7.9 (9.7) Adjuvant analgesics

Question 1

What is an adjuvant analgesic?

What are 3 clinical situations in which they can be used (if patient already on primary analgesic)

Answer 1

A medication with a primary indication other than pain but is useful as a coanalgesic during opioid therapy.

1. Combine with primary analgesic to enhance pain relief
2. Treat pain that is refractory to the analgesic
3. Allow reduction in the opioid dose (to limit adverse side effects)

Combine, replace, reduce

Question 2

List 4 ways to limit polypharmacy when using adjuvant analgesics

Answer 2

1. Consider adjuvant only after opioid response ascertained
2. Sequential drug trials to identify an effective drug. Initiate at low dose with gradual titration
3. Only one drug added at a time
4. Ineffective drugs should be stopped

FS:
- One drug at a time
- Sequential drug trial
- Optimize first drug before adding more drug
- Stop ineffective drugs

Question 3

List 3 conventional pain etiologies benefiting from adjuvant analgesics

Answer 3

1. Multipurpose
2. Neuropathic pain
3. Bone pain
4. For pain/other symptoms in a bowel obstruction

Question 4

Multipurpose adjuvant meds can be considered for diverse pain syndromes.

List 6 multipurpose adjuvant meds

Answer 4

1. glucocorticoids
2. alpha-2 adrenergic agonists
3. cannabinoids
4. topical therapies
5. botulinum toxin
6. neuroleptics
7. NMDA inhibitors

FS:
1. Antidepressant (SNRI, TCA)
2. Anticonvulsant (gaba, lyrica)
3. NMDA antagonist (ketamine)
4. Na channel blocker (lidocaine)
5. Alpha 2 adrenergic agonist (clonidine, demedetomodine)
6. Steroids
7. CBD

Question 5

When considering the use of an adjuvant analgesic a comprehensive assessment of the patient is required.

What are 3 elements of this assessment?

Answer 5

1. Characteristics of the pain (LOPQRST)
2. Impact of pain on function and quality of life
3. Distinguish nociceptive or neuropathic pain
4. Underlying etiology of pain
5. Presence of associated factors (ie assess for total pain), including physical and psychological symptoms, functional impairments, psychiatric disorder, family or social disruption, financial problems, and spiritual or religious concerns, and their effects on quality of life.

FS:
LOPQRSTUV
DDX
Neuropathic vs nociceptive vs total pain

Question 6

What three elements that make adjuvant analgesics less desirable than conventional analgesics such as opioids?

What is the implication of this for the use of adjuvant analgesics?

Answer 6

1. Less efficacy- smaller proportion of treated patients who respond adequately
2. Slower onset of analgesic effect (perhaps due to the need to initiate therapy at low doses to avoid side effects)
3. More SEs

Most patients with moderate or severe pain related to serious medical illness should have opioids optimized FIRST before trying an adjuvant analgesic

Question 7

What is sequential drug trial and why might this be required with adjuvant analgesia?

Answer 7

Sequential drug trials = only add 1 drug at a time, use low initial doses and gradual dose titration. Stop ineffective drugs

Why? Great patient variability in response to adjuvant analgesics and therefore inability to reliably predict the outcome of therapy

The process of sequential drug trials should be explained to the patient at the start of therapy to enhance adherence and reduce the distress that may occur as treatments fail.

Question 8

Name six classes of adjuvant analgesics? Provide an example from each class

Answer 8

Table 7.9.1

Antidepressants- TCAs, SNRIs, SSRIs

Anticonvulsants- Gabapentin, pregabalin, topiramate, carbamazepine, phenytoin, valproate, oxcarbazepine, lamotrigine, levetiracetam

Alpha-2 adrenergic agonists - Clonidine, tizanidine, dexmedetomidone

Botulinum toxin - A, B

Cannabinoids - Tetrahydrocanninol (THC), nabilone, THC:cannabidiol mixture

Corticosteroids - Dex

N-methyl-D-aspartate receptor antagonists - Dextromethorphan, ketamine

Sodium channel blockers Mexiletine, tocainide, flecainide

Topical agents - Capsaicin, lidocaine patch, EMLA®

Question 9

A. List 3 palliative symptoms for which RCTs support use of glucocorticoids.

B. A systematic review showed only weak evidence for analgesic efficacy of GCs - however clinical experience is positive. List 5 specific pain syndromes in which GCs seem helpful.

