Pharmacology 101

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Pharmacology 101

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Title: Pharmacology 101

1
Pharmacology 101

Drugs of Abuse

2
Basic Principles

Pharmacokinetics
What your body does to the drug
Pharmacodynamics
What the drug does to your body
Psychotropic drugs
Drugs that alter neurotransmission in the brain

Tolerance
Increasing amounts of the drug are needed to
achieve desired response
Dependence/ Addiction
Psychological
Cravings
Physiological
Physiological changes associated with drug
withdrawal (e.g. delirium tremens w/ alcohol
withdrawal

3
Part 1

What the Body does to the drug why thats
important

4
Pharmacokinetics

ADME
Absorption
Drug has to be absorbed into bloodstream
Distribution
Drug has to be distributed to its target (where
it will act)
Metabolism
Not all drugs will exert action, some be
eliminated quickly-before eliminated, drug needs
to be changed (metabolized) into a form that is
easily eliminated or some drug are metabolized
into active components
Elimination
Remaining drug or parts of drug will be
eliminated via urine, feces, sweat, saliva.

5
Administration

Multiple ways to administer drugs
Orally, safest, most popular slowest
20 minutes to site of action
Intravenously, quickest most dangerous
15 seconds from arm to brain
Inhalation-very quick, potentially dangerous both
short term- (to the brain quickly) and long term
(lung disease) but necessary if treating lung
disorders-asthma
Other routes
Intramuscularly, rectally, sublingually,
topically

6
ADME Administration

Route of administration
absorption
Large tissue surface area greater absorption
Distribution
More absorbed more distributed to brain
Goal is to get Drug to brain
Most direct route w/ greatest surface area for
absorption fastest

7
Absorption Distribution

IV
Into circulation to heart to brain (15 sec)
Inhalation
Into lungs
Huge surface area for absorption
Immediate path to distribution
LungsgtHeartgtBrain
Oral
Large surface are for absorption
(stomach-intestines)
But has to go through liver first
Job of liver is to prepare substances for
elimination
Most of oral drug lost to first pass metabolism
is liver
Most doesnt get distributed to brain

8
Metabolism Elimination

Metabolism
Liver
First pass metabolism (why oral administration
not as effective as other routes)
Prepare substances to be eliminated-
biotransformation
Enzymes in liver regulate metabolism
Lots of inter-individual variation in liver
enzyme activity
CYTP450-major metabolizer
Small molecules to kidneys
Large molecules to feces or back into
distribution for another round of action
Elimination
Kidneys
Intestines

9
Why ADME is Important

Kinetic principles determine safety of drug
Safety of drug related to dose response curve
Amount of drug (dose) needed to generate a
certain response
From the dose-response curve we get the
Therapeutic Index (TI)
The greater the TI the safer the drug
Drugs with TI under 10 are considered extremely
dangerous-risk of overdose (OD) is high
Alcohol has a TI 10
LSD has a TI of gt600
No reported deaths caused solely by LSD overdose

10
Drug Safety

Therapeutic Index
LD50/ED50
Lethal Dose
Dose at which drug causes death in 50 (LD50)
Effective Dose
Dose at which drug cause response in 50 (ED50)

?TI ?risk of OD
TI at 6 death occurs at 6X normal dose

11
Elimination of Drug OD

Drugs are metabolized prior to elimination
Rate of metabolism/elimination shortens/prolongs
response to drug
Two types of metabolism
First order
Exponential based upon amount of initial dose
Zero order
Occurs at a set pace regardless of initial dose

12
Metabolism

First-order Kinetics
Each pass through the liver eliminates ½ of the
drug from the system
Each drug has a half-life t ½ -how long to get
rid of half the drug
t ½ range from seconds to days
Drugs w/ longer t ½ usually store in fat, bone or
other tissue are released slowly over time
Marijuana t ½ 20 hrs- 10 days depending upon
amount potency of initial dose
Elimination of a drug following first order
kinetics usually requires 6 passes through the
liver to be eliminated from circulation
After 4 passes though the liver 94 of drug is
eliminated

13
Metabolism

Zero order kinetics
Drugs that follow zero order kinetics metabolize
at a constant rate regardless of size of initial
dose
Risk of OD w/ large first doses
Alcohol follows zero order kinetics
Regardless of how much or how little you drink
alcohol will metabolize at a constant rate

14
Alcohol

Big dumb stupid drug-need lots to get effect
Small molecule, easily absorbed, distributes
everywhere, gets to brain quickly
Takes a lot of the drug (in comparison to other
drugs) to exert a response
Low TI high OD rate
Zero order kinetics

15
Alcohol

25-50mg of ethanol for every 100 mL of blood to
get BAC of .025-.05-to get minimal response
BAC-blood alcohol content
.08 legal limit
1 drink (6 oz of ethanol) per 50lbs of person per
hour

