Pharmacology & Therapy: Analgesic and Morphine in Palliative Care PDF

Summary

This document provides a comprehensive overview of pharmacology and therapy for analgesic and morphine in palliative care. It discusses various aspects of pain management, including pain mechanisms and treatments. The presentation emphasizes the importance of an interdisciplinary approach in the care of patients.

Full Transcript

PHARMACOLOGY &
THERAPY
ANALGESIC and
MORPHINE
IN PALLIATIVE
Endang CARE
Isbandiati Soediono
DR, Dr, MS, SpFK
Medical Faculty, Widya Mandala Catholic
University
SURABAYA
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PALLIATIVE CARE
01
ANALGESIC
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 The goal of palliative care

improve overall quality of life for pts.,
caregivers, and families while managing
both general and disease-specific symptom

… simultaneously while a pt. is receiving
curative or life-prolonging tx.
Knowledge of pain classification is
important and necessary to determine the
appropriate medication tx. for each pt.
An interdisciplinary team approach is
beneficial throughout the care of the pt. →
evident whenFKUKWMS7.5
addressing more
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PAIN & THERAPY 01
Effective plan for …. Assessment of pts. description :
quality, precipitating or palliating factors,
region affected, radiation, temporal/time,
impact to function ability. Non-communicative pts. → nonverbal
indicators : grimacing, agitation,
restlessness, or resistance to personal care

Identifying the cause and appropriate
treatment FKUKWMS7.5 01 02 AnalgMorphPal
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PAIN & THERAPY 02
Mechanism of pain based on
Pathophysiology
 A Nociceptive pain:
Results from stimulation of pain receptors.
Somatic: damage to body tissue, well localized
Visceral: from viscera, poorly localized, may
have n.
 B Neuropathic pain:
Results from dysfunctions or lesions in either the
central or peripheral nervous systems.
 C Mixed pain syndromes:
multiple or unknown mechanisms (e.g.
headaches,
vasculitic syndromes).
 D Psychogenic :
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PAIN & THERAPY 03
A. NOCICEPTIVE. Achy, throbbing, and dull. Tx. :. non-opioid analgesic (acetaminophen) → not
for severe hepatic impairment. NSAIDs → not for renal impairment, increase
risk of CV & GI bleeding. Preferable → around the clock (not as needed). Palliative care :
severity, or CIs to non-opioid → use of opioid
( morphine, oxycodone, hydromorphone)
Tx. throughout the day : LA or ER opioid ;
(+) short-acting opioid for “breakthrough” pain
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PAIN & THERAPY 04
B. NEUROPATHIC. Tingling, sharp, burning, electric shock-
like, or numbness. Cause by damage to the central or
peripheral NS. First line tx. : adjuvant agents considered
TCA, SNRIs, Ca channel alpha-2-delta
ligands (gabapentin, pregabalin). Second – line tx.:
traditional analgesic ( opioids, tramadol). Third-line tx.FKUKWMS7.5
: morphine, oxycodone
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PAIN & THERAPY 05
More commonly tx. based on the type of pain :
neuropathic, musculoskeletal, visceral,
dysfunctional
Multimodal tx. for all types of pain :
pharmacologic, physical rehabilitation, and
cognitive behavioral therapy → should be
combined.. Interventional tx. should be considered if
possible

Tx. plan must always include evaluation of
factors :
age, comorbidities, ROA, concurrent medication,
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laboratory abnormalities, and financial resources
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PAIN & THERAPY 06
Acute pain tx. : NSAID, acetaminophen, or opioids
Chronic pain tx.:. First-line for neuropathic pain consist of :. antidepressants (SNRIs or TCA) → enhance the descending
inhibitory pain pathway. Anticonvulsants (sodium-channel blockers, CCBs, or GABA
agonists) → inhibit activation of sodium and calcium channels,
block release of EAAs such as glutamate, or block the post synaptic
receptors.
Some anticonvulsants also enhance inhibitory effects of GABA. Localized pain : topical agents (eg. capsaicin, or local anesthetics). addition of tramadol, tapentadol, or another opioid if the former
agents fail to provide analgesia.. Combination tx. more effective in some cases :
TCA-anticonvulsant or opioid-anticonvulsant. Interventional tx. may be helpful for short-term relief → nerve
blocks
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 PAIN & THERAPY 07
Chronic musculoskeletal pain :. acetaminophen, salicylates, or NSAIDs,. in addition to non-pharmacologic tx. such as heat and ice or
physical rehabilitation modalities
Opioids → tx. in the acute pain setting (immediately after injury
or surgery)
Local pain → topical tx. (NSAIDs, capsaicin)
Trigger points (taut muscle bands) → injections (SNRI)
Duloxetin → tx. musculoskeletal pain (LBP or OA pain)
Visceral pain (somatosensory pathways) → tx. antidepressant or
opioid. Additionally : anticonvulsants (reduce central sensitization and
hyperalgesia)