Answer 9

A. Anorexia, fatigue, nausea

B.
bone pain*
neuropathic pain*
pain from bowel/duct obstruction*
organ capsule expansion*
headache from raised ICP*
pain from lymphedema
target inflammation as 2ndary analgesia

Question 10

1. There is no data to inform choice of GC for pain. List 3 acceptable options.
2. List 4 toxicities of GC.
3. List 3 factors that increase the risk of GC associated toxicity

Answer 10

1. Dexamethasone
   Prednisone
   Methylprednisone
2. Hyperglycemia
   Myopathy
   Osteoporosis
   Psych disturbance (anxiety, psychosis)
3. Dose
   Duration of therapy
   Predisposing medical comorbidities

Question 11

Antidepressants have been used as analgesics for decades. Can be considered for any type of chronic pain.

List 2 ways mood factors into considering antidepressants as an adjuvant for pain.

Answer 11

1. Pain relief may be enhanced if there is positive mood effect
2. But analgesia does not require mood change
3. An early trial of antidepressant may be considered if comorbid depression

FS:
Improving mood = improving pain
Comorb depression

Question 12

List 1 biological mechanism for how antidepressants (SNRI) may have analgesic effects

Answer 12

Enhanced availability of monoamines at synapses within descending pain modulating neural pathways (suppress pain signal transmission)

Ie - inhibiting the reuptake of these monoamines = more availability at synapses = descending inhibitory pain pathways are reinforced

Question 13

List 2 classes of TCA’s and 1-2 examples of each

Answer 13

1. Tertiary amine drugs:
   - amitriptyline
   - imipramine
2. Secondary amine drugs:
   - desipramine
   - nortriptyline

Question 14

List 4 scenarios which warrant caution with TCA use

Answer 14

1. significant heart disease
2. risk factors for QTC prolongation
3. Cognitive impairment
4. Fall risk
5. Acute close angled glaucoma

Question 15

A patient has tolerated amitriptyline well but has only had partial relief despite the dose being at the maximum indicated for analgesic use.
* What should be done with the dose of this medication?
*What should be checked at relatively high doses?
* What type of TCA is amitriptyline and how does this differ from nortriptyline?

Answer 15

Given evidence of dose-dependent analgesic effects, it is reasonable to continue upward dose titration BEYOND usual analgesic doses in patients who fail to achieve benefit and have no limiting SEs. Note: there is no justification for increasing doses beyond the levels associated with antidepressant effects.

ECG to evaluate cardiac rhythm and QTC interval

Amitriptyline is a tertiary amine - more SEs, but better evidence for efficacy
Nortriptyline is a secondary amine - less SEs, but less evidence for efficacy

Question 16

List two clinical contraindications for TCA

Answer 16

1. narrow angle glaucoma
2. recent MI

Note: caution in elderly, medically ill, CV disorders (QTC prolongation), seizure hx

Question 17

List 4 side effects of TCAs (besides anticholinergic effects)

List 7 clinical findings of an anticholinergic toxidrome

Answer 17

Sedation, seizure, orthostatic hypotension, weight gain

Mad as hatter, blind as bat, red as beet, hot as hare, dry as bone, heart runs alone, bladder/bowel lose their tone

Question 18

1. How do SNRI’s compare with TCA’s re: side effects.
2. i) What is the evidence for SNRI’s re: analgesic effect.
   ii) Which SNRI is preferred? Name 3 SNRIs
   iii) What is the approach to dose titration?
3. Give 2 examples of oncology treatment related pain syndromes and 1 SNRI shown to be helpful in each case
4. How do SSRI’s compare with SNRI’s re: efficacy in pain

Answer 18

1. SNRI’s have more favourable side effect profile than TCA’s
2. There is high quality evidence for some SNRI’s - mainly duloxetine, venlafaxine, and desvenlafaxine.
   Duloxetine preferred given number of positive trials.
   Low starting doses overlap effective dose, so titration may or may not be needed.
   Can increase if no s/e but stop at upper end of antidepress. range
3. i) CIPN - duloxetine 30-60 mg daily (cymbalata)
   ii) Oxaliplatin induced PN - venlafaxine (Effexor)
   iii) Post mastectomy pain - venlafaxine
4. Limited evidence for a few of the SSRI’s (paroxetine, citalopram, escitalopram) therefore SNRI’s chosen when primary indication of pain

Question 19

List 4 side effects of SNRIs

Answer 19

Nausea, headache,
somnolence, tremor,
nervousness, hypertension,
dry mouth, diaphoresis,
constipation, sexual
dysfunction.

