1 metabolite binds to Mu greater than parent drug) *Inhibits Serotonin reuptake *Inhibits Norepinephrine uptake *α2 Agonist *NMDA receptor antagonist *5-HT2C receptor antagonist *Nicotinic Acetylcholine receptor antagonist *Muscarinic(M1/M3) Acetylcholine receptor antagonist *TRPV1 receptor agonist

DIAZAPAM (Valium): Onset/Half-life/DOA

**Onset *1-5 min IV *30-60 min PO/PR **Peak *15-60 min IV *1-2 hr PO/PR *HL: 20-50 hr **DOA: 3 hr

LORAZEPAM (Ativan): Onset/Half-life/DOA

**Onset: *1-5 min IV *20-30 min PO **Peak *15-20 min IV *2 hr PO *HL: 10-20 hr IV **DOA: 6-10 hr

CATAPRES (Clonidine): Onset/Peak/Half-life/DOA

**Onset: *< 1min IV * min PO **Peak * min IV *1-3 hr PO *DHL: 7-15min **EHL: * IV *6-24 hr PO **DOA: *min IV *hr PO

MIDAZOLAM (Versed): Onset/Half-life/DOA

**Onset: *< 1min IV *10min PO *15min IM **Peak *10 min IV *20-30 min PO *HL: 1-4 hr IV **DOA: *15-90min IV *2-6hr PO *15-90min IM

TRAMADOL (Ultram): Dose

**PO *Immediate Release: 25-400 mg/day in 4 doses *Extended Release: 100-300 mg/day in 1 dose

PYRIDOSTIGMINE (Mestinon, Regonol): Dose/Onset/Peak/HL/DOA/VD

*0.1-0.4 mg/kg *Onset: 2-4 min *Peak: 15 min *HL: 90 min *DOA: 90-180 min *VD: 1.1 L/KG *Poor lipid solubility

C Sympathetic Fiber: Diameter

*0.3-1.3 μm

C Dorsal Root Fiber: Diameter

*0.4-1.2 μm

TOF: Established anesthesia

*1-2 twitches

Aδ Fiber: Diameter

*1-4 μm

LORAZEPAM (Ativan): Dose

*1-4mg IV

Dosing for lipid emulsion therapy?

*1.5mL/kg 20% bolus followed by 0.25ml/kg/min for at least 10 minutes after circulatory stability. If circulatory stability is not attained consider another bolus and increasing infusion to 0.5ml/kg/min.

MEPERIDINE (Demerol): Considerations

*1/10 as strong at Morphine *May cause dilated pupils *May increase heart rate and decrease cardiac contractility *Structurally similar to atropine (vagolytic properties) *Associated with more euphoria, difficulty concentrating, confusion, and impaired psychomotor and cognitive performance

TRAMADOL (Ultram): Considerations

*1/6000 the Mu activity of Morphine

KETAMINE (Ketalar): PharmacoKINETICS

*10% protein binding - leaves the plasma quickly *Rapid CNS effects R/T extremely high lipid solubility and large unbound fraction *Rapid redistribution from brain out of the central circulation to peripheral tissues accounts for rapid re-awakening after a single dose

ATRACURIUM BESYLATE (Tracrium): Metabolism

*10-40% Hofmann elimination *Enzymatic ester hydrolysis and renal elimination have lesser roles (some studies suggest up to 65%). *Laudanosine metabolite excreted in urine *The Ester hydrolysis involved in atracurium metabolism is catalyzed by a nonspecific esterase distinct from the butyrylcholinesterase responsible for hydrolysis of succinylcholine and mivacurium.

LIDOCAINE (Xylocaine): EHL

*100 min

PRILOCAINE (Citanest): EHL

*100 min

FENTANYL (Sublimaze): Considerations

*100X strong as Morphine *Produce a slowing of heart rate by directly increasing vagal nerve tone in the brainstem

REMIFENTANIL (Ultiva): Considerations

*100X strong as Morphine (Same as Fentanyl) *Produce a slowing of heart rate by directly increasing vagal nerve tone in the brainstem

ROPIVICAINE (Naropin): EHL

*110 min

MEPIVICAINE (Carbocaine, Polocaine): EHL

*115 min

PROCAINE (Novocaine): Max Dose

*14 mg/kg

CODEINE: Dose

*15mg PO (antitussive) *60mg PO (Analgesia)

BUPIVICAINE (Marcaine, Sensorcaine): Metabolism

*1st pass lung (lipophilic drugs taken quickly into lungs which are the 1st vascular bed after heart) *Hepatic Metabolism *Renal excretion

LIDOCAINE (Xylocaine): Metabolism

*1st pass lung (lipophilic drugs taken quickly into lungs which are the 1st vascular bed after heart) *Hepatic P450, CYP3A4/5 *Dealkylated to monoethylglycine xylidide and glycine xylidide, which can be metabolized further to monoethylglycine and xylidide. *Both monoethylglycine xylidide and glycine xylidide retain local anesthetic activity. *∼75% of the xylidide is excreted in the urine as the further metabolite 4-hydroxy-2, 6-dimethylaniline

ROPIVICAINE (Naropin): Metabolism

*1st pass lung (lipophilic drugs taken quickly into lungs which are the 1st vascular bed after heart) *Hepatic P450, CYP3A4/5 *Metabolized to 2,6-pipecoloxylidide and 3-hydroxyropivacaine *Renal excretion

The postjunctional nicotinic acetylcholine receptor is a pentameric member of the superfamily of ligand-gated ion channels. This mature form consists of five subunits:

*2 alpha (α) *1 delta (δ) *1 beta (β) *1 epsilon (ε) **In the immature (fetal) form, the ε subunit is replaced by a gamma (γ) subunit.

The NMJ contains three types of nicotinic cholinergic receptors (nAChRs):

*2 are postsynaptic on the skeletal muscle surface -1 Junctional -1 Extrajunctional *And 1 is presynaptic on the nerve ending

DIAZAPAM (Valium): Dose

*2-10mg IV

MIDAZOLAM (Versed): Considerations

*2-4X as strong as Diazapam

BUPIVICAINE (Marcaine, Sensorcaine): EHL

*210 min

BUPRENORPHINE (Buprenex, Subutex, Suboxone, Butrans): Considerations

*25-50X Strong as Morphine *Thus, care should be taken in treating patients who also are taking known inhibitors of CYP3A4 (e.g., azole antifungals, macrolide antibiotics, and HIV protease inhibitors), as well as drugs that induce CYP3A4 activity (e.g., certain anticonvulsants and rifampin). *Unable to be reversed by Narcan d/t strong Mu binding

TOF: Attempting reversal of neuromuscular blockage

*3-4 twitches

Aγ Fiber: Diameter

*3-6 μm

COCAINE: EHL

*30-90 mins

Train-of-four

*4 impulses at 2 Hz every 1/2 seconds for 2 seconds *Most common used *Does not require baseline

COCAINE: Max Dose

*4% Topical: 3 mg/kg (200mg total)

Structure of nAChR

*5 glycoprotein subunits: -2 alpha -1 beta -1 delta -1 epsilon *arrainged in cylindrical fashion and the center is an ion channel *pre & postjunctional receptors have different affinities for ACh

ALFENTANIL (Alfenta): Considerations

*5-10X strong as Morphine *1/5 - 1/10X strong as Fentanyl *Produce a slowing of heart rate by directly increasing vagal nerve tone in the brainstem

HYDROMORPHONE (Dilaudid): Considerations

*5-8X Strong as Morphine *Less nausea and pruritis than morphine? *May have hypotension/Histamine release

NEOSTIGMINE (Prostigmin, Vagostigmin): Metabolism

*50% hydrolyzed by plasma esterases and hepatic metabolism to 3-hydroxyphenyltrimethyl ammonium (3-OH PPM) and conjugated 3-OH PPM. *Renal excretion, 50% unchanged in urine *Use cautiously in renal failure

SUFENTANIL (Sufenta): Considerations

*500-1000X strong as Morphine *5-10X strong as Fentanyl *Produce a slowing of heart rate by directly increasing vagal nerve tone in the brainstem

BUTORPHANOL (Stadol): Considerations

*5X strong as Morphine *Analgesic doses of butorphanol produce an increase in pulmonary arterial pressure and in the work of the heart; systemic arterial pressure is slightly decreased *Major side effects of butorphanol are drowsiness, weakness, sweating, feelings of floating, and nausea *While the incidence of psychotomimetic side effects is lower than that with equianalgesic doses of pentazocine, they are qualitatively similar

Aα Fiber: Diameter

*6-22 μm

Aβ Fiber: Diameter

*6-22 μm

VECURONIUM BROMIDE (Norcuron): Metabolism

*60% Liver *40% Renal

CHLOROPROCAINE (Nesacaine): EHL

*7 min

AMITRIPTYLINE (Elavil): Dose

*75 mg PO QD, may increase up to 150-300 mg PO per day

CISATRACURIUM BESYLATE (Nimbex): Metabolism

*75% Hofmann elimination *15% Renal eliminated *Laudanosine metabolite excreted in urine *Unlike Atracurium, "Not" metabolized by enzymatic ester hydrolysis

EDROPHONIUM (Tensilon, Enlon): Metabolism

*75% Renal excretion, although in the absence of renal function, hepatic metabolism accounts for the inactivation of 30%

ROCURONIUM (Zemuron): Metabolism

*80% Liver *20% Renal *Excretion is biliary (50%-70%) & Renal (10-25%)

PANCURONIUM BROMIDE (Pavulon): Metabolism

*85% Renal *15% Liver

PROCAINE (Novocaine): EHL

*9 min

B Fiber: Diameter

*<3 μm

BENZOCAINE (Anbesol, Cepacol, Lanacane, Hurricaine): Dose

*A brief spray of 20% benzocaine delivers the recommended dose of 200 to 300 mg.

What are the chemical structural requirements for a drug to be a local anesthetic?

*A lipophilic end *A hydrophilic end *An intermediate chain which is either an "Este" or an "Amide"

Single Twitch

*A single electrical pulse is delivered at 1 Hz *Requires a baseline before muscle relaxation *The ratio of the evoked twitch is compared with the twitch before muscle relaxation (control twitch) *Gives a crude indication of neuromuscular blockade. If they have any twitch they are not 100% relaxed *Used with depolarizing muscular relaxants *Degree of twitch depression used to calculate level of blockade

Ionotropic glutamate receptors (iGluR) (4):

*AMPA *Kainate *NMDA *Orphin

PHYSOSTIGMINE (Antilirium): Class

*Acetylcholine Inhibitor *Anticholinesterase *Parasympathomimetic *Naturally Occurring Tertiary Amine *Monomethylcarbamate

EDROPHONIUM (Tensilon, Enlon): Class

*Acetylcholine Inhibitor *Anticholinesterase *Parasympathomimetic *Synthetic Quaternary Ammonium Agent

NEOSTIGMINE (Prostigmin, Vagostigmin): Class

*Acetylcholine Inhibitor *Anticholinesterase *Parasympathomimetic *Synthetic Quaternary Ammonium Agent

PYRIDOSTIGMINE (Mestinon, Regonol): Class

*Acetylcholine Inhibitor *Anticholinesterase *Parasympathomimetic *Synthetic Quaternary Ammonium Agent *Dimethylcarbamate

What factors increase the likelihood of local anesthetic systemic toxicity?

*Advanced age *Heart failure *Ischemic heart disease *Conduction abnormalities *Metabolic disease *Liver disease *Low plasma protein concentration *Acidosis *Medications that inhibit sodium channels *Severe cardiac dysfunction with low ejection fraction

Aβ Fiber: Location

*Afferent from skin and joints

How do you treat local anesthetic systemic toxicity

*Airway first *Halt seizures - avoiding large doses of propofol for its cardiac effects, benzodiazepines are primary *Use succinylcholine if there is nothing else *Start ACLS with lower doses of epi *No vasopressin, no calcium channel or beta blockers *Lipid emulsion therapy *Cardiopulmonary bypass

PROPOFOL (Diprivan): Class

*Alkyphenol (2, 6 diisopropylphenol)

Common NMDA receptor antagonists include:

*Amantadine (Symmetrel) *Ketamine *Methoxetamine *Phencyclidine (PCP) *Nitrous oxide *Xenon *Dextromethorphan and dextrorphan *Ethanol *Riluzole (Rilutek)(used in ALS) *Lead (Pb2+)[25]

How do you identify Amide and Ester local anesthetics by their names?