6 oz ethanol
1.5 oz of 80 proof liquor
proof 2X ethanol content
80 proof 45 ethanol
6 oz of wine
12 oz of beer

16
Alcohol Metabolism Binges

Distribution
1 hour to 90 of alcohol into bloodstream
B/c absorbed quickly in GI tract-minutes to brain
initial effects
Metabolized at rate of 1.5 oz of 80 proof p/hour
or 1 beer p/hour
1 drink per/50lbs per hour to get BAC of .08
Metabolizes _at_ 1 drink p/hour
How much can you have per/hour stay w/in legal
limit?
How much can you drink per/hour before you kill
yourself?
BAC _at_ .4 LD50-death in 50 of population
Alcohol poisoning-DEATH _at_ approximately 5X the
legal limit
Takes less if you dont drink, are taking other
meds and/or have other medical conditions

17
BAC
18
BAC Behavior
19
Alcohol Tolerance

Repeated use of alcohol creates tolerance to drug
cross tolerance to other drugs (sedatives)
Combining alcohol sedatives ?response ?TI
(takes less of either to kill yourself)
With tolerance it takes increasing amounts of
drug to get same response TI doesnt change
But alcohol
still metabolizes at constant rate
still has narrow TI (LD50/ ED50) 10
So as tolerance sets in use increases, risk of
OD (alcohol poisoning) becomes greater b/c one
approaches the upper limits of Lethal Dose in
order to get desired response
BAC can increase even after person has passed out
Possible to ingest fatal amount of alcohol before
passing out b/c it takes time for drug to get to
brain

20
Signs of Alcohol Poisoning

Mental confusion, stupor, coma
No response to pinching
Vomiting while asleep
Seizures
Irregular reduced breathing less than 10
breaths p/min w/ more than 10 sec between breaths
Bluish tint to skin color
Cold, clammy feel to hands

21
Chronic Alcohol Use- Side effects

Liver damage
Chronic insult ? reduced functional liver mass
and local fluid retention (ascites)
Abdominal distention

22
Side effects

Pancreatitis
Acute and chronic
Can ? diabetes
Endocrine Imbalance
Diuretic effect ? volume depletion
Fetal alcohol syndrome

23
Alcohol Genetics

Alcohol metabolism requires stomach liver
enzymes from CYT P450 family-enzymes highly
variable genetically influenced
Alcohol dehyrdogenase (stomach)
Acetaldehyde dehyrdogenase (liver)
Alcohol dehydrongenase converts alcohol into
Acetaldehyde
Another liver CYTP450 enzyme-acetaldehyde
dehydrogenase into acetic acid which is
eliminated via urine
Acetaldehyde-very toxic, induces vomiting
Many Asians lack sufficient acetaldehyde
dehydrogenase activity to fully metabolize
alcohol begin vomiting more easily
Many Indians have increased acetaldehyde
dehydrogenase dont get sick as easily
Acute high doses-binges of alcohol increase
enzyme activity
Chronic alcohol decreases enzyme activity-less
enzyme more alcohol in system longer

24
Kinetics of Other Drugs

Sedatives
Benzodiazepines (diazepam, lorazapam, alprazolam
pam lam)
High TI-difficult to OD
Extremely long t ½ b/c metabolites
(biotransformed substances are often active)
Barbiturates
Fast-asking, low TI-easy to OD
Stimulants
Amphetamine
t ½ 10hrs depending upon dose
(methamphetamine t ½ 5 hrs)
Tolerance developed quickly
TI low because of actions on heart
Cocaine
t ½ determined by route of administration
Intranasal- 75 min.
Oral- 48 min.
Rapid tolerance
TI low b/c actions on heart

Hallucinogens
LSD
Rapid tolerance
T ½ 4hrs
Tolerance averted w/ 3-4 days between dosage
Marijuana
T ½ 20hrs-10 days
Not physiologically addictive
Narcotics/opioids
Heroin
Fast-acting, 4-5hrs of action, low TI (lt10) b/c
fatally depresses HR respiration if given too
much too quickly
Rapid tolerance
ED50 5mg, LD50 40-60mg

25
Part 2

What the drug does to your body/brain

26
Pharmacodynamics

All psychotropic drugs work by altering
neurotransmission in brain
All neurotransmitters have receptors in both the
Central Peripheral Nervous Systems
So all drugs will exert action in both the
central peripheral nervous systems
Actions in the peripheral nervous system are
usually considered side-effects

27
Tolerance, Dependence Withdrawal

All Drugs of abuse involve tolerance, dependence
withdrawal to some degree or another
Tolerance need more to get the desired effect
Dependence need to maintain drug levels to
maintain functioning-offset withdrawal effects
Withdrawal opposite of desired effect
Sedatives
Desired effect-relaxation sleep
As tolerance increases need more to maintain
relaxation initiate sleep
Dependency involves preventing withdrawal effects
Withdrawal- induces anxiety insomnia