Duloxetine: dizziness, fatigue

FS: NASH (nausea, anxiety, sexy dysfunction, headache)

Question 20

List two clinical contraindications for buproprion (NDRI)

Answer 20

1. seizure disorder (eg those with anorexia/bulimia)
2. use of MAOI within 14 days (can cause hypertension and bupropion toxicity)

Question 21

List four side effects of buproprion

Answer 21

Agitation, tremor, insomnia,
nausea, decreased appetite,
weight loss, headache,
dry mouth, somnolence,
hypertension, tachycardia

FS: NASH (nausea, anxiety, sexual dysfunction - although less than SSRI/SNRI, headache)

Question 22

1. List 2 examples of alpha adrenergic agonists + available routes + indication
2. Describe their mechanism for analgesia

Answer 22

1. Overall limited evidence for their use but:

Clonidine - orally, transdermally, epidural. Epidural clonidine effective for various cancer pain*

Tizanidine - oral antispasticity agent. s/e somnolence so can try 2-4 mg hs and uptitrate for pain complicated by insomnia

Dexmedetomidine - injectable sedative/hypnotic used in ICU. Evidence for pain/delirium in advanced illness*

2. Activate monoamine-dependent endogenous pain modulating pathways in the brain and spinal cord (decrease pain transmission)

Question 23

List three side effects of clonidine (alpha-2 adrenergic agonist)

Answer 23

somnolence, hypotension (usually orthostatic), and dry mouth.

tizandine - less often hypotensive due to less alpha 1 adrenergic activity

FS: think of dexmedetomidine and icu patients

Question 24

What are three first line agents for neuropathic pain?

Answer 24

selected antidepressants (SNRIs and TCAs)
gabapentinoid anticonvulsents
in context of advanced illness corticosteroid may also be firstline

Question 25

1. What are cannabinoids?
2. Which receptors do they act on?
3. List 2 examples of synthetic cannabinoids and for each:
   - Name brand name
   - Name composition (THC vs CBD)
4. Name 2 painful clinical condition in which there is evidence their use

Answer 25

1. Cannabinoids are related to chemical constituents of cannabis
2. Bind to cannabinoid receptors

i) Nabiximols (THC 50% + cannabidiol 50%)
- Sativex
- oromucosal formulation - to spray
-complex dose-response curve (efficacy for pain at low-med doses, but not high doses)

ii) Nabilone (THC)
- Cessamet
- oral synthetic

4. spasticity in MS, opioid-refractory cancer pain

** Studies of cannabis itself also support analgesic efficacy

Question 26

List 4 side effects of pharmaceutical cannabinoids

Answer 26

1. Dizziness
2. Somnolence
3. Dry mouth
4. Psychotomimetic effects related to THC

Question 27

1. How do topical analgesics work? When should they be considered?

2.What is 1 benefit of this approach?

3. What is the evidence for topical analgesics? (List 1 example for strong, moderate, low quality evidence)

Answer 27

1. Deliver low doses of analgesic compounds directly to painful site. Consider for local or regional pains.
2. Limited systemic absorption so low risk of side effects.
3. Strong evidence:***
   Topical NSAIDS (diclofenac, ketoprofen) in acute and chronic MSK pain

Topical baclofen, amitryptiline, ketamine for CIPN (1 study)

Moderate quality evidence for limited effect:***
High [conc] Capsaicin in herpetic neuralgia

Very limited evidence for other NSAIDs, low [conc] capsaicin, lidocaine, clonidine, herbal.

Little supporting evidence for topical amitriptyline, doxepin, baclofen, ketamine, gabapentin, and menthol. No data on dose, additive effects, formulation.

(So overall, other than NSAIDS, evidence is lacking and use is derived from ++ clinical experience)***

Question 28

1. Name 4 non-cancer syndromes that may respond to botulinum toxin.
2. Botox has favourable response in cancer patients with chronic post treatment pain syndromes. List 2 limitations to its use

Answer 28

1. peripheral neuropathic pain
   plantar fasciitis
   piriformis syndrome
   post-surgical pain
   joint pain
   low back pain
   osteoarthropathy
   (No evidence in carptal tunnel, myofascial pain)
2. Cost and availabilty

FS:
migraine
TMJ pain
Esophageal spasm
Bladder spasm

Question 29

1. What is the evidence for neuroleptics in pain management?
2. List atleast 4 adverse effects of these drugs

Answer 29

1. Many randomized trials have found limited evidence of analgesic efficacy. Given risk of side effects, their primary use as analgesic is NOT supported.

