L10: Benzodiazepines & Cannabinoids

Question 1

What are the 2 major compounds in marijuana?

Answer 1

Tetrahydrocannabinol (THC) and Cannabidiol (CBD).

Question 2

How can cannabinoids be used for therapy?

Answer 2

Therapeutic effects for chronic pain in adults and for chemotherapy induced nausea and vomiting.

Question 3

What receptors do cannabinoids act on?

Answer 3

CB1 and CB2

Question 4

Where in the body is CB1 found in the highest concentration? What type of receptor is it?

Answer 4

Highest concentration: in the brain

Receptor: GPCR

Question 5

What type of effects are cannabinoids responsible for when they interact with CB1?

Answer 5

Psychotropic effects. (action on CNS).

Question 6

Where in the brain can CB1 be found? What is the function of each brain area?

Answer 6

1. Basal ganglia and cerebellum: movement
2. Cerebral cortex: higher cognitive function
3. Hippocampus: learning, memory, stress
4. Medulla: nausea/vomiting, chemoreceptor trigger zone (inhibitory effect)

Question 7

Where in the body is CB2 found in the highest concentration?

Answer 7

In the immune system.

Question 8

What are the families of compounds that act on cannabinoid receptors?

Answer 8

1. Endocannabinoids
2. Phytocannabinoids
3. Synthetic cannabinoids

Question 9

What are Endocannabinoids? What are they derived from? Name 2 major compounds of Endocannabinoids.

Answer 9

What are they: Compounds made in the body (brain) that are natural ligands for the cannabinoid receptors

Derived from: arachidonic acid

Major compounds: Arachidonoylethanolamide (anandamide, AEA) and 2-arachidonoylglycerol (2-AG).

Question 10

What is arachidonic acid?

Answer 10

A constituent of the plasma membrane and is a precursor in the synthesis of many compounds, including Endocannabinoids.

Question 11

What are Phytocannabinoids derived from? Name 2 major compounds of Phytocannabinoids.

Answer 11

Derived from plants

Major compounds: THC and CBD

Question 12

What are synthetic cannabinoids? Give an example of a synthetic cannabinoid.

Answer 12

Synthetic cannabinoids are made in a pharmaceutical lab. The compounds are mimics of THC and other plant derived compounds.
Ex: Nabiolone

Question 13

What is the main pharmacodynamic mechanism of cannabinoids?

Answer 13

Retrograde signalling system: presynaptic inhibition of transmitter release.

Question 14

Explain the retrograde signalling system of cannabinoids. (F2, L10)

Answer 14

1. AEA or 2-AG are synthesized naturally from a precursor in the post-synaptic neuron and act pre-synaptically at the CB1 receptor. Feedback mechanism.
2. THC, Dronabinol, and Nabiolone can act on the pre-synaptic CB1 receptor as well.
3. Activation of the CB1 receptor on the pre-synaptic terminal decreases calcium intake and increases potassium efflux at the pre-synaptic terminal by blocking calcium channels and opening potassium channels.
4. The change in neuron potential (calcium and potassium levels) hyper-polarizes the cell which decreases the release of neurotransmitters from the pre-synaptic terminal when it receives an action potential. Ca2+ is important in the release of neurotransmitters.

Conclusion: There is less stimulation of the post-synaptic neurotransmitter receptor.

Question 15

Why are the pharmacodynamic effects of cannabinoids so effective?

Answer 15

Because cannabinoid receptors are on multiple cell types and can control the release of many transmitters.
CB1: neurons and astrocytes (regulate transmission of electrical impulses within the brain - can be between 2 neurons)
CB2: microglia (macrophage: 1st immune defense of the CNS)

Question 16

Describe the absorption of cannabinoids.

Answer 16

1. Lung: by smoking, THC gets into lungs, it is rapidly absorbed and distributed
2. Intestine: when consumed, absorption is lower than when smoked. First pass metabolism in the liver therefore the blood concentration does not elevate to high levels. However, it is readily absorbed by the intestine and the colon.
3. Skin: major compounds are lipid soluble and can cross the plasma membrane dermally.

Question 17

Describe the distribution of cannabinoids.

Answer 17

Compounds are distributed in extracellular water and can be stored in fat because they are highly lipid soluble. Some bind to serum proteins.
They can also be passed to the fetus therefore, must be avoided during pregnancy.

Question 18

Describe the metabolism of cannabinoids.

Answer 18

Leads to metabolite formation. Mainly occurs in liver.

Question 19

Describe the excretion of cannabinoids.

Answer 19

Metabolites are secreted in saliva and sweat.
Largely excreted in the urine by kidneys.
Some excreted by the small intestine into the colon: feces.

Question 20

What are the toxic effects of smoking marijuana? What are the main risks and long term effects?