*Amides contain 2 of the letter "I" in their name *Esters have only 1

KETOROLAC (Toradol): Indications

*Analgesic *Antipyretic *Anti-inflammatory

IBUPROFEN (Motrin, Advil): Indications

*Analgesic *Antipyretic *Anti-inflammatory *Rheumatoid arthritis *Osteoarthritis *Acute gouty arthritis *Migraine *Antagonizes Niacin flush *Dysmenorrhea

ACETAMINOPHEN (Tylenol): Indications

*Analgesic *Antipyretic *Migraine

DIAZAPAM (Valium): Indications

*Anxiety, ETOH withdrawal *Status epilepticus *Sedation *Relief of muscle spasms, paraplegia

LORAZEPAM (Ativan): Indications

*Anxiety, ETOH withdrawal *Status epilepticus *Sedation *Relief of muscle spasms, paraplegia

MIDAZOLAM (Versed): Indications

*Anxiety, ETOH withdrawal *Status epilepticus *Sedation *Relief of muscle spasms, paraplegia

Post-tetanic Count

*Apply 5 seconds of 5oHz tetany *Wait 3 seconds, then count eight 1 Hz twitches *Can give an pproximate time until return of response to single twitches *Permits assessment of block too deep for any other techninqu *A Post-tetanic Count (PTC) of 2 by palpation suggests no twitch response for about 20-30 minutes *PTC of 5 about 10-15 minutes

KETAMINE (Ketalar): Class

*Arylcyclohexylamine (Phencyclidine (PCP) derivative)

Current use of anti-AChE agents is limited to four conditions in the periphery:

*Atony of the smooth muscle of the intestinal tract and urinary bladder *glaucoma *myasthenia gravis *reversal of the paralysis of competitive neuromuscular blocking drugs

B Fiber: Function

*Autonomic Function *Vasomotor *Visceromotor *Sudomotor *Pilomotor

METHOHEXITAL SODIUM (Brevital): Class

*Barbiturate (N-methylated oxybarbiturate)

THIOPENTAL SODIUM (Pentothal): Class

*Barbiturate (Thiobarbiturate)

DIAZAPAM (Valium): Class

*Benzodiazepine

LORAZEPAM (Ativan): Class

*Benzodiazepine

MIDAZOLAM (Versed): Class

*Benzodiazepine -Imidazole ring

ROMAZICON (Flumazenil): Class

*Benzodiazepine Antagonist -Imidazole ring

ROMAZICON (Flumazenil): Indications

*Benzodiazepine reversal *Ambien Reversal *β-carboline Reversal

Remifentanil's ester structure renders it susceptible to hydrolysis by nonspecific plasma and tissue esterases to inactive metabolites. This unique pathway of metabolism imparts to remifentanil:

*Brevity of action *Precise and rapidly titratable effect due to its rapid onset (similar to that of alfentanil) and offset *Noncumulative effects *Rapid recovery after discontinuation of its administration

Although all local anesthetics block the cardiac conduction system through a dose-dependent block of Na+ channels, two features of bupivacaine's Na+-channel blocking abilities may enhance its cardiotoxicity:

*Bupivacaine exhibits a much stronger binding affinity to resting and inactivated Na+ channels than lidocaine. *Local anesthetics bind to Na+ channels during systole and dissociate during diastole. Bupivacaine dissociates from Na+ channels during cardiac diastole much more slowly than lidocaine. Indeed, bupivacaine dissociates so slowly that the duration of diastole at physiologic heart rates (60-180 beats per minute) does not allow enough time for complete recovery of Na+ channels and bupivacaine conduction block accumulate.

BUPRENORPHINE (Buprenex, Subutex, Suboxone, Butrans): Metabolism

*Buprenorphine is metabolized to norbuprenorphine by CYP3A4. *Thus, care should be taken in treating patients who also are taking known inhibitors of CYP3A4 (e.g., azole antifungals, macrolide antibiotics, and HIV protease inhibitors), as well as drugs that induce CYP3A4 activity (e.g., certain anticonvulsants and rifampin). *Both N-dealkylated and conjugated metabolites are detected in the urine (10-30%), but most of the drug is excreted unchanged in the feces (70-90%).

DIAZAPAM (Valium): Considerations

*Burns on injection *May induce ALA synthetase activity precipitating an acute porphyria attack

TETRACAINE (Pontocaine): Spinal Dose

*C-Section: 8mg *Abdominal Surgery: <5'6": 12mg 5'6"-6': 15mg >6": 18mg

LIDOCAINE (Xylocaine): Considerations

*CES *TNS *Most potent vasodilator *Metabolites can accumulate in liver disease causing toxicity

ACETAMINOPHEN (Tylenol): Class

*COX Inhibitor

KETOROLAC (Toradol): MOA

*COX Inhibitor *Inhibition of cyclooxygenase (COX) activity resulting in a decrease in the peripheral synthesis of prostaglandins. This inhibition of prostaglandins decreases the inflammatory response to surgical trauma and peripheral nociception and pain perception

IBUPROFEN (Motrin, Advil): MOA

*COX Inhibitor (equipotent of COX-1 & COX-2) *Inhibition of cyclooxygenase (COX) activity resulting in a decrease in the peripheral synthesis of prostaglandins. This inhibition of prostaglandins decreases the inflammatory response to surgical trauma and peripheral nociception and pain perception

ACETAMINOPHEN (Tylenol): MOA

*COX Inhibitor (highly selective for COX-2) *Inhibition of cyclooxygenase (COX) activity resulting in a decrease in the peripheral synthesis of prostaglandins. This inhibition of prostaglandins decreases the inflammatory response to surgical trauma and peripheral nociception and pain perception

ETOMIDATE (Amidate): Class

*Carboxylated Imidazole derivative

LIDOCAINE (Xylocaine): Dose

*Cardiac: 1-1.5mg/kg *Infusion: 1-4mg/min *PNB: 4mg/kg, 7mg/kg w/epi *Epi: 4mg/kg *SAB: 1.5mg/kg *Bier Block: 200mg in 10-40ml (0.5%, 1% or 2%)

Esters: Metabolism

*Catalyzed by plasma and tissue cholinesterase via hydrolysis - it occurs throughout the body and is rapid

KETAMINE (Ketalar): Physiologic Effects

*Causes mydriasis, nystagmus, salivation, lacrimation, and increased skeletal muscle tone after administration *↑HR, SV, DBP, SVR, LVEDP, PAP, RAP, cardiac O2 requirements *Great for hypovolemic patients or patients who can not endure big drop in pressure *BAD for CAD pts because of negative balance between myocardial oxygen supply and demand- propofol or midazolam can attenuate the cardiovascular effects if given prior *Potent analgesic *DOC for active bronchospasm = bronchodilates *Beneficial d/t minimal depressant effects on respiratory rate and airway skeletal muscle tone, pharyngeal and laryngeal reflexes *Can cause apnea w/ induction and increased secretions usually require glycopyrrolate *Avoid atropine or droperidol because they act centrally on the brain and increase SNS activity by blocking the PNS *Myoclonic activity after induction **CNS depression w/ undesirable psychological reactions, which occur during awakening- termed emergence reactions. Occurs in 5-30% of patients and is dose dependent at >2mg/kg. Occur about 1 hour after emergence. Common manifestations of these reactions, which vary in severity and classification, are vivid dreaming, extracorporeal experiences & illusions *Using versed pre-op may block the effects *Subsequent doses usually diminished this problem and you see it more in children, women, and people with a hx of nightmares *Administration of ketamine can prevent hyperalgesia with opioids, which is thought to be due to NMDA activation and spinal sensitization to glutamate and substance p.

PHYSOSTIGMINE (Antilirium): Indications

*Central Anticholinergic Syndrome (CAS) *Glaucoma *Postoperative shivering *Alzheimer's disease *Delayed gastric emptying. *Orthostatic hypotension *Central nervous system effects of atropine, scopolamine and other anticholinergic drug overdoses. *Antidote of choice for Datura stramonium & Atropa belladonna poisoning *Antidote for GHB poisoning *May reverse delirium in babiturate overdose

Antagonism of neuromuscular blockade by anticholinesterase drugs may be inhibited or even prevented by:

*Certain antibiotics *Hypothermia *Respiratory acidosis associated with a PaCO2 of > 50 mm Hg *Hypokalemia and metabolic acidosis

METHADONE (Dolophine): Indications

*Chronic pain *Tx of opioid abstinence syndromes *Tx of heroin users

GABAPENTIN (Neurontin): Class

*Cyclic Analog of GABA

LGICs are classified into three superfamilies which lack evolutionary relationship:

*Cys-loop receptors *Ionotropic glutamate receptors (iGluR) *ATP-gated channels

All three subtypes of the α2-AR share the same signaling pathways in native cells:

*Decrease in adenylyl cyclase activity *Suppression of voltage-gated Ca++ currents *Activation of receptor-operated K+ currents and MAP kinase activity

THIOPENTAL SODIUM (Pentothal): Considerations

*Decreased CBF, CMRO2 and ICP, without compromising CPP *Hypotension d/t peripheral vasodilation w/ reflex tachycardia. There is a decrease in contractility and CO. Mild, transient BP reductions in euvolemia, but decreased CO, systemic vascular resistance, and PVR if hypovolemic = decreased preload in shock patient could lead to death *Liver enzyme induction and decreased hepatic blood flow, but usually only w/ sustained drug delivery (2-7 days) *Anticonvulsant activity *Acute tolerance occurs quickly R/T liver enzyme induction and may require doses up to 6x higher. Physical dependence can occur w/ sustained infusions *Dose dependent resp depression w/ decreased response to hypercarbia and hypoxemia *Airway reflexes intact with smaller doses, but apnea with large doses. Salivation requires treatment *Decreases IOP *Stimulates the release of histamine and may cause allergic rxns *Hang-over, tiredness, N/V, some pain on injection *ASA and coumadin will potentiate thiopental as they compete for the metabolic binding sites *Prolonged elimination in obese *May have anti-analgesic effects

PROPOFOL (Diprivan): Considerations

*Decreases CMRO2, ICP, and CBF.; however also decreases MAP and there for CPP (head injured patients are at risk for hypoperfusion. Decreases IOP) *Myoclonic activity after induction, but has anticonvulsant properties *Dose dependent resp depression *Some bronchodilatory effects *Decreases responsiveness to hypoxia and hypercarbia with a concomitant decrease in pH and increase in PaCO2 *Mild attenuation of HPV *25- 40% decrease in ABP & SVR w/ peripheral arterial and venous dilation causing profound hypotension. There is no reflex bradycardia due to baroreceptor inhibition *Pain on injection very common. Use large IV and vein w/ 1% lidocaine and open fluids *Supports bacterial growth so discard after 6 hours *Propofol infusion syndrome is a rare but lethal syndrome associated with infusion of propofol at 4 mg/kg/hr or more for 48 hours or longer. Rhabdo, hypoxemia, hyperlipidemia, metabolic acidosis, and fatty liver are signs *Agent of choice in suspected malignant hyperthermia *Anti-emetic properties (DOC if high hx of PONV) *Direct suppression of SNS w/ reports of bradycardia and asystole after induction - pre-hydrate to avoid *Prolonged infusions w/ green urine (phenols) and increased uric acid excretion and crystallization in the urine. May see cloudy urine at low pH *Treats opioid induced pruritus and nausea at 10mg w/o reversing analgesia.