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Monitored Efficacy and Toxicity
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PAIN & THERAPY 08
Multimodal tx. : essential
Monitoring :. NSAIDs → dyspepsia, PU, GI bleeding, elevated BP, declining
renal function. Antidepressants → dry mouth, constipation, urinary retention
and drowsiness. All anticonvulsants → drowsiness, dizziness, and cognitive
dysfunction, w. short-term memory loss and word-finding difficulty. Some anticonvulsants → laboratory for liver toxicity,
electrolyte imbalance, or bone marrow abnormalities. Opioids → laboratory monitoring long-term ADR
(osteoporosis, hypogonadism, and end-organ impairment, pt. ask
about constipation, drowsiness, n, v, ). Interactions
PK interaction (eg. Hepatic enzyme interactions)
PD interaction (eg. Additive sedation)
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Age related changes 01
1 Reduction in number and function of
peripheral nociceptive neurons.
2 Sensory threshold for thermal and
vibratory stimuli increase w. age.
3 Pain receptors:
50% decrease in Pacini's corpuscles,
10%-30% decrease in Meissner's/Merkle's
disks
4 Diminished endogenous analgesic
response (endorphins) in the older pts.
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Age related changes 02
A. Peripheral nerves :
a) Myelinated nerves
Decreased density
Increase abnormal/degenerating fibers
Slower conduction velocity
b) Unmyelinated nerves
Decreased number of large fibers (1.2-
1.6 mm
No change in small fibers (0.4 mm)
Substance P content decreased
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Age related changes 03
B Central nervous system
Loss in dorsal horn neurons
Altered endogenous inhibition,
hyperalgesia
Loss of neurons in cortex, midbrain,
brainstem
18% loss in thalamus
Altered cerebral evoked responses
Decreased catecholamines, acetylcholine,
GABA, serotonin
Endogenous opioids: mixed changes
Neuropeptides: no change
Geriatric medicine: An evidence based approach 4th edition 2003

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Factors affecting perception
of pain 01
a) Pain affects quality of life far beyond
the local region of injury
b) Feeling of loneliness is predictor of
psychological distress
c) Lack of intimate relationships,
dependency, and loss increase loneliness
d) Loneliness has been shown to lower
pain threshold
e) Loneliness is a risk factor for
depression
Deane G et.al., Overview of pain management in older persons. Clin Geriatr Med 24,185-
201,2008.
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Factors affecting perception
of pain 02
 f) Depression: lack of energy, avoidance of
diversional activities, decreased
engagement in treatment
 g) Anxiety: may inhibit participation in
rehab efforts
 h) Sleep disturbance: pain is best predictor
of sleep disturbance.
 i) Increased health care needs
 j) Isolation and reduced independence:
Involvement w. family and friends can
provide pleasurable experience
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Factors affecting perception of
pain 03
 k) Focusing one's attention on pain makes the
pain worse.
 l) Patients who have low levels of pain
remember it as being worse than they
originally reported.
 m) Pain can be a learned response, rather
than a purely physical problem.
 n) Psychosocial issues like patient’s belief
about their pain , their coping skills, their
involvement in the “sick role”, all have an
impact on how much pain patients feel, and
how it affects them.
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Challenges of pain assessment in
older patients
 Myths that having pain is “natural” with
aging
 Fears about addiction to pain medications
 Sensory and cognitive impairments
 Under-reporting
 Co-morbidities complicating the clinical
picture and caregivers' beliefs and the
reliability of patients' pain.
 Lack of congruence between patients' and
caregivers' perceptions of pain
 Caregiver may misinterpret pain perception
Stein, W.M. Pain in the nursing home. Clinics in Geriatric Medicine 17, 575-94,2001
Stewart, K. et. al. Assessment approaches for older people receiving social care:
content and coverage. International Journal of Geriatric Psychiatry 14, 147-56,1999.
Horgas, A.L. et. al. Pain in nursing home residents. Comparison of residents' self-report
and nursing assistants' perceptions. Journal of Gerontological Nursing 27, 44-53, 2001.
Weiner, D., et. al. Chronic pain associated behaviours in the nursing home: resident
versus caregiver perceptions. Pain 80, 577-88,1999.

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Pain Treatment
Age-Related Physiologic Changes

Decreased renal function
Decreased VD because of decreased
lean body weight
Decreased liver mass and HBF
Decreased enzyme activity
Decreased serum protein
concentrations
Decreased pulmonary function
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Pain Treatment 01
Nonopioid Analgesics for Older
Adults
1 Acetaminophen:
1)Treatment of choice for
Osteoarthritis
2)Exhibits an analgesic ceiling
beyond which higher doses do not
provide greater pain relief.
3) Maximum dose 4 gm/day
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Pain Treatment 02
2 Nonselective NSAIDs
Inhibit PG synthesis
Appropriate for short term use
All have ceiling effect
Risk of GI bleed, renal impairment,
platelet dysfunction
3 Selective COX-2 inhibitors
(celecoxib is only one currently
available in U.S.)
Reduced GI SE and platelet inhibition
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 A wide variety of medication classes are
used for neuropathic, bone, and visceral
pain. alone or in combination w. other pain
management tx. (e.g., opioid) and. after opioid tx. has been optimized or the
pts has demonstrated intolerance to an
opioid

Clinicians should be familiar w. the
indications, common adverse effects,
adverse reactions, PKs, and dosing
guidelines of these medications for pain.