Answer 20

The carcinogens inhaled are similar to smoking cigarettes because you are burning a leaf and smoking it, thus inhaling the carcinogens.
Main risks: cancers, heart attacks, strokes
Long term effects: unknown.

Question 21

Why are Cannabinoids addicting?

Answer 21

Because they act on the reward pathway in the brain.

Question 22

What is marijuana’s effect on driving?

Answer 22

Impairs driving for a minimum of 5 hours. Can be longer if consumed orally because oral absorption is slower, the effects wear off more slowly. Can also be longer depending on the dose.

Question 23

What is psychopharmacology?

Answer 23

Using drugs to treat mental diseases or disorders.

Question 24

What is different in the brain of a schizophrenic individual?

Answer 24

Increased levels of dopamine.

Question 25

What was the first effective neuroleptic (antipsychotic) drug? What does it do? What psychotic disease can it be used for? Is it selective?

Answer 25

Chlorpromazine. Can be used for schizophrenia.
Blocks D2 dopamine receptor preventing activation by dopamine. Not selective because it blocks things other than the D2 receptor like histamine receptors and 5HT receptors. this causes negative side effects.

Question 26

What drugs can increase risk of schizophrenia or schizophrenic symptoms? How?

Answer 26

Drugs: amphetamine, cocaine

Why? because they block dopamine re-uptake which increases dopamine levels above normal.

Question 27

What does the effectiveness of antipsychotic drugs (used to treat schizophrenia) correlate with?

Answer 27

Effectiveness correlates with their ability to block D2 receptors. The better they block, the more effective they are.

Question 28

What pathways do antipsychotic drugs affect?

Answer 28

1. Mesolimbic pathway (VTA to nucleus accumbens)

2. Mesocortical pathway (VTA to prefrontal cortex)

Question 29

What is the effect of increased dopamine in the mesolimbic and mesocortical pathway?

Answer 29

1. Mesolimbic: increased dopamine causes overactivation leading to delusions and hallucinations.
2. Mesocortical: increased dopamine causes dysfunction which leads to lack of emotions, intellectual impairment and defective cognitive abilities.

Question 30

What is the main effect of the D2 receptor on a neuron?

Answer 30

Mainly inhibitory.

Question 31

How have antipsychotic drugs been improving over the years?

Answer 31

Their selectivity for D2 receptors has been increasing.

Question 32

What 4 drugs can be used to treat depression? What is their main function?

Answer 32

1. Monoamine Oxidase Inhibitors (MAOIs)
2. Tricyclic antidepressants
3. Selective Serotonin Re-uptake Inhibitors (SSRIs)
4. Atypical noradrenaline 5HT re-uptake inhibitors

they mainly act on the metabolism and uptake of transmitters.

Question 33

Explain how monoamine oxidase inhibitors (MAOIs) work.

Answer 33

MOAIs block monoamine oxidase (enzyme) which are found in the pre-synaptic terminal and in the synaptic cleft. Monoamine oxidases act on metabolism by breaking down neurotransmitters (Noradrenaline, dopamine, serotonin). MAOI’s therefore increase the levels of excitatory neurotransmitters in the synapse and at post-synaptic receptors.

Question 34

Explain how tricyclic antidepressants work.

Answer 34

They interfere with the re-uptake of neurotransmitters by blocking the 5HT and the noradrenaline re-uptake transporter. Blocking leads to an increase in neurotransmitters (serotonin and noradrenaline) in the synaptic cleft and at the post-synaptic receptors.

Question 35

What are the side effects of tricyclic antidepressants? why?

Answer 35

They block adrenergic receptors, histamine receptors, and cholinergic receptors. This affects the vascular system (due to noradrenaline blockage effect on sympathetic nervous system), it produces sedation (due to block of histamine receptors), acts on GI tract and vision (due to blockage of acetylcholine receptors).

Question 36

Why are tricyclic antidepressants used despite their many side effects?

Answer 36

It is still used because more specific SSRIs (newer drugs) are not responsive in some patients. Therefore, they use older types of drugs that are less specific but still effective.

Question 37

Explain how Selective Serotonin Re-uptake Inhibitors (SSRIs) work.

Answer 37

They are more specific drugs that interfere with the re-uptake of serotonin by blocking the 5HT re-uptake transporters. They DON’T inhibit other transmitter re-uptake. Blocking leads to an increase of serotonin in the synapse and at the post-synaptic receptors.

Question 38

Where are the 5HT receptors found? What type of receptor are they?

Answer 38

Found in the smooth muscle, platelets, CNS, PNS, GI tract, blood vessels.
Most are GPCRs.

Question 39

What’s the most effective type of SSRI and why?

Answer 39

Fluoxetine (Prozac)
why? it has a high potency of inhibiting the 5HT re-uptake compared to the other antidepressants that have a lower potency of blocking the re-uptake of NA.
Overall, it has the lowest adverse side effects compared to other antidepressants due to their higher selectivity.