Potential for analgesia could influence timing/dose of neuroleptic for other indication

e.g. Case series suggest olanzapine benefit in opioid-refractory cancer pain

2. EPS*
   somnolence*
   weight gain*
   diabetes*
   hypotension
   arrhythmia
   sexual dysfunction

FS: think olanzapine

Question 30

1. Mechanism of action of NMDA antagonists as analgesics?
2. What is the evidence for Ketamine use in non-cancer and cancer pain.
3. List 2 other NMDA antagonists (not methadone) studied with mixed results in neuropathic pain (but rarely considered for refractory pain)

Answer 30

1. Activation of the NMDA receptor is associated with peripheral and central sensitization of pain, resulting in neuronal excitation and abnormal pain manifestations (spontaneous pain, allodynia, hyperalgesia) -> blocking NMDAR (by not allowing glutamate binding) therefore decrease pain
2. Ketamine - systematic reviews in CRPS support ketamine as multipurose analgesic. Insufficient evidence in cancer pain.
3. Memantine*
   Amantadine
   Dextromethorphan*

Question 31

1. List 4 different approaches to starting and titrating Ketamine for pain control

Answer 31

1. Intranasal ketamine (but used in acute pain, need more experience to suggest in chronic pain)* (FS: 10mg intranasal Q2H PRN)
2. Burst therapy for severe pain:*
   - brief infusion, i.e. 100 mg/day, inc by 100mg/day for 3-5 days.
   - risk AE with rapid dose escalation
3. Continuous infusion protocols i.e. loading bolus 0.1-0.5 mg/kg, then 0.05-0.2 mg/kg/h. Can increase rate q few hours if still pain and no major s/e*
4. Alternative approach for infusion irrespective of weight:
   50-100 mg/day, increase by 25-50% every day
5. Oral ketamine 10-25 mg PO 3-4 times per day then titrate up until benefits or side effects*
   (Retrospective study: mean effective oral dose 2mg/kg)

Question 32

1. List 3 cognitive side effects of ketamine
2. List 2 ways to reduce the risk of side effects.

Answer 32

1. dysphoria
   dissociation
   hallucinations
2. Side effects are generally lower with subanesthetic doses, but can consider:

• co-admin of benzo or neuroleptic
• reduce opioid pre-emptively by 25-50% when initiating ketamine

FS: k hole, psychomimetic symptoms

Question 33

1. How do gabapentinoids work on pain?
2. What is the evidence for their analgesic efficacy (cancer versus non cancer pain)

Answer 33

1. Bind to alpha-2 delta site of voltage gated calcium channel -> reduce calcium influx -> decrease likelihood of depolarization –> decrease release of excitatory neurotransmitters (substance P etc) = decreased pain transmission
2. Considered multipurpose analgesics due to efficacy in pre-emptive analgesia, acute pain, neuropathic pain.

Evidence in chronically ill population for opioid refractory pain is inconclusive.

Question 34

What are 3 limitations of evidence-based guidelines for neuropathic pain published by several professional societies (i.e. NeuPSIG, NIHCE, CPS)*

Answer 34

1. Vary substantively in interpretation of the best available evidence
2. Applicability to populations with serious chronic illness unknown
3. None discuss use of glucocorticoids, important adjuvant in cancer related neuropathic pain

Question 35

What does the Canadian Pain Society list as 1st, 2nd, 3rd, and 4th line agents for neuropathic pain? Give 1 example of each

Answer 35

Table 7.9.2:

FIRST line:
gabapentin/pregabalin
SNRI
TCAs

SECOND:
tramadol
strong opioids

THIRD:
cannabinoids

FOURTH:
other opioids (methadone/tapentadol)
Botox
lacosamide
lamotrigine
lidocaine cream
lidocaine patch

Question 36

List four side effects of gabapentinoids

Answer 36

1. Sedation*
2. Delirium*
3. Nausea
4. Dry mouth*
5. Peripheral oedema*
6. Weight gain
7. Headache

SS:
NB - are not metabolized in liver
Have no known drug-drug interactions per oxford?

Question 37

1. How might patients respond to gabapentin vs. pregabalin?
2. Is one more effective or preferred over the other?
3. In the medically frail, what are appropriate starting doses for each medication?
4. What is the range of an effective dose for each?

