pharmacology

Question 1

When do we used sodium valproate?

Answer 1

1. epilepsy (anti convulsion)

2. bipolar disorder (acute disorders and prophylaxis): mood stabiliser

Question 2

What is the mechanism of action of sodium valproate?

Answer 2

1. weak inhibitor of neuronal voltage gated NA+: stabilises resting membrane potentials and reduces neuronal excitability
2. GABAergic: inhibits GABA transaminase (increases GABA concentration at receptor sites)

Question 3

What are the side effects of sodium valproate?

Answer 3

nausea, dyspepsia, weight gain, hepatic and renal impairment, dizziness, drowsiness, thrombocytopenia, hair loss

Question 4

What are the problems with using valproate sodium during pregnancy?

Answer 4

folate antagonist properties: inhibits the DHFR protein (enzyme used to activate folic acid and before it enters folate metabolism cycle)

Question 5

What is the mechanism of action of lithium?

Answer 5

increase GABA

Question 6

When do you use Gabapentin?

Answer 6

1. epilepsy ( anticonvulsant): usually as an add on treatment if other epileptic drugs provide inadequate control
2. Neuropathic pain
3. Migraine prophylaxis
4. GAD

Question 7

What is the mechanism of action of gabapentin?

Answer 7

reduction of axon excitability:
acts on voltage sensitive calcium channels (binds to alpha-2 delta subunits): prevents inflow of calcium which inhibits neurotransmitter release (glutamate, noradrenaline and substance P)

Question 8

What are side effects of gabapentin?

Answer 8

somnolence, dizziness, ataxia, fatigue

Question 9

When do you use tricyclic antidepressants?

Answer 9

1. moderate to severe depression (when first line SSRIs are ineffective)
   (2. anxiety)
2. neuropathic pain

Question 10

What are the side effects of tricyclic antidepressants?

Answer 10

1. antimuscarinic receptors: dry mouth & nose, constipation, urinary retention and blurred vision
2. histamine and adrenergic receptors: sedation, hypotension
3. arrhythmia,ECG changes
4. convulsions, hallucination and mania

DON’T STOP THEM SUDDENLY

Question 11

What are the mechanism of actions of tricyclic antidepressants?

Answer 11

1. inhibits presynaptic 5-HT and NA reuptake transporters: increase synaptic neurotransmitter availability (monoamine theory of depression)
2. analgesic mechanism unknown: thought to result from modulation of inhibitory systems and opioid systems in CNS

Question 12

When do you use lidocaine?

Answer 12

1. local anaesthesia

2. ventricular arrhythmias

Question 13

What is the mechanism of action of lidocaine?

Answer 13

Blockage of fast voltage-gated NA+ channels in neuronal membrane: prevents depolarisation along axon (propagation)

Question 14

What are the side effects of lidocaine?

Answer 14

• dizziness/drowsiness

- paraesthesia

Question 15

When do you use paracetamol?

Answer 15

• analgesic effects in acute and chronic pain

- reduce fever: antipyretic effects

Question 16

What is the mechanism of action of paracetamol?

Answer 16

increases pain threshold in CNS by inhibiting COX (cyclooxyrgenase)

2. reduces prostaglandin PGE2 concentration in thermoregulatory region of hypothalamus
3. COX 2 inhibition: reduces inflammation (weak anti-inflammatory)

Question 17

What are the SE of paracetamol?

Answer 17

in overdose: liver failure

Question 18

When do you use ibuprofen?

Answer 18

1. analgesia (mild to moderate pain)
2. anti-inflammatory
   (3. antipyretic)

Question 19

What is the mechanism of action of ibuprofen?

Answer 19

-inhibition of COX2: prevents prostaglandin formation from arachidonic acid
(COX2 is expressed in response to inflammatory stimuli–> causes pain)

Question 20

What are the SE of ibuprofen?

Answer 20

• -> due to COX1 inhibition:
• nausea and dyspepsia
• GI ulceration/bleeding
• risk of hypertension in chronic use
• cardiovascular event

Question 21

When do you use morphine?