Question 40

What is seasonal affective disorder (SAD)? Treatment?

Answer 40

It is seasonal depression during the winter because the days have less sunlight. Treatment: exposure to light source that emits same wavelength of sun (Light box).

Question 41

What is the main drug family used to treat anxiety?

Answer 41

Benzodiazepines.

Question 42

Who are candidates for anti-anxiety drugs?

Answer 42

Those who have high levels of anxiety for natural events that occur in life or high anxiety in a short term crisis.

Question 43

What are anxiety states? How can they manifest?

Answer 43

They are various combinations of physical (ex: heart pounding, increased BP, shaking) and mental manifestations (ex: sense of dread). They are not attributable to real danger and they occur in either attacks (intermittent) or as a persistent state.

Question 44

What is panic disorder?

Answer 44

An extreme state of anxiety. People become non-functional and disoriented.

Question 45

What are some causes of anxiety?

Answer 45

1. Stress
2. Generalized anxiety disorder
3. Phobias
4. secondary anxiety disorder (the person assumes that their original anxiety is itself something dangerous)
5. Drug induced

Question 46

What are the major effects of benzodiazepines? Where?

Answer 46

1. Antianxiety (hippocampus and amygdala)
2. Induced sleep (sedative/hypnotic in cerebral cortex)
3. Anti-convulsant (cerebllum & hippocampus)
4. Muscle relaxant (spinal cord, cerebellum, and brainstem)
5. Impairs memory formation (amnesia - cerebral cortex and hippocampus)
6. Addiction potential (midbrain - dopamine)

There are many different benzodiazepine structures which allows them to be better at managing certain of these effects.

Question 47

What kind of anxiety are benzodiazepines most useful for?

Answer 47

Acute, stress related anxiety.

Question 48

Why are benzodiazepines relatively safe?

Answer 48

Because their lethal to therapeutic dose ratio is 1000.

Question 49

What was the first widely used drug for anxiety?

Answer 49

Diazepam.

Question 50

What is stage fright? What do musicians use to treat it?

Answer 50

Stage fright can cause slight tremors and palpitations which can interfere with performance. Instead of using anti-anxiety drugs, because they’re not necessarily anxious, musicians tend to use beta blockers which block beta-receptors in the autonomic nervous system to prevent palpitations.

Question 51

What receptors do benzodiazepines act on? Where are the receptors found?

Answer 51

GABA A receptors which are found everywhere in the brain.

Question 52

How do GABA receptors work? What neurotransmitter systems does it effect?

Answer 52

When GABA binds to its 2 binding sites on the receptor, the channel opens to allow influx of chloride ions. This leads to a hyperpolarizarion and an inhibitory post synaptic potential across the membrane. GABA has an inhibitor effect on many neurotransmitter systems such as 5-HT, dopamine, and noradrenaline which leads to antianxiety, sedative effects and other effects of benzodiazepines.

Question 53

What is the mechanism of benzodiazepines?

Answer 53

The benzodiazepine binding site (BZD binding site) is an allosteric binding site different from the GABA binding site. The binding facilitates the binding of the 2 GABA neurotransmitters to open the chloride channel and causes a larger chloride influx. Therefore, it increases the activity of GABA and facilitates GABAergic inhibition. BINDING BY ITSELF DOES NOTHING.

Question 54

What parts of the synapse are GABA A receptors found? Wha are they responsible for?

Answer 54

Subsynaptically and extrasynaptically.
Subsynaptic: responsible for phasic inhibition and the major site of action of banzodiazepines.
Extrasynaptic: For tonic inhibition.

Question 55

What is the first benzodiazepine?

Answer 55

Chloridiazepoxide (librium)

Question 56

Whats a commonly used benzodiazepine?

Answer 56

DIazepam (Valium)

Question 57

How do benzodiazepines affect the dose response curve of GABA? Why?

Answer 57

It shifts the curve to the left because benzodiazepines magnify the ability of GABA to open Cl- channels and hyperpolarize the cell. This leads to a higher effect at lower doses of GABA.

Question 58

What are the differences between benzodiazepines and barbiturates?

Answer 58

• Benzodiazepines affect the frequency and number of opening GABA A channels and has no direct action (needs to bind with GABA to open the Cl- channel). They’re safer and selective. They’re safer because the log dose of benzodiazepines plateau at anesthesia so it is hard to overdose.
• Barbiturates increase the duration of channel opening and act directly (DOESN’T need GABA) to increase chloride passage through the GABA A channel. They’re not as selective as benzodiazepines, and therefore less safe, an increase in dose can be lethal. Barbiturates log dose curve do not plateau therefore there is a risk of overdose.

Question 59

What are the different units of the GABA A receptor and what are they useful for?