28
Peak Effects

Some point after administration, a drug exerts
its effect, the point at which the effect is
strongest is the Peak Effect
Repeated administration causes tolerance to a
drug
Tolerance delays diminishes peak effect
Tolerance requires more drug to elicit the same
peak effect

29
Sedative-Hypnotics

Sedatives-Hypnotics
GABA agonists
Decrease excitability of neurons
Reduces heart-rate respiration
parasympathomimetic
Cross tolerance w/ alcohol
Used in high doses for anesthesia
Moderate doses for sleep
Low doses for anti-anxiety (anxiolytic)
anti-depressive

30
Sedative-Hypnotics

Benzodiazepines
Moderate dependence with withdrawal symptoms
Extended t ½-active metabolites
Diazepam-Valium
Oxapam-Serax
Clorazepate-Thanxene
Lorazapam-Ativan
Prazepam-Centrax
Alprazolam-Xanax
Halazepam-Paxipam
Barbiturates
Highly addictive, short duration, rapid tolerance
Withdrawal can be life threatening
Thiobarbital-anesthestic fast acting ultra short
duration-15 minutes
Secobarbital-sleep induction, 1.5 hours duration
Pentobarbital sedative, anticonvulsant,
intermediate duration 4-6 hours

31
Dose-Response Curves-Sedatives
32
Sedative-Hypnotic Withdrawal Syndrome

First 12-15 hours, patient appears to improve
16 hours
Restless, anxious, tremulous, weak, abdominal
cramping
Vomiting, orthostatic hypotension, tremors,
increased deep tendon flexion, convulsions
Days 2-3
Delirium, hallucinations (persecutory)
disorientation to time place
Once delirium starts cant be reduced by
administration of other sedative hypnotics-has to
run its course
Includes hyperthermia (increased body temp),
exhaustion, cardiovascular collapse sometimes
death
Depending upon type of drug, withdrawal symptoms
reach peak severity at days 2-3 last upwards of
a week ( in some cases, some of the symptoms
may last several weeks)

33
Sedative-Hypnotics

Alcohol
Large dose to get effect compared to other
sedatives
Addictive
Rapid tolerance
Low therapeutic index
GABA agonist
Additive effect when taken w/ other
sedative-hypnotics
Makes cell membrane more fluid-inhibits the
movement of NA K across the membrane
Prevents action potentials
Decreases Glutamate (excitatory NT)-depresses NT
even further
Increase release of DA _at_ nucleus accumbens
-reinforcement

34
Alcohol Peak Effect vs. Peak BAC

Feel more of alcohols behavioral effects before
BAC levels reach peak concentration
This means that we begin to feel less drunk
before the alcohol has been metabolized

35
Alcohol Withdrawal

Symptoms begin 12-72 hours after last drink
Tremors
Nausea, vomiting, anxiety, sweating, abdominal
cramps, hyperreflexia, increased BP w/
orthostatic hypotension,
Hallucinations, seizures, muscle weakness,
increased body temp-sweating
Day 3
Exhaustion cardiovascular collapse
The acute alcohol abstinence is self-limiting.
If the patient does not die, recovery usually
occurs within 5-7 days.

36
Marijuana

Leaves Buds used as far back as 2737
BC-medicinally
Last 100 years- recreationally
Psychoactive component delta-9-tetrahydrocannabino
l (THC)
30 metabolites
Avg dose 20-30 mg

37
Marijuanas Psychological Affects

Impaired memory, speaking, problem-solving
Lack of motivation
Interestingly marijuana makes drivers more
cautious (not better, but more cautious)
Sedative
Increased appetite
Decrease pain

38
Marijuana Site of Action

Cannabinoid Receptors located through-out the
Cerebral cortex
Hippocampus (memory)
Hypothalamus (hunger sleep)
Amygdala (pleasure)
Endogenous cannabis- neurotransmitter anandamide
(Sanskrit word meaning internal bliss)
Variable activity on almost all other NTs

39
Marijuana Tolerance/Withdrawal

Continued use-reverse tolerance-more sensitive to
less
With 10mg p/day tolerance doesnt usually develop
Psychological not physical dependence unless
using well above the norm
Acute intoxication-increased HR conjunctival
reddening of eyes

40
Stimulants

Stimulant effect on the CNS
Three main categories
Convulsants and respiratory stimulants
Act on brain stem and spinal cord
Little to no effect on mental function
Exaggerated reflex excitability
High doses ? convulsions
Psychomotor stimulants (Amphetamines Cocaine)
Affect mental function, behavior and motor
activity
Psychomimetics (Hallucinagens)
Affect thought and perception, distort cognition
Effects resemble psychosis