Adjuvant …
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Non-opioid medications for
pain
(adjuvant ) 01
a)TCA ( amytriptyline,
desipramine) for neuropathic pain,
depression, sleep disturbance. Not
used often due to SEs.
b)Duloxetine (Cymbalta )
is newer antidepressant FDA
approved for
neuropathic pain.
c)Anticonvulsants ( gabapentin,
pregabalin, carbamazepine)
for neuropathic pain.
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Non-opioid medications for
pain
(adjuvant ) 02
 d)Muscle relaxants :
for muscle spasm, monitor for sedation
 e)Local anesthetics (lidocaine patch,
topical voltaren gel, capsaicin).
Capsaicin depletes substance P, take weeks
to reach full effect, AE include burning and
erythema.. Lidocain patch FDA approved for post
herpetic
neuralgia.
 f)Placebos:
unethical
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ANALGESICs
Adjuvant analgesics :
medications w. primary indications
other than pain but w. analgesic
properties in pts w. certain pain
syndromes

Typical adjuvant are antidepressants
(AD), anticonvulsants (AC),
corticosteroids, and disease-
modifying medications/therapies
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Adjuvant Analgesics
1. Corticosteroids. MOA : PG synthesis inhibition; central
action on mood and appetite; antitumor
effects in lympho-proliferative
disorders, breast and prostate cancer. Indication : pain related to raised ICP,
extradural spinal cord compression,
tumor compression and invasion of
nerve roots or individual peripheral
nerve. Indication as adjuvant analgesics :
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1. Corticosteroid (continued 01 ). Neurological : raised ICP, SC compress., nerve
compress./ infiltration. Bone metastases. Capsular stretching : liver metast., visceral
metast.. Soft tissue infiltration: head &neck tumors,
abdominal & pelvic tu.. Vascular obstruction: vena cava obst.,
lymphedema. Metastase to joints (intra-articular inj.). Tenesmus (rectal suppository or enema). Effect of hematological malignancies
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1. Corticosteroid (continued 01 ‘). Preparation :. Prednisolone, Dexamethasone,
Hydrocortisone. Choice :. Acute neurological (spinal cord
impression, raised ICP) :
dexamethasone16-24mg/D; weaned as
soon as clinically feasible. Other indications :
dexamethasone 2-4mg/D or prednisolone
15-30mg/D
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1. Corticosteroid (continued 02). SE (related to the dose and duration of treatment) :. Cushingoid facies and body habitus. Cataract. Oropharyngeal candidiasis. CV : HT, thrombosis. Dyspepsia (particularly pt. w. aspirin or NSAID):
tx. antacids, H2-R antagonist, or misoprostol. Proximal myopathy, weakness (chronic adm.). Osteoporosis, arthralgia. Skin (atrophy, thining, striae, hirsutism, easy bruising, purpura). Production or aggravation of diabetes. Fluid retention, edema (Hi-Do.). Hypoadrenalism (abrupt withdrawal). Neuropsychological (improved sense of well-being, insomnia,
frank psychosis). Neutrophilia, lymphopenia
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Adjuvant Analgesics (2)
2. Progestogen. Medroxyprogesterone acetate, megestrol
acetate :
analgesic for metastatic breast, prostate,
endometrial, renal cancer. (antitumor action). Dose : 200-500mg/D MPA
or
160mg/D MA. SE : n, v, fluid retention, weight gain, edema,
CF, HT, vaginal bleeding
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Adjuvant Analgesics (3)

3. Anticonvulsants. Indication : neuropathic pain. Carbamazepine, sodium valproate,
clonazepam (lack of cross-resistance). Tx. w. second AC sometime
successful. SE : n, v, sedation, ataxia,
dizziness, confusion
carbamazepine → leucopenia
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 Anticonvulsant for neuropathic pain
starting increase
usual

effective
dose by
dose

Carbamazepine 100mg/D 100mg each 3D 400-

800mg/D
Sodium valproate 200mg/D 200mg each 3D 800-

2000mg/D
Clonazepam 0,5mg/D 0,5mg each 3D 2-
4mg/D

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Adjuvant Analgesics (4)
4. Antidepressants. Indication : neuropathic p., constant burning
dyesthetic type p., (+) insomnia or depression p.. Analgesia by increasing night-time sedation,
improving mood , relieving depression. Dose : lower than AD, 50-75mg/D amitriptyline
( effect occurs 2-3D). TCA (amitriptyline, imipramine, doxepin) →
superior than the newer non-TCA. Amitriptyline started 25-50mg at night , increasing
to 50-75mg at night (one week no response,
stopped). SE: sedation, anticholinergic , postural hypotension34
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Adjuvant Analgesics (5)
5. Neuroleptics. Chlorpromazine, haloperidol : no analgesic,
reducing anxiety, improving night-time sedation. Specifically for tx. delirium, nausea