SUCCINYLCHOLINE (Anectine, Quelicin): Class

*Depolarizing Agent

Why do we need neuromuscular monitoring?

*Determination of the exact point for intubation *Intraoperative titration of muscle relaxants *determining the exact point for extubation *avoid reversal of muscle relaxants *avoid residual neuromuscular block *avoid possible post operative complications *reduce cost (OR time and medications)

LA Neuroaxial MOA:

*Diffuses through the axolemma, across the dura in an uncharged form to act on nerve roots and the spinal cord. Once inside the neuron, where the pH is lower, the drug becomes protonated and binds to the Na+ channel on the cytoplasm side. It blocks initiation and transmission of nerve impulses by inhibiting passage of sodium ions through inner portion of ion-selective sodium channels in nerve membranes. Inhibition of sodium permeability slows the rate of depolarization so that threshold potential is not reached.

CATAPRES (Clonidine): Considerations

*Do not withhold prior to surgery d/t rebound HTN *Significant hypotension is more likely in patients with high sympathetic tone such as diabetics, the elderly, and those with hypovolemia. *Benefits include anesthesia include preoperative sedation and anxiolysis, drying of secretions (antisialagogue effects), and analgesia *Antishivering effects (α2B)

CARBAMAZEPINE (Tegretol, Equetro): Dose

*Dosing starts at 100 mg PO BID and is increased up to 400-800 mg/day

CATAPRES (Clonidine): Side effects

*Dry mouth *Sedation *Bradycardia *Sexual dysfunction

Protein Binding best indicates...

*Duration of Action

Endogenous Ligand: Kappa (κ)

*Dynorphin

PANCURONIUM BROMIDE (Pavulon): Dose/ED95

*ED95: 0.05mg/kg *Intubating Dose (X ED95): 1-1.5

VECURONIUM BROMIDE (Norcuron): Dose/ED95

*ED95: 0.05mg/kg *Intubating Dose (X ED95): 2-4

CISATRACURIUM BESYLATE (Nimbex): Dose/ED95

*ED95: 0.05mg/kg *Intubating Dose (X ED95): 3-5

ATRACURIUM BESYLATE (Tracrium): Dose/ED95

*ED95: 0.25mg/kg *Intubating Dose (X ED95): 2

ROCURONIUM (Zemuron): Dose/ED95

*ED95: 0.3mg/kg *Intubating Dose (X ED95): 2-4

SUCCINYLCHOLINE (Anectine, Quelicin): Dose/ED95

*ED95: 0.3mg/kg *Intubating Dose (X ED95): 3-5 *Adult: 1-1.5mg/kg *Pediatric: 1-2mg/kg IV and IM: 4mg/kg *Infants: 2-3mg/kg IV *Laryngospasm: 0.1-0.5mg/kg IV or 4-6mg/kg IM *Dosing: TBW

Aγ Fiber: Location

*Efferent to muscle spindles

Aα Fiber: Location

*Efferent to muscles

SUCCINYLCHOLINE (Anectine, Quelicin): Contraindications/Precautions

*Elevated serum potassium levels & cardiac arrest - burns, crush injuries, de-enervation, immobility, spinal cord transections, stroke, trauma, upper motor neuron injury due to up-regulation of extra-junctional receptors, which are very sensitive to succ *<10 y/o *Personal/familial MH *Myopathies, elevated CPK, narrow angle glaucoma, penetrating eye injuries *Atypical pseudocholinesterase patients *Myotonia is an abnormal delay in relaxation after contraction and the use of Succ will result in difficult ventilating conditions so it should be avoided *Echothiophate & Isoflurophate drops (glaucoma) because it depresses plasma cholinesterase activity and inhibits acetylcholinesterase

Nerve axons are further organized within three layers of connective tissue:

*Endoneurium *Perineurium *Epineurium

NALBUPHINE (Nubain): Considerations

*Equipotent to Morphine 1:1 *Less likely to produce dysphoric side effects than is pentazocine *Depresses respiration as much as do equianalgesic doses of morphine; however, exhibits a ceiling effect such that increases in dosage beyond 30 mg produce no further respiratory depression as well as no further analgesia *Does not produce an increase in cardiac index, pulmonary arterial pressure, or cardiac work, and systemic blood pressure

Order of Paralysis for NMB

*Eyes *Extremities *Trunk (from neck down through intercostals) *Abdominal muscles *Diaphragm

CHLOROPROCAINE (Nesacaine): Considerations

*Fast onset *Fast offset *Lowest PB *Neurotoxic with SAB

Aδ Fibers: General

*Fast/Sharp Pain *Synapse at Rexed lamina 1 & 5 *First order neurons form A-delta fibers communicate with second order neuron in Rexed lamina 1 & 5. *The major neurotransmitter released from A-delta fibers is Glutamate which binds to AMPA receptors on the post synaptic membrane of A-delta interneurons.

The ketorolac package insert advises the following intravenous dosing protocol:

*For a single dose, 30 mg IV or 15 mg if patient age is greater than 65 or body weight less than 50 kg. *For multiple dosing, patients should be commenced on 30 mg q6 hrs, not to exceed 120 mg in a 24-hour period; in those older than 65 yrs or weighing less than 50 kg, the dosing should be 15 mg every 6 hrs, not to exceed 60 mg in 24 hrs. *In no circumstance should dosing go beyond 5 days of therapy.

GABAPENTIN (Neurontin): MOA

*G Protein-Coupled Receptor *Ion Channel Gated Ion *Ca2+ Channel Antagonist *NMDA Receptor Inhibitor *Alpha2 Adrenergic Receptor Agonist *Adenosine A1 Receptor Agonist *Analgesic effects may be related to calcium influx inhibition as well as inhibition of the release of excitatory neurotransmitters in spinal and supraspinal pathways *Interacts with voltage-sensitive calcium channels in cortical neurons. *Increases the synaptic concentration of GABA, enhances GABA responses at non-synaptic sites in neuronal tissues, and reduces the release of mono-amine neurotransmitters *Reduction of the axon excitability measured as an amplitude change of the presynaptic fibre volley (FV) in the CA1 area of the hippocampus

CATAPRES (Clonidine): MOA

*G-protein coupled receptors *α2 Receptor Agonist *α1 Receptor Agonist *I1 (Imidazoline) Receptor agonist *α2:α1-receptor affinity of 220:1

PRECEDEX (Dexmedetomidine): MOA

*G-protein coupled receptors *α2 Receptor Agonist *α1 Receptor Agonist *α2:α1-receptor affinity of 1620:1 *Acts presynaptically and postsynaptically *Leads to hyperpolarization via K+ influx with a subsequent decrease in neuronal firing as well as reduced norepinephrine release mediated by inhibitory presynaptic autoreceptors. It also decreases cAMP concentration by inhibiting adenylyl cyclase. *Decreases sympathetic tone by inhibition of Ca2+ influx in locus ceruleus neurons *Sedative effects are produced by actions in the "locus ceruleus"

Anionic Cys-loop Receptors (2):

*GABAA *Glycine (GlyR)

Signs of Recovery from Neuromuscular Blockers

*Good TV and RR *Resp. smooth and unlabored *Opens eyes widely *Sustained protrusion and purposeful movement of tongue *Swallows effectively *Head lift for 5 seconds *Strong/constant hand grip *effective cough *VC of 15mml/kg *Inspiratory force of 25-30cm H2O *Sustained tet response to 50Hz for 5 sec *TOFR >0.9 w/o fade *No fade to double burst stimulation (DBS)

G-proteins: The α subunit may be "Stimulatory" or "Inhibitory"...

*Gsα stimulates adenylate cyclase and increases cyclic AMP production *Giα decreases cyclic AMP production.

AMITRIPTYLINE (Elavil): HL

*HL: 22 hrs (26 hr for active metabolite, nortriptyline)

NALBUPHINE (Nubain): Half-life

*HL: 3 hrs

CATAPRES (Clonidine): Indications

*HTN *Preoperative sedation and anxiolysis *Tx of diarrhea in diabetics *Differential Dx in pheochromocytoma *Treating and preparing addicted subjects for withdrawal from narcotics, alcohol, and tobacco *Additive for prolongation of regional anesthesia *Other off-label uses are: -Atrial fibrillation -ADHD -Constitutional growth delay in children -Cyclosporine-associated nephrotoxicity -Tourette's syndrome -Hyperhidrosis -Mania -Posthepatic neuralgia -Psychosis -Restless leg syndrome -Ulcerative colitis -Allergy-induced inflammatory reactions in patients with extrinsic asthma

KETOROLAC (Toradol): Metabolism

*Hepatic *Metabolized principally by glucuronic acid conjugation. *Renal excretion (40% as metabolites and 60% unchanged)

HYDROMORPHONE (Dilaudid): Metabolism

*Hepatic *Metabolized to Hydromorphone-3-Glucoronide which is potentially neurotoxic in high doses (may accumulate in renal failure)=dose not have any analgesic properties *Renal excretion

MEPERIDINE (Demerol): Metabolism

*Hepatic 90% *Hydrolyzed to meperidinic acid, which in turn is partially conjugated. *Also N-demethylated to normeperidine, which then may be hydrolyzed to normeperidinic acid and subsequently conjugated. *Active metabolite normeperidine (which has HL of 15-20hrs) *First pass pulmonary uptake exceeds 65% of first dose *Excreted in urine

MEPIVICAINE (Carbocaine, Polocaine): Metabolism

*Hepatic Metabolism *Renal excretion

PRILOCAINE (Citanest): Metabolism

*Hepatic Metabolism *Renal excretion

METHOHEXITAL SODIUM (Brevital): Metabolism

*Hepatic Metabolism *Renal excretion of inactive metabolites

ACETAMINOPHEN (Tylenol): Metabolism

*Hepatic Metabolism (>90%) *3 metabolic pathways are notable: *Glucuronidation in 40-66% *Sulfation (sulfate conjugation) in 20-40% *N-hydroxylation and rearrangement, then GSH conjugation, accounts for less than 15%. P450 (CYP2E1, CYP1A2 & CYP2D6) metabolism forms a minor yet significant alkylating metabolite known as NAPQI (N-acetyl-p-benzo-quinone imine)(also known as N-acetylimidoquinone). NAPQI is then irreversibly conjugated with the sulfhydryl groups of glutathione. *Renal Excretion

CARBAMAZEPINE (Tegretol, Equetro): Metabolism

*Hepatic P45, CYP3A4, to active epoxide form (carbamazepine-10,11 epoxide) *Excretion via Renal (70%) and Feces (30%)

IBUPROFEN (Motrin, Advil): Metabolism

*Hepatic P450, CYP2C9 *90% is metabolized to hydroxylate or carboxylate derivatives *Renal excretion of metabolites

CODEINE: Metabolism

*Hepatic P450, CYP2D6 *Metabolized in part by O-demethylation into morphine, a metabolic process mediated by the liver P450 isoform CYP2D6. *Patients who lack CYP2D6 because of deletion, frame shift, or splice mutations (approximately 10% of the Caucasian population) or whose CYP2D6 is inhibited (e.g., patients taking quinidine) do not respond normally to codeine even though they exhibit a normal response to morphine. *Effective orally d/t decreased 1st pass metabolism *Conversely, certain ethnic groups (e.g., Ethiopians) carry frequently duplicated, functional CYP2D6 genes, resulting in the ultra rapid conversion of codeine to morphine, and are thought to be particularly susceptible to the effects of codeine. *Renal Excretion **Prodrug to "Morphine" (10%) and "Hydrocodone" (1%)

AMITRIPTYLINE (Elavil): Metabolism

*Hepatic P450, CYP2D6 *Renal Excretion

OXYCODONE: Metabolism

*Hepatic P450, CYP2D6 & CYP3A *Oxidized to Oxymorphone by CYP2D6 and N-demethylated by CYP3A to norOxycodone. *Effective orally d/t decreased 1st pass metabolism *Renal (and sweat) excretion of drug and metabolites **Prodrug to "Oxymorphone"

HYDROCODONE: Metabolism

*Hepatic P450, CYP2D6 & CYP3A4 *Metabolized by CYP2D6 to Hydromorphone *A major metabolite, norhydrocodone, is predominantly formed by CYP3A4-catalyzed oxidation *Renal excretion of drug and metabolites *Prodrug to "Hydromorphone"

ALFENTANIL (Alfenta): Metabolism

*Hepatic P450, CYP3A4 *Alfentanil is metabolized predominantly by two independent pathways: -Piperidine N-dealkylation to noralfentanil -Amide N-dealkylation to N-phenylpropionamide *10% pulmonary first-pass uptake *Noralfentanil is the major metabolite recovered in urine, with < 0.5% of an administered dose of alfentanil being excreted unchanged. *Efficiency of hepatic metabolism is emphasized by clearance of about 96% of alfentanil from the plasma within 60 minutes of its administration.