Answer 21

• acute severe pain
• chronic pain
• breathlessness (in end of life care)
• acute pulmonary oedema (breathlessness and anxiety)

Question 22

What is the MOA of morphine?

Answer 22

Activation of mu receptors (G protein-coupled receptors) in CNS

• -> reduces neuronal excitability (post-synaptic opioid receptor activation causing hyper polarisation) recent and pain transmission (activation of pre-synaptic opioid receptors: reduced intracellular cAMP C°, decreased Ca ion influx and thus inhibits release of excitatory neurotransmitters)
• -> in medulla: blunt response to hypoxia and hypercapnoea (reduces rest drive and breathlessness)
• -> reduces fight or flight activity (by reducing pain, breathlessness and associated anxiety)

(also acts on GABA neurones that modulate dopamine: by inhibition GABA you are able to increase dopamine)

Question 23

What are the SE of morphine?

Answer 23

• respiratory depression (by reducing respiratory drive)
• euphoria and detachment/ neurological depression
• nausea and vomiting (activa° of chemoreceptors trigger zone)
• pupillary constriction (stimulation of E-W nucleus)
• constipation (increase smooth muscle tone and reduces motility)
• skin itching (histamine release)
• -> tolerance, dependence, withdrawal reaction

Question 24

What is co-codamol?

Answer 24

codeine and paracetamol

Question 25

When do you use co-codamol?

Answer 25

mild to moderate pain, as a second line treatment when simple analgesics are insufficient

Question 26

What is the MOA of co-codamol?

Answer 26

• mechanism of paracetamol

- metabolised by cytochrome P450 enzymes to morphine (or morphine related metabolites)

Question 27

What are the SE of co-codamol?

Answer 27

• at recommended dose, SE from paracetamol are rare

- codeine: nauseas, constipation and drowsiness

Question 28

When do you use aspirin?

Answer 28

1. acute coronary syndrome an acute ischemic stroke
2. long term secondary prevention in cardiovascular, cerebrovascular and peripheral arterial disease
3. atrial fibrillation (if warfarin and oral anticoagulants are contraindicated)
4. control mild to moderate fever and pain

Question 29

What is the MOA of aspirin?

Answer 29

Irreversible inhibition of COX to reduce production of pro-aggregators factor thromboxane from arachidonic acid, reducing platelet aggregation

Question 30

What are the SE of aspirin?

Answer 30

• gastrointestinal irritation and ulceration
• haemorrhage
• bronchospasm
• life threatening in overdose

Question 31

What type of drug is diazepam?

Answer 31

benzodiazepines

Question 32

When do you use benzodiazepines?

Answer 32

• seizures (first line)
• alcohol withdrawal reactions
• severe, disabling or distressing anxiety or insomnia (short term treatment)

Question 33

What inhibits benzodiazepines? how?

Answer 33

flumazenil

displaces diazepam from GABA receptor

Question 34

What is the MOA of benzodiazepines?

Answer 34

• positive allosteric modulator (POM): facilitate and enhance binding of GABA to GABA-A receptor (between alpha and gamma subunits): depressant effect on synaptic transmission (hyperpolarisation)
• -> effects: sleepiness, reduces anxiety, sedation and anticonvulsant effects

Question 35

What are the SE of benzodiazepines?

Answer 35

• dose dependent drowsiness, sedation and coma
• loss of airway reflexes (airway obstruction and death)
• dependence, withdrawal reaction

Question 36

Name an SSRI?

Answer 36

sertraline

Question 37

When do you use SSRIs?

Answer 37

• moderate to severe depression (first line treatment BUT only if psychological treatments fail
• panic disorders
• obsessive compulsive disorder

Question 38

What is the MOA of SSRIs?

Answer 38

inhibit neuronal re-uptake of serotonin from the synaptic cleft: increase availability for neurotransmission

Question 39

What are the SE of SSRIs?