6. Anxiolytic Drugs. Benzodiazepine (diazepam, oxazepam,
lorazepam) → advanced cancer → anxiolytic
effect. Diazepam: tx. muscle spasm, acute
musculoskeletal p.. SE : drowsiness, weakness, postural hypotension

7. Antihistamines. Hydroxyzine FKUKWMS7.5
→ opioid sparing effect
01 02 AnalgMorphPal 35
(sedative, anxiolytic)
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Adjuvant Analgesics (6)

8. Psychostimulants. Cocaine : no analgesic effect. Amphetamines :
augment post-op. pain control by
opioids
counteract severe sedation caused by
opioid
elderly → dysphoric. Methylphenidate : to counteract opioid
induced sedation
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Adjuvant Analgesics (7)
9. Oral Local Anaesthetics. Indication : refractair pain. MOA : neuronal membrane stabilization. Mexiletine, 150mg/D, increased each few days in the same
amount up to max. 750mg/D; should not taken w. food. SE : n, sedation, tremor. Caution : IHD, cardiac arrhythmias. (flecainide , risk of sudden death)

10. Ketamine. Dissociative anaesthetic ( short surgical). NMDA –R antagonist. Indication : relieve unresponsive neuropathic p.. SC infusion, subanaesthetic: 0,1-0,5 mg/kg/H , titrated against
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Adjuvant Analgesics (8)

10. Muscle Relaxants
A. Skeletal muscle spasm :. Benzodiazepines (diazepam). Baclofen (reduced function), sedation. Dantrolene : directly on muscle, less
sedation, hepatotoxic
B. Smooth muscle :. nifedipine → tx. tenesmus p. ,
oesophageal spasm
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Adjuvant Analgesics (9)
Drugs for Neuropathic pain
1. Clonidine. Indication : refractair neuropathic p.. Starting Lo-Do, increasing to a max. 300 g/D. ROA (also epidural). SE : hypoT., sedation
2. Nifedipine. Indication : sympathetic type p.. Dose : 20mg 2dd. SE : edema, flushing, postural hypotension
3. Capsaicin. Topical : depletion of substance P neuron in the
treated area. Applied at least 3 or 4 times /D. SE : initially transient stinging
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Adjuvant Analgesics (10)
Drugs for Bone pain
1. Bisphosphonates. Inhibit bone resorption. Indication :
tx. Hypercalcaemia, metastatic bone dis.. (+) pamidronate → less pain

2. Radioisotopes. Stronium (99SR) : relieving bone pain,
osteoblastic activity (response takes 2-
4weeks)
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 Adjuvant Analgesics
Medication Class Dosing Indication

Antidepressants
Amitriptyline TCA 10–150 mg daily Neuropathic pain syndromes
Nortriptyline TCA 10–150 mg daily Neuropathic pain syndromes
Paroxetine SSRI (AD) 10–40 mg daily Neuropathic pain syndromes
Citalopram SSRI (AD) 10–40 mg daily Neuropathic pain syndromes
Duloxetine SNRI 60 mg daily Neuropathic pain syndromes

Anticonvulsants
Carbamazepine 1th generation AC 400–800 mg daily Neuropathic pain syndromes
Gabapentin 2nd generation AC 1,200–1,800 mg daily Neuropathic pain syndromes Pregabalin
2 generation AC
nd
150–300 mg daily Neuropathic pain syndromes

Corticosteroids
Prednisone Corticosteroids 20–80 mg daily Bone pain
Dexamethasone Corticosteroids 4–20 mg daily Bone pain

Other
Lidocaine Anesthetics dependent on dosage form Neuropathic pain syndromes
Baclofen Muscle relaxant 40–80 mg daily Neuropathic pain syndromes
Calcitonin PP hormone 100–200 IU/day IV/SQ Bone pain
Pamidronate Bisphosphonates 30–90 mg IV Bone pain
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 Antiemetic Drugs
Antiemetic Site of Action Dosage/Route Major
Adverse Effect.