SUFENTANIL (Sufenta): Metabolism

*Hepatic P450, CYP3A4 *Significant 1st pass lungs, hepatic extractions *Weak active metabolite *Excretion of metabolites in urine and feces

FENTANYL (Sublimaze): Metabolism

*Hepatic P450, CYP3A4 *n-demethylation to norfentanil *75% First pass pulmonary uptake *Excreted in urine (metabolites), less than 10% unchanged

METHADONE (Dolophine): Metabolism

*Hepatic P450, CYP3A4 as well as CYP2B6, CYP2D6, CYP1A2 & CYP2C19 *Undergoes extensive biotransformation in the liver *A substrate for the P-Glycoprotein efflux protein in intestine and brain *Bioavailability and elimination half-life of methadone is subject to substantial inter-individual variability *N-demethylation and cyclization to form pyrrolidines and pyrroline, are excreted in the urine and the bile along with small amounts of unchanged drug. *Amount of methadone excreted in the urine is increased when the urine is acidified.

LORAZEPAM (Ativan): Metabolism

*Hepatic conjugation with glucuronic acid, inactive metabolites *Renal excretion, 80% unchanged in urine *d/t less hepatic metabolism, may be safe in liver failure

KETAMINE (Ketalar): Metabolism

*Hepatic cytochrome P450 enzymes (especially CYP3A4) metabolize ketamine to norketamine by N-methylation in a perfusion-limited manner. *norketamine is 1/3 as potent as Ketamine *These products are conjugated to water-soluble glucuronide derivatives and are excreted in the urine *Renal >90%, but less than 4% unchanged

TRAMADOL (Ultram): Metabolism

*Hepatic demethylation and glucuronidation via: -CYP2D6 -CYP3A4 -Conjugation with subsequent renal excretion (90%). *The rate of formation of the active metabolite is dependent on CYP2D6 and therefore is subject to both metabolic induction and inhibition.

ROMAZICON (Flumazenil): Metabolism

*Hepatic metabolism by microsomal enzymes to inactive metabolites *Renal excretion, 90% in urine unchanged

DIAZAPAM (Valium): Metabolism

*Hepatic using an oxidative pathway of N-demethylation. The two principal metabolites of diazepam are desmethyldiazepam and oxazepam, with a lesser amount metabolized to temazepam *Renal excretion of metabolites *CYP3A4-5, CYP1A2 and CYP2C19

MORPHINE: Metabolism

*Hepatic via glucuronidation by phase II metabolism enzyme UDP-glucuronosyl transferase-2B7 (UGT2B7) *Morphine-6-glucoronide (can produce its own resp depression & analgesia) - adjust dose for renal pts *Morphine-3-glucoronide (Relatively benign, can produce CNS excitatory effects...ie. Clonus, Seizures) *Metabolites excreted in urine

MIDAZOLAM (Versed): Metabolism

*Hepatic: Extensive hydroxylation by cytochrome P-450/CYP3A4-5 to 1-hydroxymidazolam, >50% 1st pass *Affected by changes in hepatic blood flow and drugs that alter cytochrome P-450A *Renal excretion *Not altered by renal failure.

THIOPENTAL SODIUM (Pentothal): Metabolism

*Hepatic: Oxidative metabolism to hydroxythiopental and carboxylic acid in the liver *Slow metabolism related to redistribution and its high affinity for adipose tissue *30% of the dose remains in 24 hours

NALOXONE (Narcan): Metabolism

*Hepatic: metabolized in the liver primarily by conjugation with glucuronic acid to form naloxone-3-glucuronide; other metabolites are produced in small amounts. *Renal excretion

SUCCINYLCHOLINE (Anectine, Quelicin): Metabolism

*Hepatically metabolized by plasma cholinesterase (pseudocholinesterase, butyrylcholinesterase) before reaching the NMJ and renally excreted *Succinylcholine --> succinylmonocholine + choline (plasma cholinesterase) *Succinylmonocholine --> succinic acid + choline (plasma cholinesterase)

PENTAZOCINE (Talwin): Considerations

*High doses cause an increase in blood pressure and heart rate *Higher doses of pentazocine (60-90 mg) elicit dysphoric and psychotomimetic effects *Does not antagonize the respiratory depression produced by morphine *Ceiling effects for analgesia and respiratory depression are observed at doses above 50-100 mg of pentazocine

BUPIVICAINE (Marcaine, Sensorcaine): Considerations

*Highest risk for cardiotoxicity *Concentrations >0.5% contraindicated in OB *Not for Bier Blocks or trans-art Axillary blocks

MORPHINE: Considerations

*Histamine Release *Morphine-6-glucoronide (can produce its own resp depression & analgesia) - adjust dose for renal pts *Stimulates vasopressin secretion in high doses *Inhibits vasopressin secretion in low doses

ATRACURIUM BESYLATE (Tracrium): Precautions

*Histamine release- avoid in asthmatics, prone to bronchospasm *Laudanosine is a metabolite that can cause CNS excitation and CV disturbances

PHYSOSTIGMINE (Antilirium): Metabolism

*Hydrolyzed by AChE *Mainly by hydrolytic cleavage by plasma esterases *Renal excretion plays only a minor role in its elimination

How is spinal bioavailability of the opioids affected by their ionization?

*Hydrophilic drugs like morphine or dilaudid are less available than lipophilic opioids such as fentanyl or sufentanil

Two types of nonadrenergic imidazoline receptors have been identified:

*I1 receptors in brain *I2 receptors in brain, pancreas, and kidney **A number of the α2 agonists also have activity at I1 receptors.

NALOXONE (Narcan): Dose

*IV/IM/SQ/IL: 0.4-4 mg or 1-4 mcg/kg *Larger doses of 5-20 mg may be needed for specific agents *Pedi: 10 mcg/kg *Infusion:

BUPRENORPHINE (Buprenex, Subutex, Suboxone, Butrans): Dose

*IV/IM: 0.3 mg q6 hrs *SL: 0.4-0.8 mg

BUTORPHANOL (Stadol): Dose

*IV/IM: 1-4 mg q3-4 hrs

NALBUPHINE (Nubain): Dose

*IV/IM: 10 mg q3-6 hrs

PENTAZOCINE (Talwin): Dose

*IV/IM: 30 mg q3-4 hrs

PHYSOSTIGMINE (Antilirium): Dose

*IV: 0.01-0.03 mg/kg *IV: 15-60 mcg/kg for CAS (central anticholinergic syndrome)

NEOSTIGMINE (Prostigmin, Vagostigmin): Dose

*IV: 0.025-0.075 mg/kg

ROMAZICON (Flumazenil): Dose

*IV: 0.2mg (8-15mcg/kg), may repeat 0.1mg q1min to a total dose of 1mg. May give up to 3mg/hr. Consider other causes if 5mg administered w/o effect

HYDROMORPHONE (Dilaudid): Dose

*IV: 0.4-2 mg or 0.01-0.04 mg/kg

ALFENTANIL (Alfenta): Dose

*IV: 0.5-1 mg (aka. 500-1000 mcg)

EDROPHONIUM (Tensilon, Enlon): Dose

*IV: 0.5-1 mg/kg *Tensilon test: 2mg IV, followed 45 sec later by an additional 8mg if the first dose is without effect

REMIFENTANIL (Ultiva): Dose

*IV: 1 mcg/kg *Infusion: 0.05-2 mcg/kg/min

LIDOCAINE (Xylocaine): Onset

*IV: 1 min *PNB: 5 min/1-3 hrs *Epi: 5 min/1-2 hrs *SAB: <5 min/ 30-60 mins

MEPERIDINE (Demerol): Dose

*IV: 12.5-100 mg *Epidural: 25-50mcg, 5-20mg/hr *Spinal: 10mcg

MORPHINE: Dose

*IV: 2-10 mg or 0.1 mg/kg *Epidural: 2-5mg, 0.1-1mg/hr *Spinal: 0.1-0.3mg *PCA: 1mg/ml, bolus 0.5-3 mg Q5-10 min; Infusion 0.5-10 mg; LO 1-2 mg Q10-15 min

SUFENTANIL (Sufenta): Dose

*IV: 2.5-10 mcg *Induction 2.5-25 mcg *Infusion 0.1-0.5 mcg/kg/min *Epidural: 25-50mcg, 10-50mcg/hr *Spinal: 5-10mcg

FENTANYL (Sublimaze): Dose

*IV: 25-100 mcg or 0.5-2 mcg/kg *IV Induction as sole agent: 5-50 mcg/kg *Epidural: 50-100 mcg, 25-100 mcg/hr *Spinal: 10-25 mcg

KETOROLAC (Toradol): Dose

*IV: 30 mg followed by 15 mg q6hrs (60 mg/day max) -1/2 dose if >65 yrs or <50kg *Pedi: 0.5 mg/kg/day one time dose IV

PRECEDEX (Dexmedetomidine): Considerations

*If bolus administered rapidly the peripherally mediated α2B receptors will dominate prior to the centrally acting α2A receptors causing hypertension. Typical hypotensive effects occur as a result of α2A stimulation. *Significant hypotension is more likely in patients with high sympathetic tone such as diabetics, the elderly, and those with hypovolemia. *Infusions longer than 24hrs could be associated with rebound hypertension/withdrawl *Benefits include anesthesia include preoperative sedation and anxiolysis, drying of secretions (antisialagogue effects), and analgesia *Antishivering effects (α2B) *Maintains resp drive *Mimics real sleep more and any other anesthetic

CARBAMAZEPINE (Tegretol, Equetro): Class

*Iminostilbene derivative

CARBAMAZEPINE (Tegretol, Equetro): MOA

*Increases limbic GABAB receptors and has effects on inositol cycling. It has unique effects at peripheral-type benzodiazepine receptors, increases stimulatory G protein alpha subunits (Gsα), and decreases inhibitory G protein subunits (Giα). It appears to lack the effects on GSK-3 and protein kinase C possessed by lithium and valproate. It has anticholinergic, antidiuretic, and muscle relaxant properties.