Answer 39

• gastrointestinal upset, appetite and weight disturbance (loss or gain) an hypersensitivity reactions
• suicidal thoughts and behaviour
• -> sudden withdrawal may cause problems

Question 40

Name an SNRI

Answer 40

venlaxafine

Question 41

What does SSRI stand for?

Answer 41

selective serotonin reuptake inhibitor

Question 42

What does SNRI stand for?

Answer 42

serotonin and norepinephrine reuptake inhibitors

Question 43

When do we use SNRIs?

Answer 43

• second line treatment for MDD

- general anxiety disorder

Question 44

What is the MOA of SNRIs?

Answer 44

-serotonin and noradrenaline reuptake inhibitor (from synaptic cleft)

Question 45

What are the SE of SNRIs?

Answer 45

• gastrointestinal upset
• CNS effect (abnormal dreams, insomnia, headache, convulsion etc)
• suicidal thoughts
• -> sudden withdrawal causes big effects

Question 46

What is in co-beneldopa?

Answer 46

• levadopa (L-DOPA)
• peripheral dopa-decarboxylase inhibitor
• -> reduces conversion to dopamine outside the brain

Question 47

When do you use co-beneldopa?

Answer 47

parkinson’s disease

Question 48

What is the MOA of co-beneldopa?

Answer 48

precursor of dopamine (L-DOPA) which can cross the BBB via membrane transporters and then be converted into dopamine

Question 49

What are the SE of Co-beneldopa?

Answer 49

• nausea, drowsiness, confusion, hallucinations and hypotension
• wearing off effect
• dyskinesias (on-off effect: phases of immobility and phases of dyskinesias)

Question 50

Name a MAO-B inhibitor

Answer 50

selegiline

Question 51

what does MAO-B stand for?

Answer 51

monoamine oxidase type B

Question 52

When are MAO-B inhibitors used?

Answer 52

Parkinson’s disease

Question 53

When are MAO-A inhibitors used?

Answer 53

depression

Question 54

What is the MOA of MAO-B inhibitors?

Answer 54

inhibition of MAO-B which metabolises dopamine and phenylethylamine, increasing available dopamine
+enhances effects of L-DOPA

Question 55

What are the Se of MAO-B inhibitors?

Answer 55

• dizziness, nausea, fatigue
• possible hyper sexuality or similar behaviour (due to increased dopamine)
• can cause worsening of levodopa induced dyskinesia
• sometimes hallucinations

Question 56

Name two second generation (atypical) antipsychotic

Answer 56

clozapine and risperidone

Question 57

When do we use second generation (atypical) antipsychotics?

Answer 57

• psychomotor agitation (urgent treatment)
• schizophrenia
• bipolar disorder (in episodes of mania or hypomania)

Question 58

What are the SE of second generation (atypical) antipsychotics?

Answer 58

• sedation
• EPSE (ie Parkinsonism)
• metabolic disturbances
• arrhythmias
• agrunolocytosis

Question 59

Which nerve fibres are more sensitive to local anaesthetics?

Answer 59

small nerve fibre> large nerve fibres

myelinated fibres> non myelinated fibres

Question 60

when using an anaesthetics, which are the order of loss of nerve functions?

Answer 60

pain, temperature, touch, proprioception and finally skeletal muscle tone

Question 61

Why is ketamine used in surgery?

Answer 61

-reduces incidence of post surgical pain

Question 62

What is an adjuvant?

Answer 62

enhancing the effectiveness of medical treatment

Question 63

what are examples of adjuvants in pain management?

Answer 63

• gabapentin/pregabapentin
• SNRIs/ tryclic antidepressants
• alpha2agonists

Question 64

what is the MOA of cannabis?

Answer 64

activation of presynaptic CB1 receptors (G coupled receptors) in the hypothalamus, sustantia nigra,mesolimbic pathways and association areas of the cerebral cortex
–> causes inhibition of voltage gated Ca channels: reducing transmitter release

Question 65

when is propofol used?

How is given?

Answer 65

• hypnosis

- bolus: fast acting but short acting

Question 66

What is isoflurane used? How is given?

Answer 66

• hypnosis

- inhalant gas