Metoclopramide D2 ( GIT) , 5HT3 (HiDo) 5–20 mg po/sc or IV ac ; BBT Dystonia, akathisia,
esophageal
spasm, colic
GIT obstruction
Haloperidol D2 (CTZ) 0.5–4 mg po /sc/IV every 6H Dystonia , akathisia
Prochlorperazine D2 ( CTZ) 5–10 mg po /IV every 6H,
or 25 mg rectally every 6H Dystonia,
akathisia,
sedation
Chlorpromazine D2 (CTZ) 10–25 mg po every 4H,
25–50 mg IM or IV every 4H
or 50–100 mg rectally every 6H Dystonia, akathisia,
sedation,
pos.hypotension
Promethazine H1, mAChR, D2 (CTZ) 12.5–25 mg po/IV every 6H
or 25 mg rectally every 6 h Dystonia,
akathisia,
sedation

Source: Wood GJ, Shega JW, Lynch B, VonRoenn JH. Management of intractable nausea and
vomiting. JAMA 2007;298:1196-1207. Copyright © 2007 American Medical Association. All rights
reserved.
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 Diphenhydramine H1 25–50 mg po/ IV/sc every 6H Sedation, dry
mouth, ur.
ret.
Scopolamine mAChR 1.5 mg transd.patch every 3D Dry mouth,
blur.vi.,
ileus,
ur.ret.,
confusion
Hyoscyamine mAChR 0.125–0.25 mg sl/po every 4H
or 0.2–0.5 mg sc/ IV every 4H Dry
mouth,blur.vi.,
ileus,
ur.ret.,
confusion
Ondansetron 5HT3 4–8 mg po by pill or dis. tab.
or IV every 4–8 h Headache,
fatigue,
constipation. Mirtazapine 5HT3 15–45 mg po every night Somnolence at
LoDo, dry
mouth,
increased
appetite
Source: Wood GJ, Shega JW, Lynch B, VonRoenn JH. Management of intractable
nausea and vomiting. JAMA 2007;298:1196-1207. Copyright © 2007 American
Medical Association. All rights reserved.

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PALLIATIVE CARE
02
MORPHINE
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Opioids Treatment
 Stimulates µ opioid receptor.
 Used for moderate to severe pain.
 Used for both nociceptive and neuropathic
pain.
 Opioid drugs have no ceiling to their
analgesic effects and have been shown to
relieve all types of pain.
 Elderly people, compared to younger people,
may be more sensitive to the analgesic
properties.
 Advanced age is associated w. a prolonged
half-life and prolonged PKs of opioid drugs
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 Opioid peptide in both. The brain stem. The spinal cord

specific opioid receptors

reduce the activity of the dorsal horn relay
neurones

analgesia

Opioid analgesics → mimic endogenous opioid
peptides

prolonged activation of opioid receptors
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 Opioid analgesics. Strong.
Moderate/weak. Morphine. codeine. Diamorphine (heroin). dihydrocodeine. Oxycodone.
dextropropoxyphene. Pentazocine +. Methadone. Pethidine. Buprenorphine x. Fentanyl

+ partial agonist
x mixed agonist / antagonist
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 Opiod analgesic. Analgesia. Respiratory depression. Depression of vasomotor centre →
postural hypotension. Euphoria. Sedation. Miosis (except pethidine → weak atropine-
like activity). N, v (stimulation of chemoreceptor trigger
zone)

Pain act as an antagonist of respiratory
depression FKUKWMS7.5 01 02 AnalgMorphPal 50
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 The goal of palliative care