ETOMIDATE (Amidate): Dose

*Induction: 0.1-0.4mg/kg

METHOHEXITAL SODIUM (Brevital): Dose

*Induction: 1-2mg/kg

KETAMINE (Ketalar): Dose

*Induction: 1-4 mg/kg IV, 4-6 mg/kg IM *Infusion: 15-45 mcg/kg/min (1-3 mg/min)

THIOPENTAL SODIUM (Pentothal): Dose

*Induction: 3-5 mg/kg

2 mechanisms underlying the potent analgesic effects of intrathecally or epidurally applied opioids:

*Inhabition of Ca2+ influx of incoming peripheral sensory neurons and the subsequent spinal release of glutamate and neuropeptides such as substance P *Open G-protein-coupled inwardly rectifying K+ (GIRK) channels and hyperpolarize the membrane

Anticholinesterase agents: mechanism of action

*Inhibiting activity of acetylcholinesterase *More ACh available at NMJ, compete for nAChRs *Actions at mAChRs -bradycarda -hypersecretion -increased intestinal tone

IBUPROFEN (Motrin, Advil): Considerations

*Inhibition of platelet production & aggregation *Bronchospasm in pts with nasal polyps, asthma, & ASA sensitivity (sampter's triad) *Renal toxicity *GI upset

KETOROLAC (Toradol): Considerations

*Inhibition of platelet production & aggregation *Bronchospasm in pts with nasal polyps, asthma, & ASA sensitivity (sampter's triad) *Renal toxicity *GI upset

GABAPENTIN (Neurontin): Dose

*Initial dose: 300 mg PO on day 1, 300 mg PO twice a day on day 2, then 300 mg PO 3 times a day on day 3 *Dose may be titrated up as needed for pain relief to a daily dose of 1800 mg. *Maintenance dose: 900-1800 mg PO in 3 divided doses...up to 3600mg per day may occur

What is the downside to adding bicarbonate sodium to local anesthetics?

*It reduces the onset but can induce hypotension during the administration of epidural anesthesia

What is the onset for local anesthetic toxicity?

*It varies *If under 60 seconds, it implies intravascular injection *If 60-300 seconds, it implies partial intravascular - but can occur up to 30 minutes after injection

Local Anesthetic MOA:

*LA blocks voltage gated NA+ channels. The unionized form of the LA diffuses through the nerve axon into the axolemma. A lower pH inside the neuron/axolemma causes nonionized portion to split into ionized/unionized portions; the ionized portion binds to a receptor on the sodium channel when the channel is in the inactivated state. When the sodium channel is inactivated, action potentials cannot be generated. *2-3 nodes of Ranvier must be blocked to stop nerve conduction *Conduction block is frequency dependent=>the greater the frequency of action potentials, the faster the nerve is blocked by LA and LA must attach to sodium channel when it is in the inactivated/closed (yet open)/absolute refractory state, thus the faster the nerve fires, the more opportunities for LA to catch the sodium channel in inactivated state and sensory fibers fire at greater frequency than motor fibers thus more likely to be blocked; both unionized and ionized forms of the LA are required for conduction block. *Local anesthetics, once bound to the inside of the voltage-gated sodium channel, stabilize and prolong the duration of the inactivated state, thus inhibiting VGSC opening during further depolarization. This inhibits neuronal conduction.

CISATRACURIUM BESYLATE (Nimbex): Precautions

*Laudanosine is a metabolite that can cause CNS excitation and CV disturbances *Some renal elimination that can account for slightly prolonged DOA in renal failure patients

SUCCINYLCHOLINE (Anectine, Quelicin): MOA

*Ligand-gated ion channel *nAChR Agonist (α-subunit) *mAChR Agonist in subsequent doses and in children *Only depolarizing neuromuscular blocking agent **Phase I Block: Binds to the 2 alpha subunits of the post-synaptic nAchR, causing an opening in the center of the rosette and allowing entrance of sodium ions and exit of potassium ions, causing depolarization of the post-junctional membrane at the motor endplate *Not degraded by acetylcholinesterase at the NMJ, so it will continue to bind the alpha subunits rendering the site inactive to further Ach release *Sustained depolarization causes muscle paralysis - essentially a very long refractory period *Inactivation of sodium channels in the junctional and peri-junctional areas, which prevents the propagation of the action potential *No TOF or fade observed because succinylcholine has no effect on the presynaptic receptors that release Ach **Phase II Block: After 7-10mg/kg or 30-60 min, TOF and tetanic fade become evident, indicating overdose. Neostigmine and edrophonium can antagonize this block.

VECURONIUM BROMIDE (Norcuron): MOA

*Ligand-gated ion channel *nAChR Antagonist (Predominately post-junctional, some pre-junctional) *Intermediate acting NMBA *"Competitively" antagonizes/blocks ACh from binding to the motor endplate receptors thus preventing depolarization *Binds to one of the 2 alpha subunits on the Nicotinic Ach post-synaptic receptor, preventing access to the receptor by Ach such that the receptor does not open for the transmission of sodium ions, which blocks the action potential that leads to contraction. Non-depolarizing NMB produce a characteristic TOF and tetanic fade by blocking presynaptic nicotinic Ach receptors, preventing the mobilization of more of the stored Ach vesicles. Onset of action is inversely proportional to potency. Only around 25% of Ach receptors need to be filled to initiate contraction; however, NMB agents must block around 75% of the receptors to stop the impulse so there is a wide margin of safety.

ATRACURIUM BESYLATE (Tracrium): MOA

*Ligand-gated ion channel *nAChR Antagonist (Predominately post-junctional, some pre-junctional) *Intermediate acting NMBA *"Competitively" antagonizes/blocks ACh from binding to the motor endplate receptors thus preventing depolarization *Binds to one of the 2 alpha subunits on the post-synaptic nAchRs, preventing access to the receptor by Ach such that the receptor does not open for the transmission of sodium ions, which blocks the action potential that leads to contraction. Non-depolarizing NMB produce a characteristic TOF and tetanic fade by blocking presynaptic nAchRs, preventing the mobilization of more of the stored Ach vesicles. Onset of action is inversely proportional to potency. Only around 25% of Ach receptors need to be filled to initiate contraction; however, NMB agents must block around 75% of the receptors to stop the impulse so there is a wide margin of safety.

CISATRACURIUM BESYLATE (Nimbex): MOA

*Ligand-gated ion channel *nAChR Antagonist (Predominately post-junctional, some pre-junctional) *Intermediate acting NMBA *"Competitively" antagonizes/blocks ACh from binding to the motor endplate receptors thus preventing depolarization *Binds to one of the 2 alpha subunits on the post-synaptic nAchRs, preventing access to the receptor by Ach such that the receptor does not open for the transmission of sodium ions, which blocks the action potential that leads to contraction. Non-depolarizing NMB produce a characteristic TOF and tetanic fade by blocking presynaptic nAchRs, preventing the mobilization of more of the stored Ach vesicles. Onset of action is inversely proportional to potency. Only around 25% of Ach receptors need to be filled to initiate contraction; however, NMB agents must block around 75% of the receptors to stop the impulse so there is a wide margin of safety.

ROCURONIUM (Zemuron): MOA

*Ligand-gated ion channel *nAChR Antagonist (Predominately post-junctional, some pre-junctional) *mAChR Agonist minimally in cardiac muscle *Intermediate acting NMBA *"Competitively" antagonizes/blocks ACh from binding to the motor endplate receptors thus preventing depolarization *Binds to one of the 2 alpha subunits on the post-synaptic nAchRs, preventing access to the receptor by Ach such that the receptor does not open for the transmission of sodium ions, which blocks the action potential that leads to contraction. Non-depolarizing NMB produce a characteristic TOF and tetanic fade by blocking presynaptic nAchRs, preventing the mobilization of more of the stored Ach vesicles. Onset of action is inversely proportional to potency. Only around 25% of Ach receptors need to be filled to initiate contraction; however, NMB agents must block around 75% of the receptors to stop the impulse so there is a wide margin of safety. *Rapid onset of action similar to succyncholine, but longer duration of action

PANCURONIUM BROMIDE (Pavulon): MOA

*Ligand-gated ion channel *nAChR Antagonist (Predominately post-junctional, some pre-junctional) *mAChR Agonist modestly in cardiac muscle *Long acting NMBA *"Competitively" antagonizes/blocks ACh from binding to the motor endplate receptors thus preventing depolarization *Binds to one of the 2 alpha subunits on the post-synaptic nAchRs, preventing access to the receptor by Ach such that the receptor does not open for the transmission of sodium ions, which blocks the action potential that leads to contraction. Non-depolarizing NMB produce a characteristic TOF and tetanic fade by blocking presynaptic nAchRs, preventing the mobilization of more of the stored Ach vesicles. Onset of action is inversely proportional to potency. Only around 25% of Ach receptors need to be filled to initiate contraction; however, NMB agents must block around 75% of the receptors to stop the impulse so there is a wide margin of safety.

KETAMINE (Ketalar): MOA

*Ligand-gated ion channels *G-protein coupled receptors *NMDA Receptor Antagonist *GABAA Receptor Agonist (weak) *nAChR Antagonist *mAChR Antagonist *Na+ Channel Blocker *µ-opioid Receptor Antagonist *κ-opioid Receptor Agonist *5-HT Receptor Agonist *Monoaminergic Receptors (antinociceptive action may involve descending inhibitory monoaminergic pain pathways). *Depresses function in the cortex and thalamus, while stimulating the limbic system *Produces a functional dissociation between the thalamocortical and limbic systems, a state termed "dissociative anesthesia." *NMDAR antagonism prevents central sensitization and tolerance *mAChR antagonism causes salivation & lacrimation *Depresses transmission in the reticular formation, which affects the affective component of pain

METHOHEXITAL SODIUM (Brevital): MOA

*Ligand-gated ion channels *GABAA Agonist (δ and β subunits are possible sites of action) *AMPA Antagonist *Kainate Antagonist *nAChR Antagonist *Binds to the barbiturate receptor on the GABAA complex and at low concentrations, it enhances the effects of GABA at the GABAA complex *Decreases the rate of dissociation of GABA from the complex and increases the duration of GABA activated chloride channels *Net effect is hyper-polarization of the cell membrane and an increased threshold of excitability *At higher concentration, it directly stimulates the GABAA receptor complex, resulting in barbiturate anesthesia *Depression of the RAS

THIOPENTAL SODIUM (Pentothal): MOA

PROPOFOL (Diprivan): MOA

*Ligand-gated ion channels *GABAA Receptor Agonist *Glycine Receptor Agonist *NMDA Receptor Antagonist *AMPA Receptor Antagonist *5-HT Receptor Antagonist *GABAA-binds to β subunit, though there is now evidence that α, β, and γ subunits all contribute to GABAA sensitivity to propofol *Binds to the B subunit of the GABAA receptor, enhancing GABA induced chloride currents, inhibiting Ach release in the hippocampus and pre-frontal cortex and hyper-polarizing the cell *Decreases the rate of dissociation of GABA from the GABAA receptor *Possesses ion-channel blocking effects at the cerebral cortex and at the nicotinic Ach receptors *May inhibit NMDA glutamate receptors through modulation of channel gating

DIAZAPAM (Valium): MOA

*Ligand-gated ion channels *GABAA Receptor Agonist (Indirect) *Benzodiazepines do not activate the GABAA receptors by themselves; rather, they promote the binding of the major inhibitory neurotransmitter γ-aminobutyric acid (GABA) to the GABAA subtype of GABA receptors. *Believed to bind at the interface between α and γ subunits

LORAZEPAM (Ativan): MOA

MIDAZOLAM (Versed): MOA

ETOMIDATE (Amidate): MOA

*Ligand-gated ion channels *GABAA Receptor Agonist (β1 subunit) *Glycine Receptor Agonist *2PK Receptor Agonist *Of all of the clinically used intravenous anesthetics, etomidate exhibits the greatest selectivity for GABAA receptors and has the fewest relevant interactions with other ion channels *Binds to the B subunit of the GABAA receptor, enhancing GABA induced chloride currents, inhibiting Ach release in the hippocampus and pre-frontal cortex and hyper-polarizing the cell *Decreases the rate of dissociation of GABA from the GABAA receptor *Possesses ion-channel blocking effects at the cerebral cortex and at the nicotinic Ach receptors

ROMAZICON (Flumazenil): MOA

*Ligand-gated ion channels *GABAA Receptor Antagonist (Indirect) *Competitive antagonist *Reverses "all" the agonist effects of benzodiazepines in a dose dependent manner *Minimal agonist activity

NEOSTIGMINE (Prostigmin, Vagostigmin): MOA

*Ligand-gated ion channels (for nAChRs) *G-protein coupled receptors (for mAChRs) *nAChR Agonist *mAChR Agonist (effects are prominent) *Primary actions are post-synaptic *Produce "reversible" inhibition of acetylcholinesterase by forming a carbamyl ester complex at the esteratic site of ACh

EDROPHONIUM (Tensilon, Enlon): MOA

*Ligand-gated ion channels (for nAChRs) *G-protein coupled receptors (for mAChRs) *nAChR Agonist *mAChR Agonist (least of of all the anticholinesterases) *Primary actions are presynaptic *Produces "reversible" inhibition of acetylcholinesterase by electrostatic attachment to the anionic site and hydrogen bonding at the esteratic site of the enzyme.