Answer 59

1. Alpha 1 units: useful for sedation

2. Alpha 2 units: useful for anxiety

Question 60

What is a benzodiazepine antagonist? What can it be used for?

Answer 60

It’s a drug that can be used if someone is very heavily sedated by benzodiazepines. Increasing amounts can wake a person.

Question 61

What is the shift of the dose response curve of benzodiazepine agonist? antagonist? inverse agonist?

Answer 61

Agonist: to the left
antagonist: to the right
inverse agonist: even more to the right

Question 62

What are beta-carbolines? what are their effects?

Answer 62

They are inverse-agonists (blocks the agonist AND causes the opposite effect of the agonist) of benzodiazepines.
Effects: opposite of benzodiazepines- increases anxiety.

Question 63

Where do Benzodiazepines, benzodiazepine agonists, benzodiazepine antagonists and reverse agonists bind?

Answer 63

they all bind to the BZD binding site.

Question 64

What are the effects of benzodiazepine agonists, benzodiazepine antagonists and reverse agonists on the GABA A receptor (at the binding site of BZD)?

Answer 64

1. GABA alone = normal response
2. GABA + benzodiazepine agonist = increased effect of GABA
3. GABA + inverse agonist = reduced effect of GABA
4. GABA + benzodiazepine antagonist = no effect on GABA

Question 65

What is zolpidem?

Answer 65

A drug acting on GABA A receptors at a different site than benzodiazepines. It has a range of side effects.

Question 66

What can drugs that act on GABA B receptors do? where are GABA B receptors found?

Answer 66

Found in spinal cord.

Drugs can cause muscle relaxation.

Question 67

Describe the absorption of benzodiazepines?

Answer 67

1. Well absorbed orally
2. Highly lipid soluble
3. Gets to the brain quickly - quick relief
4. Peaks in 1 hour

Question 68

Describe the distribution of benzodiazepines?

Answer 68

1. Widely distributed
2. Variable protein binding
3. Rapidly enters brain

Question 69

Describe the metabolism of benzodiazepines?

Answer 69

1. Benzodiazepines are metabolized by CYP3A and CYP2C19 into intermediates.
2. Many drugs from this family have multiple active intermediates with long half-lives. It is therefore important to consider the effect of the parent drug and the intermediate drug.
3. Geriatric populations have slower metabolisms therefore the use of anti-anxiety drugs must be closely monitored for accumulation and overdose.
4. Accumulation of active metabolites can cause side effects and takes time to get back to normal.

Question 70

Describe the excretion of benzodiazepines?

Answer 70

Excreted into the urine by the kindeys.

Question 71

What is diazepam metabolized into? What is the half life of the first metabolite?

Answer 71

First metabolite: nordiazepam with a 60 hour half-life.

Nordiazepam is further metabolized into Oxazepam.

Question 72

What are the side effects of benzodiazepines?

Answer 72

1. Amnesia: Cognitive impairment, chronic high blood level
2. Sedation: do not combine with other CNS depressants
3. Muscle relaxation, ataxia: don’t drive, especially with drugs with high half life
4. Tolerance may develop; differential, pharmacodynamic tolerance
5. Dependence liability
6. Withdrawal seizures may occur

Some of the side effects are “just” side effects but some have some clinical relevance

Question 73

What is the toxicity of benzodiazepines?

Answer 73

1. When taken alone its a low toxicity

2. In combination it can be fatal especially with CNS depressants

Question 74

How can you treat overdose of benzodiazepines?

Answer 74

1. Stomach pump
2. Activated charcoal
3. Hemodialysis
4. Flumazenil: a benzodiazepine antagonist that can be used to block its adverse effects.

Question 75

What are the types of tolerance that can develop against benzodiazepines?

Answer 75

1. Differential: different targets of drugs do not develop tolerance at the same speed and to the same degree.
2. Pharmacodynamic

Question 76

What pharmacodynamic changes makes the brain tolerant to benzodiazepines?

Answer 76

Changes in re-uptake of GABA receptors.

Question 77

What are the withdrawal symptoms of taking high doses benzodiazepines for a long time?

Answer 77

Anxiety, hallucinations, loss of coordination, restless leg syndrome, more severe seizures, coma, death.

Question 78

What can be used to treat insomnia? Side effects?

Answer 78

Benzodiazepines with short half-lives. When you stop taking the drug, there may be a rebound of hyper-dreaming if you have been taking the drug for a long time. Since benzodiazepines suppresses REM sleep there is REM rebound when in withdrawal which causes people to have nightmares.

Question 79

What are non-benzodiazepine sedative hypnotics? Give an example.

Answer 79

They act on GABA A receptors. They are selective for certain subtypes of the receptor so there are fewer side effects.
Zolpidem is a non-benzodiazepine that only binds alpha 1. This treats insomnia without altering REM sleep. It binds next to the BZD site.