improve overall quality of life
for pts., caregivers, and families while managing
both general and disease-specific symptom
… simultaneously while a pt. is receiving curative or
life-prolonging tx.. Knowledge of pain classification is important and
necessary to determine the appropriate
medication tx. for each pt.. An interdisciplinary team approach is beneficial
throughout the care of the pt. → evident when
addressing more psychologically based
symptoms, such as delirium.
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Strong opioid analgesics
Morphine. Pe. → widely used to tx. severe pain. Po. → DOC in terminal care. May cause histamine release
→ vasodilatation ,
itching. Tolerance w. continuous adm.. Little tolerance : miosis and constipation. Physical and psychological dependence on opioid
analgesics gradually developed. Sudden termination adm. → withdrawal
syndrome
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Morphine
Opioid analgesic regimen :. Monitor and manage ADR
→ constipation, n, v, sedation, confusion. < ADR : pruritus, urinary retention, myoclonus. Careful monitoring sedation → respiratory
depression : slow dose titration. Tolerance :
after initial days of therapy or after an increase in
dose
→ not for constipation :
tx. (+) simultaneous stimulant
laxative. ADR pts. experience unacceptable w. one opioid
rotation to another agent
FKUKWMS7.5 within
01 02 the class
AnalgMorphPal
lCarePharmacolTheEIS2023Nov
53
Morphine
Cancer Pain Management
Mo. is the DOC for moderate and severe cancer-
related pain
Wide tx. range
Efficacy by many ROA
Reliability
Availability
Low cost
Pharmacology. HL : 2-3Hs; DOA 4 Hs. M6G : chronic adm. > analgesia than single dose. Elderly : increase plasma and CNS fluid of M6G
→ increase neurotoxcicity
FKUKWMS7.5 01 02 AnalgMorphPal 54
lCarePharmacolTheEIS2023Nov
 MOA:
a (direct) spinal
b Brain : modulating peripheral nociceptive
input, activation the descending inhibitory
system from the brain stem to the basal
ganglia
c Limbic system and higher centers →
modify the emotional response to pain
There is no standard dose of Mo. for the tx. of
chronic cancer-related pain
The correct dose of Mo. → controls the pain
whilst tolerable SEs
The dose must be titrated for each pts.
Relative : opioid sensitive and opioid-
insensitive pain
FKUKWMS7.5 01 02 AnalgMorphPal 55
lCarePharmacolTheEIS2023Nov
 Contraindications & Cautions :. renal impairment. severe hepatic dysfunction. Pulmonary dis., acute/ severe bronchial
asthma. CNS depression from any cause. Mo. intolerance or allergy → alternative
opioid. Explanation, reassurance, and antiemetic for
the first few days
FKUKWMS7.5 01 02 AnalgMorphPal 56
lCarePharmacolTheEIS2023Nov
Morphine : side effects
… induce CNS) adverse effects, divided into
three groups.. The first group : effects that lower the level
of consciousness–sedation, drowsiness and
sleep disturbance.. The second group affects the thinking
process and the ability to react–cognitive
impairment, psychomotor impairment, delirium,
hallucinations, dreams and nightmares.. The third group is of the direct toxic effects
of opioids on neurons and includes myoclonus
(perhaps), hyperalgesia and tolerance.
FKUKWMS7.5 01 02 AnalgMorphPal 57
lCarePharmacolTheEIS2023Nov
Morphine : side
effects
CNS : sedation, drowsiness, confusion, narcosis,
coma, dysphoria, psychotomimetic effects (fear,
panic, agitation, feeling unreality,
depersonalisation, vivid dreams, nightmares,
hallucinations, disorientation, delusion,
psychosis), myoclonus, miosis
GIT : n, v, delayed gastric emptying, constipation,
dry mouth, biliary colic
Respiratory : resp. depression, cough reflex
suppression
CV : postural hypotension
Urinary : urgency, retention
Skin : flushing, sweating, pruritus
Tolerance
Physical dependence
Psychological dependence
FKUKWMS7.5 01 02 AnalgMorphPal 58
lCarePharmacolTheEIS2023Nov
Morphine : side
effects
Sedation. Occurs more frequently in pts.”. Elderly or frail. Renal impairment. Have other causes of CNS depression. Opioid naïve. Only mild pain. Have had pain acutely relieved by a procedure such a nerve block. Usually mild and last 2 to 5Ds. In a few cases → severe drowsiness and confusion occur → dose
reduction. Persistent sedation :
assessment of renal function, exclusion of other causes CNS
depression → metabolic disturbances, infection, cerebral
FKUKWMS7.5 01 02 AnalgMorphPal 59
metastase, DI -sedationlCarePharmacolTheEIS2023Nov
Morphine : side effects
Narcosis. Too La-Do → severe sedation or
narcosis w. loss of consciousness and
respiratory depression. Tx. :. Naloxone,. suspected OD 0,4 – 2,0mg iv. ,
q33min, up to 5 doses. Buprenorphine , 8-16mg to
reverse narcosis
FKUKWMS7.5 01 02 AnalgMorphPal 60
lCarePharmacolTheEIS2023Nov
Morphine : side
effects
Dysphoria and psychotomimetic effects. May occur w. morphine or other opioid drugs.
Tx. Tranquilizer (e.g haloperidol)

GIT, nausea, vomiting. Constipation every pt. commencing therapy w. morphine
requires dietary advice and prescrition of laxatives to px.
constipation
Tolerance does not develop to the constipating effects of
morphine and dietary and laxative tx. are necessary for the
duration of tx.

Xerostomia. Tx. Symptomatic
if severe → assessment of for other causes should be
made → drugs w. anticholinergic SE (antidepressants)
FKUKWMS7.5 01 02 AnalgMorphPal 61
lCarePharmacolTheEIS2023Nov
Morphine : side
effects
Hallucinations, Dreams, and Nightmares. Hallucinations and nightmares
associated w. opioid use, mainly in the
post-operative rather than the palliative
care setting.. In the terminally ill, nightmares,
particularly about death, have been
associated w. opioid use. little evidence to suggest opioid-
induced dreams, nightmares or
hallucinations in palliative care, other
than as part of a delirium, perhaps as
prodromal symptoms.
FKUKWMS7.5 01 02 AnalgMorphPal
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62
 Toxic Effects on neurons. Neurotoxic effects : endocytosis of
opioid receptors, and activation of
NMDA-Rs.. Glutamate, activates NMDA-Rs and
opioid-induced neurotoxicity regulation,
at least in part, by spinal glutaminergic
activity and NMDA-Rs.. NMDA-Rs w. antagonists (ketamine) →
px., tx.. Modulating glutamate transporter
activity in SC px. development of opioid-
induced neurotoxic
FKUKWMS7.5 01 02 AnalgMorphPal 63
lCarePharmacolTheEIS2023Nov
 Toxic Effects on neurons. Opioid rotation → alleviation of
neurotoxicity.