PHYSOSTIGMINE (Antilirium): MOA

*Ligand-gated ion channels (for nAChRs) *G-protein coupled receptors (for mAChRs) *nAChR Agonist *mAChR Agonist (peripheral effects are prominent) *Primary actions are post-synaptic *Produce "reversible" inhibition of acetylcholinesterase by forming a carbamyl ester complex at the esteratic site of ACh *Only anticholinesterase that crosses the blood brain barrier (because the quaternary amine is replaced by a smaller tertiary amine), causes increase in central ACh levels

PYRIDOSTIGMINE (Mestinon, Regonol): MOA

*Ligand-gated ion channels (for nAChRs) *G-protein coupled receptors (for mAChRs) *nAChR Agonist *mAChR Agonist (prominent, yet less than neostigmine) *Primary actions are post-synaptic *Produce "reversible" inhibition of acetylcholinesterase by forming a carbamyl ester complex at the esteratic site of ACh

NALBUPHINE (Nubain): Metabolism

*Liver

PENTAZOCINE (Talwin): Metabolism

*Liver

BUTORPHANOL (Stadol): Metabolism

*Liver *Renal excretion (75%)

PRECEDEX (Dexmedetomidine): Dose

*Loading: 0.5-1 mcg/kg over 10 min *Infusion: 0.2-0.7 mcg/kg/hr, may use as high as 0.1 mcg/kg/hr

EMLA Cream: Class

*Local Anesthetic

ARTICAINE (Septocaine): Class

*Local Anesthetic *Aminoamide

LIDOCAINE (Xylocaine): Class

*Local Anesthetic *Aminoamide

PRILOCAINE (Citanest): Class

*Local Anesthetic *Aminoamide

BUPIVICAINE (Marcaine, Sensorcaine): Class

*Local Anesthetic *Aminoamide -pipecoloxylidide

MEPIVICAINE (Carbocaine, Polocaine): Class

*Local Anesthetic *Aminoamide -pipecoloxylidide

ROPIVICAINE (Naropin): Class

*Local Anesthetic *Aminoamide -pipecoloxylidide

BENZOCAINE (Anbesol, Cepacol, Lanacane): Class

*Local Anesthetic *Aminoester

CHLOROPROCAINE (Nesacaine): Class

*Local Anesthetic *Aminoester

PROCAINE (Novocaine): Class

*Local Anesthetic *Aminoester

TETRACAINE (Pontocaine): Class

*Local Anesthetic *Aminoester

COCAINE: Class

*Local Anesthetic *Aminoester -ester of benzoic acid,

BENZOCAINE (Anbesol, Cepacol, Lanacane, Hurricaine): Class

*Local Anesthetic *Aminoester -the ethyl ester of p-aminobenzoic acid (PABA)

The respiratory depression associated with local anesthetic overdose results in hypoxia and acidosis - what are the CNS implications?

*Local anesthetic accumulation in the fetal circulation is enhanced by the fact that fetal pH is lower than maternal pH. This may result in high fetal levels of local anesthetics

PRECEDEX (Dexmedetomidine): Indications

*MAC anesthetic cases *Adjunct to GA when cardiovascular stability decreased analgesics are desired

KETAMINE (Ketalar): Indications

*MAC anesthetics *GA induction when adrenergic stability or bronchodilation are desired *Chronic Pain *Depression *Bi-polar disorder

MEPERIDINE (Demerol): Contraindications

*MAOI's or within 14 days of use

CHLOROPROCAINE (Nesacaine): Max Dose

*MAX DOSE: 14mg/kg *PNB: 10 mg/kg *EPI: 10 mg/kg

TETRACAINE (Pontocaine): Dose

*MAX DOSE: 1mg/kg

MEPIVICAINE (Carbocaine, Polocaine): Dose

*MAX DOSE: 7mg/kg *PNB: 5 mg/kg *Epi: 5 mg/kg *SAB: 1.5 mg/kg

PRILOCAINE (Citanest): Dose

*MAX DOSE: 8.5mg/kg

TRAMADOL (Ultram): Precautions

*May cause Serotonin Syndrome in pts taking TCA's or SSRI's *Can lower seizure threshold

METHOHEXITAL SODIUM (Brevital): Considerations

*May induce ALA synthetase activity precipitating an acute porphyria attack *Can increase ictal activity, and seizures have been described in patients who received doses sufficient to produce burst suppression of the EEG. This property makes it a good choice for anesthesia in patients who undergo electroconvulsive therapy.

KETAMINE (Ketalar): Contraindications/Precautions

*May induce ALA synthetase activity precipitating an acute porphyria attack *Co-administration with Theophylline will cause seizures *Gluacoma (increases IOP) *Pts who require stable ICP. It increases ICP, CMRO2, CBF, and brain metabolism R/T cerebral vasodilation and sympathimimetic qualities *Pt with ischemic heart disease or who can't tolerate increased myocardial oxygen demand *Pts w/ psychiatric disorders

MIDAZOLAM (Versed): Precautions/Adverse Reactions

*May induce ALA synthetase activity precipitating an acute porphyria attack *HOTN *Tachycardia *Vasovagal *PVCs *Bronchospasms *Laryngospasm *Respiratory depression *Apnea *Euphoria *Delirium *Prolonged emergence *N/V *Salivation *Rash *Puritus, *Pain at injection site.

PROPOFOL (Diprivan): Contraindications/Precautions

*May induce ALA synthetase activity precipitating an acute porphyria attack *Hypersensitivity/allergy to propofol or its components, egg, soybean, soy products *Allergies related to phenyl nucleus and diisoprpyl side chain *Sodium sulfite preparation may cause anaphylaxis *Caution in people with multiple drug allergies *Pt's who can not sustain a large drop in BP *Does not release histamine- only barbiturates do!

ETOMIDATE (Amidate): ETOMIDATE (Amidate): Contraindications/Precautions

*May induce ALA synthetase activity precipitating an acute porphyria attack *Relative contraindications for pts with adrenal insufficiency. *Suppresses adrenal steroid synthesis after a single dose up to 8 hours by inhibiting 11-B hydroxylase, which inhibits ascorbic acid re-synthesis that is necessary for corticosteroid and mineralocorticoid production. The effect is usually very short lived and studies indicate it is not clinically significant, though it should probably be avoided in at risk patients *Avoid in focal epilepsy as it may stimulate seizure activity.

THIOPENTAL SODIUM (Pentothal): Contraindications/Precautions

*May induce ALA synthetase activity precipitating an acute porphyria attack *Respiratory obstruction or an inadequate airway *Severe cardiovascular instability or shock *Status asthmaticus *Porphyria may be precipitated or acute attacks may be accentuated by the administration of thiopental. This is a disorder of the metabolism of the heme precurors, which are toxic when they accumulate. The urine may turn black, HTN, renal dysfunction. Give pre-op versed and hydrate *Hepatic Failure *Intra-arterial injections is BAD - it will vasoconstrict the arteries and causes vasospasm and pain down the arm, blanching of skin with loss of distal pulses, and gangrene. It must be diluted with saline ASAP and treated w/ papaverine (40-80mcg), phentolamine (alpha 1, 2 blocker), lidocaine and heparinization and brachial plexus block

MEPIVICAINE (Carbocaine, Polocaine): Considerations

*May induce ALA synthetase activity resulting in acute porphyria attack *Not used in OB *Lacks vasodilator properties

ROMAZICON (Flumazenil): Considerations

*May precipitate seizures in benzo dependent patients *Caution in concurrent TCA overdose

How does preeclampsia change the accumulation of local anesthetics?

*May result in a greater accumulation of the drug

ACETAMINOPHEN (Tylenol): Considerations

*Metabolite p-aminophenol=nephrotoic *Acetlylcysteine=antioxidant scavenger for OD *Analgesic ceiling at 1000 mg *Contra/Caution in Hepatic disease *May potentiate coumadin

Amides: Metabolism

*Metabolized in the liver by enzymes. A significant blood level may develop.

ETOMIDATE (Amidate): Metabolism

*Metabolized in the liver primarily by hepatic microsomal enzymes and plasma esterases into the corresponding carboxylic acid (ester hydrolysis). *Main metabolite is inactive *Excreted by the kidneys (80%) and Biliary (20%)

Dual opioid and NMDA receptor antagonists:

*Methadone *Dextropropoxyphene *Tramadol *Kratom alkaloids

BENZOCAINE (Anbesol, Cepacol, Lanacane, Hurricaine): Considerations

*Methemoglobinemia

EMLA Cream: Considerations

*Methemoglobinemia

AMITRIPTYLINE (Elavil): Indications

*Migraine prophylaxis *Neuropathic pain disorders *Fibromyalgia *Vulvodynia *Nocturnal enuresis *IBS *ADHD *Pseudobulbar affect *Insomnia *Cyclic vomiting syndrome *Tinnitus *Chronic cough *Interstitial cystitis *Preventive for pts w/ recurring biliary dyskinesia (sphincter of Oddi dysfunction)

Benzylisoquinoliniums

*Mivacurium *cis-atracurium *Atricurium

ROPIVICAINE (Naropin): Considerations

*More motor sparing than Bupivacaine *Less cardiotoxic than Bupivicaine *S Enantiomer *Favored in OB as "walking" epidurals

TETRACAINE (Pontocaine): Considerations

*Most potent *Most Toxic ester LA *No IV injection *Max topical 100 mg *Avoided for PNB

Aα Fiber: Function

*Motor

Aγ Fiber: Function

*Muscle tone

Events associated with up-regulation of nAChRs:

*Myasthenia Gravis *Anticholinesterase overdose *Organophosphate overdose

There are three known mammalian tachykinin receptors termed:

*NK1 *NK2 *NK3

KETOROLAC (Toradol): Class

*NSAID -heteroaryl acetic acid derivative

IBUPROFEN (Motrin, Advil): Class

*NSAID -propionic acid class

PAPAVERINE: Class

*Naturally Occurring Opium Alkaloid (Benzylisoquinoline derivative)

CODEINE: Class

*Naturally Occurring Opium Alkaloid (Phenanthrene Derivative)

MORPHINE: Class

*Naturally Occurring Opium Alkaloid (Phenanthrene Derivative)

GABAPENTIN (Neurontin): Indications

*Neuropathic pain *Epilepsy

REMIFENTANIL (Ultiva): Metabolism

*Non specific plasma esterases (not prolonged in cholinesterase deficiency) *Excreted in urine

PANCURONIUM BROMIDE (Pavulon): Class

*Nondepolarizing Agent (Aminosteroid)

ROCURONIUM (Zemuron): Class

*Nondepolarizing Agent (Aminosteroid)

VECURONIUM BROMIDE (Norcuron): Class

*Nondepolarizing Agent (Aminosteroid)

ATRACURIUM BESYLATE (Tracrium): Class

*Nondepolarizing Agent (Benzylisoquinoline)

CISATRACURIUM BESYLATE (Nimbex): Class

*Nondepolarizing Agent (Benzylisoquinoline)

COCAINE: MOA

*Norepinephrine Reuptake Inhibitor *Dopamine Reuptake Inhibitor *Serotonin Reuptake Inhibitor

GABAPENTIN (Neurontin): Metabolism

*Not appreciably metabolized *Renal excretion-excreted unchanged in the urine with 10% to 23% excretion in the feces.