41
Psychomotor stimulants

Amphetamines and Related Drugs
Amphetamine, methamphetamine, dexamphetamine,
methylphenidate, fenfluramine, Ecstasy (MDMA)
Release catecholamine, inhibit catecholamine
reuptake
Cocaine
Inhibition of catecholamine reuptake
Local anesthetic
Methylxanthines
Caffeine, theophylline
Inhibit phosphodiesterase
Adenosine type 2 receptor antagonists

42
History-Amphetamines

Amphetamines
Sympathomimetic
Synthesized in late 1800s
Medical uses in 1920s -Benzedrine
Asthma inhalers-bronchodilator
Military used Benzedrine in WWII to help soldiers
stay awake
Discovered d-isomer more potent
Developed Dexedrine
Diet pill-suppresses appetite
More modifications yielded methamphetamine
(Desoxyn, Methedrine)
Even more molecular modifications yielded
methylphenidate (Ritalin), tranylcypromine
(Parnate)
Amphetamine injected w/ heroin-speed ball- speed
(began as cocaine heroin together but as
cocaine supplies diminished, amphetamines were
substituted
Methamphetamine-smoked ice or crystal meth

43
Amphetamines

Central effects
Locomotor stimulation
Run around more
Behavioral changes
Less attention paid to surroundings
Exploratory behavior reduced
Conditioned response altered
No evidence of positive learning effects
Aggression increased
Impulse control declines
Become busier, not brighter
Improved performance in simple tasks

44
Amphetamines

Release biogenic amines
Amphetamines
NE and D most important for desired street effect
Fenfluramine
5-HT release more pronounced
Prevent reuptake
Central effects
Locomotor stimulation
Euphoria, excitement
Behavioral changes
Anorexia (especially fenfluramine)
Peripheral effects
Sympathomimetic
Increased BP, decreased GI motility

45
Amphetamines

Stereotypical Effects at high doses
Repeated actions, inappropriate to environment
Dose dependent
Repetitions increase with dose
Euphoria
With IV administration orgasmic
Confident, hyperactive, talkative, overtly
sexual, reduced fatigue (physical, mental)
Duration of Effect
Related to PK, averages 3-6 hrs
PK half-life 5 hrs to 30 hrs
Routes of administration oral, inhalation,
mucosal
Metabolism
P450 mediated

46
Amphetamines

Tolerance and dependence
Tolerance
Rapid for peripheral and anorexic effects
Slower for central effects
Dependence
No true physical dependence
Coming down unpleasant (catecholamine
depletion)
Sleep (deep, long), depression, anxiety, hunger
Insistent memory of euphoria ? psychological
dependence
Binge use drugs

47
Behavioral Effects of Amphetamines

Performance enhancer _at_ low doses, impairs
performance _at_ high doses
Increased alertness
Decreased fatigue
Decreased appetite
At high doses precipitates psychosis, stereotypic
behaviors, aggression violence
Rebound depression, suicidality upon withdrawal
Rapid tolerance BUT increased sensitivity to
psychotic effects
If use elicits psychotic behavior, each
additional use is going to be more likely rather
than less like to elicit negative reaction

48
Amphetamine Mechanisms of Action

Increases release of catecholamines DA NE by
increasing leakage of the neurotransmitters both
at rest during action potential
Inhibits reuptake (which means more has to be
produced)
Inhibits one of the enzymes that metabolize the
neurotransmitters

49
Cocaine

Sympathomimetic
Derived from coca leaf
Freud used it to treat depression
self-medicated
In wine coca cola
Local anesthesia-eyes
Derivatives-lidocaine-topical anesthetic
Rapid tolerance
Highly addictive

50
Cocaine

Forms of administration
Cocaine - HCl salt (H2O soluble)
Intravenous
With heroin (speedballs)
Nasal inhalation
Causes atrophy and necrosis of nasal septum
Crack cocaine free base
Smoked

51
Cocaine

Binges last 12 hours-several days w/ some users
re-dosing every 15 min.
Usually crash between binges
Mood elevation, perceived increase in
self-esteem, mental physical capacity
Appetite sleep are decreased
Increased sexual interest, impaired judgment,
hyperactive

Psychological Toxicity
Hyper vigilance
Paranoia
Suspiciousness
Aggressive homicidal against those perceived
persecutory
Physiological toxicity
Myocardial infarction
Arrhythmias
Seizure

52
Amphetamine/Cocaine Withdrawal

The Crash
Increased anxiety
Increased irritability
Depression
Need for sleep
Withdrawal shouldnt kill you.

53
Opioids (narcotics)

Heroin
From the seeds of the poppy plant
Metabolized into morphine
2x as strong as morphine
25X as strong as codeine
Produce action by interacting w/ opioid receptors
to activate endogenous opioids
Enkephalins
Endorphins
Dynorphins