Pt. who had a poor analgesic to Mo.
and morphine-induced neurotoxicity,
rotation to methadone, an NMDA
antagonistic , aided analgesia and
alleviated the neurotoxicity.

FKUKWMS7.5 01 02 AnalgMorphPal 64
lCarePharmacolTheEIS2023Nov
 MYOCLONUS. Chronic opioid, particularly Hi-Do.;
risk increased in the presence of
spinal cord lesions.. MOI of myoclonus :. glycine inhibition in dorsal horn
neurons → decrease in the inhibitory
effects of this neurotransmitter →
myoclonus and hyperalgesia.. Glutamate activation of NMDA-
Rs, or serotonergic and GABA-
aminergic pathways in the brain
stem. FKUKWMS7.5 01 02 AnalgMorphPal
lCarePharmacolTheEIS2023Nov
65
 MYOCLONUS. Dopamine antagonism in the basal
ganglia
→ EP pathways.. Myoclonus associated w. Mo. →
accumulation of the active metabolite
M-6-G and the toxic metabolite M-3-G.. Tx. : a opioid rotation or dose
reduction.
b (+) benzodiazepines, or
baclofen
→ alleviate myoclonus.

FKUKWMS7.5 01 02 AnalgMorphPal 66
lCarePharmacolTheEIS2023Nov
 HYPERALGESIA
…. develop in conjunction w. opioid tolerance
→ a result of opioid-induced apoptosis of certain cells.. The loss of GABA neurons → changes in spinal neuronal
circuits involved in pain and pain modulation
→ sensitivity to pain increased → hyperalgesia.
… NMDA-R agonism also has a major role in the
development of hyperalgesia, as does glycine, an inhibitory
neurotransmitter that mediates the post synaptic inhibition
of spinal neurons.
…. Glycine is inhibited by Mo.
→ a reduction of postsynaptic inhibition at the spinal cord
level and an increase in pain.
…. The treatment of hyperalgesia is not well established.

NMDA antagonists, ketamine,
→ prevented fentanyl-induced hyperalgesia.
FKUKWMS7.5 01 02 AnalgMorphPal 67
lCarePharmacolTheEIS2023Nov
 TOLERANCE. The same dose → less analgesia or
an increase in dose fails to increase
analgesia. Characterized → a shortened DOA and
decreased extent of analgesia, euphoria,
sedation and other effects caused by
CNS depression, as well as by marked
elevation of the average lethal dose

Escalating dose of opioids may be
indicative of pharmacological tolerance,
it may also reflect escalating pain from
disease progression.
FKUKWMS7.5 01 02 AnalgMorphPal 68
lCarePharmacolTheEIS2023Nov
 Tx. or px. of opioid tolerance :. NMDA receptor antagonism and nitrous oxide
synthetase inhibition.. NMDA receptor antagonists, ketamine, px. and
reverse tolerance and abolish hyperalgesia.. NMDA antagonism is specific for Mo. and not other
opioids. Methadone, some NMDA antagonistic activity,
decrease the development of tolerance. Tolerance minimized by opioid rotation → to
methadone
Tolerance to methadone less commonly than other
opioid-tolerance FKUKWMS7.5 01 02 AnalgMorphPal
lCarePharmacolTheEIS2023Nov
69
ROA of Morphine
Immediate-release oral
Controlled-release oral
Subcutaneous infusion
Intravenous
Intramuscular
Rectal
Spinal
Intraventricular
FKUKWMS7.5 01 02 AnalgMorphPal 70
lCarePharmacolTheEIS2023Nov
 Immediate-release oral Mo.. POC for pts w. moderate or severe pain who are
able to take oral medication. 30mg PO equiv. to 10mg IM
Mo. sulphate 30mg tabl., longer acting po.

Oral Mo. Mixture. Mo. HCl 2mg/ml, 5mg/ml and 10mg/ml. Advantage : cheap, well absorbed, well tolerated,
(self adm.), easy to take (30-100ml/24Hs) compare
to imm.-rel. tab., effective in 85% pts, flexibility of
dose, wide T range, frequent dose adjustment
poss., no cummulative toxicity, Hi-Do. poss. in small
volumes. No other drug should be included in a Mo. mixture 71
FKUKWMS7.5 01 02 AnalgMorphPal
lCarePharmacolTheEIS2023Nov
 Initial dose :
estimated from the amount of opioid drugs the pt. is
currently taking.
Breakthrough pain :
tx. w. extra doses of mixture taken as often as
necessary
Incident pain :
occurs only in certain circumstances such as after a
particular movement or on standing.
Adjustment of dose:
if pain relief is inadequate or more than occasional
backup dose are required, the dose is titrated
upwards watch the SE.
If pain worse at night or troubled by
sedation during the day
→lower dose byFKUKWMS7.5
day and higher dose at night
01 02 AnalgMorphPal 72
lCarePharmacolTheEIS2023Nov
 Controlled-release oral Mo.. Preparations given 12-hourly, TOC for
pt. able to take oral Mo., once the
general dose requirements have been
established. Should be swallowed whole.. For pts. not currently receiving opioid
drugs and those on tx. w. opioids other
than Mo., the best methode of starting
controlled-release Mo. is to stabilize the
pt. on immed.-release oral Mo. mixture
for one to a few days.
FKUKWMS7.5 01 02 AnalgMorphPal 73
lCarePharmacolTheEIS2023Nov
 Subcutaneous infusion Mo.
compatible :