Acute Porphyria Attack: Treatment

*O2 *Discontinue precipitating agent *Initiate a glucose 10% infusion *Hematin (trade name Panhematin) is the drugs of choice in acute porphyria *Any sign of low blood sodium (hyponatremia) or weakness should be treated as these are signs of impending syndrome of inappropriate antidiuretic hormone (SIADH) or peripheral nervous system involvement that may be localized or severe progressing to bulbar paresis and respiratory paralysis. *Cimetidine has also been reported to be effective for acute porphyric crisis and possibly effective for long term prophylaxis *Pain should be treated as early as medically possible, due to its severity

Anticholinesterases are typically given only once spontaneous recovery of neuromuscular function has begun. Under these circumstances, recovery of neuromuscular transmission is the function of primarily two processes:

*Ongoing spontaneous recovery of neuromuscular function as the NMBA is eliminated from the neuromuscular junction *The increase in acetylcholine at the neuromuscular junction due to the effect of the anticholinesterase

COCAINE: Metabolism

*Only LA that metabolized by both liver and pseudocholinesterase *Hepatic P450, CYP3A4 *Plasma pseudocholinesterase *1% excreted unchanged in the urine *Renal metabolites are benzoylecgonine and ecgonine methyl ester

COCAINE: Considerations

*Only vasoconstrictor, *High PB *SE: HTN, Tachy, coronary vasospasm, V-fib, MI, *Caution with TCAs, EPI, ketamine& Pancuronuim

TRAMADOL (Ultram): Onset/Peak/Half-life/DOA

*Onset: 1 min *Peak: *HL: 5-7 hrs *DOA:

MORPHINE: Onset/Peak/Half-life/DOA (IV)

*Onset: 1 min *Peak: 45-90 min *HL: 2-3hrs *DOA: 4 hrs

BUPRENORPHINE (Buprenex, Subutex, Suboxone, Butrans): Onset/Peak/Half-life/DOA

*Onset: 1 min *Peak: 5 min *HL: 20-75 hrs *DOA:

ROMAZICON (Flumazenil): Onset/Half-life/DOA

*Onset: 1-2 min *HL: 1 hr *DOA: 45-90 min

ROCURONIUM (Zemuron): Onset/Peak/HL/DOA

*Onset: 1-2 min *Peak: 2 min *HL: 70 min *DOA: 30-60min

SUFENTANIL (Sufenta): Onset/Peak/Half-life/DOA

*Onset: 1-3 min *Peak: 3-5 min *HL: 2-4 hrs *DOA: 30-60 min: Dose dependent

OXYCODONE: Onset/Half-life/DOA (PO)

*Onset: 15 min *HL: 4 hrs *DOA: 4 hrs

HYDROCODONE: Onset/Half-life/DOA

*Onset: 15-30 min *HL: 4-6 hrs *DOA: 4-8 hrs

IBUPROFEN (Motrin, Advil): Onset/Peak/DOA/HL

*Onset: 15-30 mins *Peak: 1-2 hrs *DOA: 4-8 hrs *HL: 2 hrs

ETOMIDATE (Amidate): Onset/Peak/Half-life/DOA

*Onset: 15-45 sec *Peak: 1 min *DHL: 2-4 min *EHL: 2-5 hr *DOA: 5-10 min

REMIFENTANIL (Ultiva): Onset/Peak/Half-life/DOA

*Onset: 1min *Peak: 1-2 min *HL: 10 min *DOA: 5-10min

NALOXONE (Narcan): Onset/Half-life/DOA

*Onset: 2 min *HL: 11 hrs *DOA: 20-60min

PENTAZOCINE (Talwin): Onset/Half-life/DOA

*Onset: 2-3mins *HL: 2-3hrs *DOA: 2-3hrs

CISATRACURIUM BESYLATE (Nimbex): Onset/Peak/HL/DOA

*Onset: 2-4 min *Peak: 5 *HL: 22 mins *DOA: 30-60min

CARBAMAZEPINE (Tegretol, Equetro): Onset/Peak/HL

*Onset: 2-4 weeks *Peak: 2-6 weeks *HL: 36 hrs

PANCURONIUM BROMIDE (Pavulon): Onset/HL/DOA

*Onset: 2-4min *HL: 130min *DOA: 60-90min

VECURONIUM BROMIDE (Norcuron): Onset/Peak/HL/DOA

*Onset: 2-4min *Peak: 5 *HL: 70min *DOA: 30-60min

ATRACURIUM BESYLATE (Tracrium): Onset/Peak/HL/DOA

*Onset: 2-4min *Peak: 5 min *HL: 20 min *DOA: 30-60min

PRECEDEX (Dexmedetomidine): Onset/Half-life/DOA

*Onset: 2-5 min *DHL: 6 mins *EHL: 2 hrs *DOA: 1-2 hrs

FENTANYL (Sublimaze): Onset/Peak/Half-life/DOA (IV)

*Onset: 2-5 min *Peak: 3-5 min *HL: 2-6hr *DOA: 30-60min

FENTANYL (Sublimaze): Onset/Half-life/DOA (Epidural)

*Onset: 20-30min *HL: 2-4hrs *DOA: 2-3hrs

THIOPENTAL SODIUM (Pentothal): Onset/Half-life/DOA

*Onset: 30 Sec *Peak: <1 min *DHL: 2-4 min *EHL: 12 hr *DOA: 5-10 min

PROPOFOL (Diprivan): Onset/Peak/Half-life/DOA

*Onset: 30 sec *Peak: 1 min *DHL: 2-4 min *EHL: 2 hr *DOA: 5-10 min

KETAMINE (Ketalar): Onset/Half-life/DOA

*Onset: 30-60 sec **Peak *1 min IV *10-15 min IM *15-30 min PO *DHL: 11-17 min *EHL: 2-3 hr *DOA: 10-15 min

METHADONE (Dolophine): Onset/Half-life/DOA (PO)

*Onset: 30-60min *HL: 15-30hrs *DOA: 6-8hrs

CODEINE: Onset/Half-life/DOA (PO)

*Onset: 30-60min *HL: 4-6hr *DOA: 2.5-3.5hr

SUCCINYLCHOLINE (Anectine, Quelicin): Onset/Peak/HL/DOA

*Onset: 30-60sec *Peak: 1 min *HL: 1-2 min *DOA: 5-10 min

PHYSOSTIGMINE (Antilirium): Onset/DOA/VD

*Onset: 5 min *DOA: 1-2 hrs *VD: 2.4 L/kg *High lipid solubility

NEOSTIGMINE (Prostigmin, Vagostigmin): Dose/Onset/Peak/HL/DOA/VD/PB

*Onset: 5 min *Peak: 10 min *HL: 75 min *DOA: 30-120 min *VD: 0.7 L/kg *PB: 20%

EMLA Cream: Onset/Peak

*Onset: 5 min *Peak: 30-45 mins

MORPHINE: Onset/Half-life/DOA (Epidural)

*Onset: 60-90min *HL: 3-5hrs *DOA: 8-24hrs

MEPERIDINE (Demerol): Onset/Peak/Half-life/DOA (IV)

*Onset: <1 min *Peak: 5-20 min *HL: 3-5 hrs *DOA: 2-4hrs

METHOHEXITAL SODIUM (Brevital): Onset/Half-life/DOA

*Onset: <1min *DHL: 5 min *EHL: 4 hr *DOA: 10-15 min

HYDROMORPHONE (Dilaudid): Onset/Half-life/DOA

*Onset: <1min *Peak: 30-60min *HL: 1-3hr *DOA: 4-5hr

EDROPHONIUM (Tensilon, Enlon): Onset/Peak/HL/DOA/VD

*Onset: <2 min *Peak: 1-5 min *HL: 110 min *DOA: 30-60 min *VD: 1.1 L/KG *Poor lipid solubility

KETOROLAC (Toradol): Onset/Peak/HL

*Onset: IV- 5 mins IM- 20 mins *Peak: 2-3 hrs *HL: 4-6 hrs

COCAINE: Onset/Peak/DOA

*Onset: IV-Immediate Intranasal- *Peak: IV- 5 mins Intranasal- 15 mins *DOA: IV-30 min after peak Intranasal- 60 mins after peak

BUTORPHANOL (Stadol): Onset/Half-life/DOA

*Onset: Immediate *HL: 2.5-3hrs *DOA: 3-4hrs

ALFENTANIL (Alfenta): Onset/Peak/Half-life/DOA

*Onset: Immediate *Peak: 5 min *HL: 1.5 hr *DOA: 1-3 hrs

BENZOCAINE (Anbesol, Cepacol, Lanacane, Hurricaine): Onset/Peak/DOA/HL

*Onset: Rapid *DOA: 30-60 mins

PRILOCAINE (Citanest): Onset/DOA

*PNB: 10 min/1-2 hrs *Spinal: 5 min *Epidural: 5-15 min

BUPIVICAINE (Marcaine, Sensorcaine): Onset/DOA

*PNB: 15 min/4-14 hrs *Epi: 10 min/2-5 hrs *SAB: 5 min/1-6 hrs

ROPIVICAINE (Naropin): Onset/DOA

*PNB: 15 min/5-8 hrs *Epi: 10 min/2-6 hrs *SAB: 5 min

BUPIVICAINE (Marcaine, Sensorcaine): Dose

*PNB: 2.5 mg/kg *Epi: 2 mg/kg *SAB: 0.3 mg/kg

ROPIVICAINE (Naropin): Dose

*PNB: 3.5 mg/kg *Epi: 3 mg/kg

MEPIVICAINE (Carbocaine, Polocaine): Onset/DOA

*PNB: 5 min/2-4 hrs *Epidural: 15 min/1-3 hrs *SAB: 10 min/1-2 hrs

CHLOROPROCAINE (Nesacaine): Onset

*PNB: 5 min/30-60 min *Epi: 5 min/30-60 min

TETRACAINE (Pontocaine): Onset/DOA

*PNB: 7-10 min/1-3 hrs *Spinal: 7-10 min

CATAPRES (Clonidine): Dose

*PO: 0.1-0.6 mg in 2-3 doses *IV: 10 mcg/kg *Shivering: 75 mcg IV

HYDROCODONE: Dose

*PO: 2.5-10 mg -normally mixed with tylenol

METHADONE (Dolophine): Dose

*PO: 20-30 mg starting dose (0.1-0.5 mg/kg) *IV: 20 mg *Epidural: 5mg, 0.3-0.5mg/hr

ACETAMINOPHEN (Tylenol): Dose

*PO: 325-650mg Q 4-6º or 15mg/kg , Max 4 gm/day *Pedi: 10-15 mg/kg q6-8 hrs *PR: 20-60 mg/kg *IV (OFIRMEV ): give over 15 minutes Adults >50 kg: 1000 mg q6 hrs or 650 mg q4 hrs, with a maximum single dose of OFIRMEV of 1000 mg, a minimum dosing interval of 4 hours, and a maximum daily dose of acetaminophen of 4000 mg per day. Adults <50 kg: 15 mg/kg q6 hrs or 12.5 mg/kg q4 hrs, with a maximum single dose of OFIRMEV of 15 mg/kg, a minimum dosing interval of 4 hours, and a maximum daily dose of acetaminophen of 75 mg/kg per day.

IBUPROFEN (Motrin, Advil): Dose

*PO: 400-800 mg QID *Pedi: 7.5-10 mg/kg QID

OXYCODONE: Dose

*PO: 5-30 mg

CODEINE: Indications

*Pain *Cough

HYDROCODONE: Indications

*Pain *Cough

HYDROMORPHONE (Dilaudid): Indications

*Pain *Epidural analgesia *PCA

MEPERIDINE (Demerol): Indications

*Pain *Epidural analgesia *PCA *Shivering/Rigors

Aδ Fiber: Function

*Pain *Temperature *Touch

C Dorsal Root Fiber: Function

*Pain *Temperature *Touch

ETOMIDATE (Amidate): Physiologic Effects

*Pain on injection (85%) due to propylene glycol solution - give in a large catheter in a large vein with fluids wide open and an analgesic *Highest incidence of nausea and vomiting among agents *May cause initial hyperventilation *Apnea usually only occurs in conjunction with opioids and benzos *Ventilatory response to carbon dioxide is diminished. Less depressant effects than thiopental *Myoclonic activity after induction mimics seizure - give opioid or versed to diminish *Decreases ICP, CBF, and cerebral metabolism R/T cerebral vasoconstriction without a decrease in MAP or CPP *Lowers plasma cortisol and depresses the immune response.