Answer 37

1. Patients may be responders to one, both, or none.
2. 1 trial in cancer-related neuropathic pain = pregabalin superior to gabapentin but has not been replicated.

Pharmacokinetics of pregabalin supports easier/rapid titration

3. Pregabalin: 25-50 mg/day
   Gabapentin: 100-200 mg/day

Titration every few days until benefit or side effects occur

4. Pregabalin: 150-600 mg/day
   Gabapentin: 900-3600 mg/day
   (FS: 4x range)

Question 38

Is there evidence for other anticonvulsants in patients with opioid-refractory neuropathic pain that has not responded to the analgesic antidepressants and gabapentinoids?

Answer 38

1. Per Cochrane reviews, no high quality evidence that other anticonvulsants are analgesic in neuropathic pain

BUT per Oxford text, other reviews/clinical experience says to consider trial in opiod refractory neuropathic pain (??):
- carbamazepine (in trigeminal neuralgia but ++ heme toxcity)
- phenytoin, valproate (limited evidence, ++side effects)
- oxcarbazepine in peripheral neuro pain
- lacosamide, topiramate in painful diabetic neuropathy
- lamotrigine in some neuro pain but no in CIPN
- no evidence for levetiracetem
-

Question 39

1. GABA agonist - mechanism of action?
2. What evidence is there for analgesic effect of GABA agonists?
3. List 2 meds and for each 1 condition when it might be useful

Answer 39

1. GABA agonists: increase chloride ion influx -> neuron hyperpolarization -> inhibition of neuronal transmission
2. Limited evidence for their effect in pain
3. i) Clonazepam - if pain accompanied by severe anxiety
   ii) Baclofen - management of spasticity
   *** taper to avoid withdrawal seizures

Question 40

A patient is receiving a lidocaine infusion. List 3 side effects that may occur with each of the following:

1. Low (safe) blood level of lidocaine
2. Medium blood level
3. High blood level

Answer 40

Low:
1. Numbness, tingling (perioral, fingers, toes)
2. Metallic taste in mouth
3. Ringing in ears
4. Lightheaded or dizzy

Med:
1. Facial twitching
2. Nausea and vomiting
3. Decreased hearing
4. Severe dizziness

High:
1. Convulsion/seizure
2. Cardiac arrest*
3. Respiraory depression*
4. Loss of consciousness

Fs:
LoC
Seizure -> twitching -> tingling
Resp depression -> nv-> metallic taste
Cardiac arrest -> decrease hearing -> ringing

Question 41

List three contraindications to the use of ketamine as an adjuvant analgesic

Answer 41

1. Increased ICP*
2. Uncontrolled seizure
3. Hypertension*
4. Heart failure, angina or recent MI
5. Psychotic disorders*

Question 42

List four side effects associated with the use of ketamine

Answer 42

1. Sedation *
2. Sympathomimetic: Hypertension, tachycardia*
3. Psychomimetic (K hole): hallucinations, dysphoria, vivid dreams*
4. symptoms of increase ICP - nausea *
5. Tonic–clonic movements or tremor
6. Nystagmus or diplopia
7. Airway resistance
8. myocardial depression

FS: think of CIs

Question 43

List two agents with evidence for the management of trigeminal neuralgia

Answer 43

baclofen and carbamazepine

Question 44

What receptor does capsaicin act on?

What is the effect?

How must capsaicin patches be used?

FS: only last question is in 6th version of book

Answer 44

Topical capsaicin:
1. Bind to the transient-receptor-potential-vanilloid type 1 (TRPV1) receptor
2. Inhibit release of substance P and other compounds
3. Less signal to afferent C-fibers

• Low dose patch (0.075%) - apply for a week, for regional neuropathic pain and joint pain*
• High-dose capsaicin patch (8%) - apply for 30 min, for post-herpetic neuralgia* and HIV-associated painful peripheral neuropathy (duration of effect can last several months)

Question 45

List 3 ways to reduce SRE’s (skeletal-related events) in patients with multiple metastases

Answer 45

1. Conventional anti-cancer therapies
2. Bone-targeting medical therapy
3. Calcium and vit D supplements

Question 46

List 4 treatments for bone pain

Answer 46

1. Corticosteroid
2. Octeoclast inhibitors
3. Radioisotope
4. If refractory pain, concurrent trial of multipurpose analgesic reasonable, usually antidepressant, given neuropathic process in bone pain

Question 47

3 examples of osteoclast inhibitors?

Answer 47

1. Bisphosphonate - Pamidronate, ZA
2. Calcitonin
3. RANKL Inhibitor - Denosumab

Question 48

The use of bisphosphonates as adjuvant analgesics reduces skeletal-related events - what are 4 examples of this?

Answer 48

1. Bone pain
2. Pathological fractures
3. spinal cord compression
4. hypercalcaemia
5. necessity for radiation to adress impending fracture
6. Need for bone surgery

Question 49

1. How do osteoclast inhibitors work for metastatic bone pain?
2. What is the evidence for their analgesic efficacy?

Answer 49

1. Mechanism is not certain : Inhibit osteoclast -> reduce bone resorption -> reduce bone pain
2. Early studies - ZA decreases bone pain from breast, prostate, lung cancer, and multiple myeloma

2016 systematic review of bisphosphonates - reduce pain, rapid onset, relief for 1-3 months but positive effect on QOL not decomstrated

Question 50

List 2 common, 2 less common, and 2 rare side effects of bisphosphonate therapy

Answer 50

Common:
1. Transitory flu-like syndrome
2. Upper GI symptoms with oral therapy*
3. AKI (contraindicated in severe renal insufficiency) *

Less common:
1. Ocular inflammation
2. Severe MSK pain*
3. Hypocalcemia*

Rare:
With treatment for months/years: Osteonecrosis of the jaw
Atypical femur fracture

Question 51

In cancer patients, the risk of jaw pathology from bisphosphonate use is directly associated with what 3 factors:

Answer 51

• cumulative dose/duration of bisphosphonate
• comorbidities: dental pathology, diabetes
• concurrent drugs: longterm glucocorticoid therapy

Question 52

1. How does denosumab work as an osteoclast inhibitor?
2. It is said to be effective for bone pain. How does it compare to bisphosphonates re:
   i) efficacy for SRE’s
   ii) adverse effects

Answer 52

1. It is a human monocolonal antibody that binds to RANKL and prevents activation of osteoclasts -> reduce bone resorption.

i) Studies favour denosumab over bisphosphonate

ii) Denosumab more likely to cause hypocalcemia and less likely to case renal toxicity

Question 53

1. What are 2 relative contraindications for radioisotope therapy for bone pain?
2. What is the efficacy of radioisotope therapy on pain relief?
3. What is the evidence for radioisotopes vs osteoclast inhibitors in bone pain?

Answer 53

1.
i) existing bone marrow suppression (as risk of leukopenia, thrombocytopenia)
ii) Renal insufficiency

2. meaningful pain relief to 75% patients, and complete to 10-25%
3. Insufficient data to compare with osteoclast inhibitors

**Cost, complexity of treatment & risk of toxicity as above likely limits use of radioisotopes

Question 54

List three classes of drugs that are helpful as adjuvant analgesics in the setting of bowel obstruction. Give an example of a drug from each class

Answer 54

Anticholinergic drugs - theoretically relieve the symptoms of bowel obstruction by reducing propulsive and non-propulsive gut motility and decreasing intraluminal secretions - hyoscine butylbromide (buscopan) > hyoscine hydrobromide (scopolamine)

Somatostatin analogues - inhibits the secretion of gastric, pancreatic, and intestinal secretions and reduces gastrointestinal motility. Octreotide

Corticosteroids - dexamethasone

Question 55

List two muscle relaxants that can be used for MSK pain or MS spasticity

FS: not in oxford 6th edition

Answer 55

1. Anticholinergic (cyclobenzaprine)
2. Gaba agonist (baclofen, benzo)
3. Alpha-2 adrenergic agonist (clonidine, tizanidine)

Note: there is actually no evidence that these drugs relax skeletal muscle in the clinical setting. They should not be administered in the mistaken belief that they relieve muscle spasm.

Question 56

List five medications that can be used topically

Answer 56

ketamine
amitryptiline
lidocaine
opioids
NSAIDS
baclofen 
capsaicin

Question 57

Why should SNRIs be tapered slowly and not d/c’d abruptly?

Answer 57

rapid discontinuation may lead to seratonin withdrawal (FINISH) and worsening agitation or anxiety

FINISH =
- Flu like symptoms
- Insomnia
- Nausea
- Imbalance
- Sensory disturbance
- Hyperarousal

Question 58

Significant adverse effect of carbamazepine:

Answer 58

leukopenia