OXYCODONE: Indications

*Pain, post-operative, chronic, cancer

Aminosteroids

*Pancuronium *Vercuronium *Rocuronium

PENTAZOCINE (Talwin): MOA

*Partial Mu agonist *Weaker Mu antagonist *Kappa agonist

GABAPENTIN (Neurontin): Peak/HL

*Peak: 1.5-4 hrs *HL: 5-7 hrs

ACETAMINOPHEN (Tylenol): Peak/HL

*Peak: 30-60 mins *HL: 2 hrs

GABAA receptors have the important ability to convey two different types of inhibition within the brain:

*Phasic inhibition involves temporally and spatially precise responses to very brief, high levels of synaptic GABA *Synaptic spillover produces prolonged low levels of GABA in the extrasynaptic space that activate highly sensitive GABAA receptor subtypes, thereby producing a tonic inhibitory current.

Peripheral nerves are covered by a nerve sheath while axial nerves are encased in three layers of meninges:

*Pia matter *Arachnoid *Dura matter

PYRIDOSTIGMINE (Mestinon, Regonol): Metabolism

*Plasma Esterases *25% is metabolized by the hepatic microsomal enzyme system to 3-hydroxy-methyl pyridinium, its major metabolite, and six other minor metabolites. All of these metabolites are excreted in the urine. *Renal excretion, 75% unchanged in urine *use cautiously in renal failure

PROCAINE (Novocaine): Metabolism

*Plasma cholinesterases *Metabolite is PABA

TETRACAINE (Pontocaine): Metabolism

*Plasma cholinesterases *Metabolite is PABA

CHLOROPROCAINE (Nesacaine): Metabolism

*Plasma cholinesterases *Resulting pharmacologically inactive metabolites of chloroprocaine are 2-chloro-aminobenzoic acid and 2-diethylaminoethanol. *Metabolite is PABA

C Sympathetic Fiber: Location

*Postganglionic sympathetic

Lipid Solubility best indicates...

*Potency

PANCURONIUM BROMIDE (Pavulon): Precautions

*Potential for arrhythmias d/t release of catecholemines *Use caution w/ TCA's and Halothane *Caution in CAD and unwanted tachycardia

B Fiber: Location

*Preganglionic sympathetic

How does pregnancy affect the effects of local anesthetics?

*Pregnancy enhances their effect *Due to progesterone's effects on the susceptibility of nerves to conduction blockade and probably partly due to venous dilation

Opioids bind to presynaptic and postsynaptic receptor sites, which selectively blocks transmission of afferent nociceptive stimuli from Aδ and C fibers:

*Presynaptic effects include release of spinal adenosine, which seems to be an important mediator specific for spinally mediated analgesia, as well as inhibition of Ca2+ influx and the subsequent release of glutamate and neuropeptides (such as substance P) from primary afferent terminals *Postsynaptic effects include an increase in K+ conductance, hyperpolarizing ascending second-order projecting neurons without affecting somatosensory or motor evoked potentials

There are two necessary components of LTP:

*Presynaptic glutamate release *Postsynaptic depolarization

CATAPRES (Clonidine): Metabolism

*Primarily in Liver by glucuronidation with a small portion undergoing hydroxylation by CYP2A6. *Undergoes rapid hepatic metabolism involving conjugation, N-methylation, and hydroxylation, followed by conjugation. *Metabolites are excreted in the urine and bile

PRECEDEX (Dexmedetomidine): Metabolism

HYDROCODONE: Considerations

*Prodrug (CYP2D6) *1.5 times less potent as oxycodone

CODEINE: Considerations

*Prodrug (CYP2D6) *60% as effective as morphine.

OXYCODONE: Considerations

*Prodrug (CYP2D6) *Accumulation of metabolites during renal failure *1.5 times as potent as Hydrocodone

Using opioids in administration of neuraxial anesthesia does what exactly?

*Produces analgesia without loss of sensation or proprioception *When combined with a local anesthetic it increases block density and allows for lower doses of local anesthetic

METHADONE (Dolophine): Considerations

*Prolongs QTi (females>males)

How does the addition of epinephrine affect local anesthetics?

*Provides a marker for inadvertent intravascular injection *Decreases the rate of vascular absorption *Decreases onset time *Decreases peak concentration *Increases blockade *Increases duration of action *Increases area of blockade

All NSAIDs, including aspirin, can induce hypersensitivity reactions of two general types, both likely related to the inhibition of prostaglandin synthesis:

*Provocation of asthmatic attacks in patients with vasomotor rhinitis and nasal polyposis is likely related to inhibition of normal production of the bronchodilator PGE2. *NSAIDs also rarely induce the syndrome of urticaria and angioedema related to inhibition of prostaglandin effects that normally stabilize histamine stores in mastocytes and inhibit the inflammatory response.

What are the most common side effects of neuraxial opioid administration in obstetrics?

*Pruritus & N/V *Fetal bradycardia and maternal respiratory depression are the most serious complications

NALOXONE (Narcan): Considerations

*Pts on chronic opioid therapy *Pts with cardiovascular disease *Opioid tolerant parturients

PROPOFOL (Diprivan): Metabolism

*Rapidly metabolized in the liver by conjugation to glucuronide and sulfate --> inactive water soluble metabolites *It is excreted by the kidneys, but propofol clearance exceeds hepatic blood flow *The lungs are responsible for 30% of the uptake and first pass elmination *Rapid renal clearance of 75% in first 24 hours

METHOHEXITAL SODIUM (Brevital): Contraindications/Precautions

*Respiratory obstruction or an inadequate airway *Severe cardiovascular instability or shock *Status asthmaticus *Porphyria may be precipitated or acute attacks may be accentuated by the administration of thiopental. This is a disorder of the metabolism of the heme precurors, which are toxic when they accumulate. The urine may turn black, HTN, renal dysfunction. Give pre-op versed and hydrate *Hepatic Failure *Stimulates the release of histamine and may cause allergic rxns *Intra-arterial injections is BAD - it will vasoconstrict the arteries and causes vasospasm and pain down the arm, blanching of skin with loss of distal pulses, and gangrene. It must be diluted with saline ASAP and treated w/ papaverine (40-80mcg), phentolamine (alpha 1, 2 blocker), lidocaine and heparinization and brachial plexus block

NALOXONE (Narcan): Indications

*Reversal of Opioid induced respiratory depression *Reversal of pruritus associated with opioids *Reversal of intraoperative sphincter of oddi spasm *Drug addiction/rehab tx programs

PYRIDOSTIGMINE (Mestinon, Regonol): Indications

*Reversal of the paralysis of competitive neuromuscular blocking drugs *Atony of the smooth muscle of the intestinal tract and urinary bladder *Myasthenia gravis *Combat the effects of curariform drug toxicity *Sometimes is used to treat orthostatic hypotension *May be of benefit in chronic axonal polyneuropathy *Prescribed "off-label" for the postural tachycardia syndrome

NEOSTIGMINE (Prostigmin, Vagostigmin): Indications

*Reversal of the paralysis of competitive neuromuscular blocking drugs *Atony of the smooth muscle of the intestinal tract and urinary bladder *myasthenia gravis

EDROPHONIUM (Tensilon, Enlon): Indications

*Reversal of the paralysis of competitive neuromuscular blocking drugs *Tensilon Test: Used to differentiate myasthenia gravis from cholinergic crisis and Lambert-Eaton myasthenic syndrome

EMLA Cream: Dose

*Roughly 2.5 g of the cream applied over a 25 cm2 area of skin. *Lidocaine 2.5%/Prilocaine 2.5% *Apply 1 hr prior and no longer than 4 hrs

PROCAINE (Novocaine): Onset/DOA

*SAB: 2-5 min/30-60 min

MIDAZOLAM (Versed): Dose

*Sedation: 1.0-2.5mg IV *Induction: 0.1-0.2 mg/kg IV *Anxiolysis: 0.5-5 mg IV *0.5 mg/kg PO kids

BUTORPHANOL (Stadol): Class

*Semi-Synthetic Opioid (Phenanthrene Derivative)

HEROIN: Class

*Semisynthetic Derivative of Opium Alkaloid (Morphine Derivative)

BUPRENORPHINE (Buprenex, Subutex, Suboxone, Butrans): Class

*Semisynthetic Derivative of Opium Alkaloid (Thebaine Derivative)

OXYCODONE: Class

*Semisynthetic Derivative of Opium Alkaloid (Thebaine Derivative)

HYDROMORPHONE (Dilaudid): Class

*Semisynthetic Derivative of Opium Alkaloid -Hydrogenated ketone of Morphine Derivative

HYDROCODONE: Class

*Semisynthetic Opioid Agonist

Aδ Fiber: Location

*Sensory roots and Afferent peripheral nerves

C Dorsal Root Fiber: Location

*Sensory roots and Afferent peripheral nerves

Cationic Cys-loop Receptors (3):

*Serotonin (5-HT) *Nicotinic acetylcholine (nAChR) *Zinc-activated ion channel (ZAC)

What is the mechanism of action of local anesthetics?

*Short answer: Blocks sodium channels *Longer answer: The non-ionized portion which is lipid soluble enters the nerve, reequilibrates and the remaining ionized fraction attaches to the local anesthetic receptor on the inside of the sodium channel.

Patterns of Stimulation

*Single-twitch *Train-of -Four *Tetanic Stimulation *Post-Tetanic Count *Double-burst stimulation

C Fibers: General

*Slow/Chronic Pain *Synapse at Rexed lamina 2 & 3 (Substantia gelatinosa) *First order neurons from C-fibers release the excitatory neurotransmitter substance P (SP) which binds to NK-1 receptors on the postsynaptic membranes of second order neurons in the substantia gelatinosa

pKa best indicates...

*Speed of Onset

What does carbonation do to local anesthetics?

*Speeds the onset and intensity of action of neural blockade - CO2 readily diffuses into the nerve lowering its pH - the lipid form of anesthetic enters the nerve and becomes more ionized, increasing the concentration affecting sodium channels

Events associated with down-regulation of nAChRs:

*Spinal cord injury *CVA *Thermal injury *Prolonged immobility *Prolonged exposure to neuromuscular blocking agents *Multiple Sclerosis *GBS

What is "Tumescent Anesthesia"?

*Subcutaneous injection of dilute local anesthetic with epinephrine with doses of lidocaine from 35 to 55mg/kg which peak in 8 to 12 hours after infusion - used most commonly by plastic surgeons during liposuction. Mostly good outcomes.

Electrodes

*Surface or needle *Small conducting area of 7-8mm *Skin clean & dry *Hand held stimulators do not use electrodes or needles *For HH stimulators clean skin w/ alcohol or skin cleaner, then dry

Tetanic Stimulation

*Sustained burst of pulse at 30,50 or 100Hz *Usually held for around 5 seconds *Used to "kick start" the nerve under deep paralysis *Sustained tetnus >5 sec means <50% of receptors are occupied *Sensititive test

PENTAZOCINE (Talwin): Class

*Synthetic Agonist-Antagonist Opioid (Benzomorphan)

NALBUPHINE (Nubain): Class

*Synthetic Opioid (Morphinan)

METHADONE (Dolophine): Class

*Synthetic Opioid (Phenylheptylamine)

PROPOXYPHENE: Class

*Synthetic Opioid (Phenylheptylamine)

ALFENTANIL (Alfenta): Class