tx. in home setting → effective and safe. Given 4-hourly injection or by continuous
infusion, via a sc-butterly needle.. Sc infusion is the preferred method as it
avoids fluctuating blood levels and
requires drug preparation only once a day.. Compatible drug w. Mo.:
metoclopramide, haloperidol,
clonazepam,
midazolam, buscopan
FKUKWMS7.5 01 02 AnalgMorphPal 74
lCarePharmacolTheEIS2023Nov
UNDERUTILISATION OF MO.:
OPIOPHOBIA
Professional :. Only be used when pts. are dying. Hasten death. Doesn’t work :. Incorrect admin.. Opioid-insensitive pain. Ignoring psychosocial aspect of care
Causes respiratory depression
Causes unacceptable SEs :. Constipation, nausea, somnolence
Fear of :. Tolerance. Physical dependence. Psychological dependence
FKUKWMS7.5 01 02 AnalgMorphPal
lCarePharmacolTheEIS2023Nov
75
 Patient opiophobia :. “ means I’am going to die soon”. Nothing left for when the pain gets worse. Fear of addiction. Allergy. Didn’t work :. Incorrect adm.. No instruction for breakthrough pain. Mo.-insensitive pain. Ignoring psychosocial issues. Couldn’t take the Mo. :. Somnolence. Confusion. Nausea. Constipation
FKUKWMS7.5 01 02 AnalgMorphPal
lCarePharmacolTheEIS2023Nov
76
 Analgesic Morphine in
palliative care :

Given adequate explanation, good
prescribing and individual titration
dosage, most patients will achieve
good pain relief without
unacceptableside effects.

FKUKWMS7.5 01 02 AnalgMorphPal 77
lCarePharmacolTheEIS2023Nov
Other Opioid Analgesic
Diamorphine (heroin,
diacetylmorphine). More lipid soluble → more rapid OOA by
injection. Higher peak level → more sedation. Diamorphine : tx. control severe pain

Methadone. Long DOA; less sedation. Used orally for maintenance tx. for morphine,
heroin addicts → px. “buzz” of iv. drugs
FKUKWMS7.5 01 02 AnalgMorphPal 78
lCarePharmacolTheEIS2023Nov
Other Opioid Analgesic
Buprenorphine. Partial agonist, agonist, antagonist. PK : po well absorbed, liver metab., excretion in
bile & urine, HL 3Hs. Slow OOA. Effective analgesic sublingual adm.. PD : DOA 6-9Hs. Indication : moderate to severe pain. SE : similar opioid; respiratorry depression
LaDo. Naloxone (but difficult to
reverse → dissociates very slowly from Rs).. Prolonged vomiting
FKUKWMS7.5 01 02 AnalgMorphPal 79
lCarePharmacolTheEIS2023Nov
Other Opioid Analgesic
(2)
Buprenorphine. Tx. Depression : naloxone > (2 -3 mg inj.). DDI :. if (+) second opioid
prevent or delay the
second drug. pts. w. HiDo Mo.(+) buprenorphine

withdrawal sy.. Dose : 0,3 – 0,6mg IM, or 0,4 – 0,8mg SL, q8H. Dose equivalence :
0.3mg IM eq. to Mo. 10mg IM
0,4mg SL eq.to Mo. 30mg PO
FKUKWMS7.5 01 02 AnalgMorphPal 80
lCarePharmacolTheEIS2023Nov
Other Opioid Analgesic
(3)
Codeine (methylmorphine). Po. well absorbed, liver metab., urine excretion. HL 2,5 0 3H. DOA :4 – 6 Hs. Indication : mild to moderate pain, cough, diarrhoea. SE : similar to Mo., more constipating. Dose : 30 – 60 mg q4 – 6H. Dose eq. : 240mg PO eq. to Mo. 30mg PO. Preparation :. codeine tablet 30mg. codeine 8mg (+) aspirin / paracetamol. codeine 30mg (+) aspirin/ paracetamol
FKUKWMS7.5 01 02 AnalgMorphPal 81
lCarePharmacolTheEIS2023Nov
Other Opioid Analgesic
(4)
Dextromoramide. PK : po well absorbed. DOA : 2-3Hs. Indication : severe pain. SE : similar to Mo.
more rapid tolerance devel.. Preparation : 5mg tablet. Dose equiv.: 10mg PO equiv. to 30mg PO
Mo. (but may last only 2Hs)
FKUKWMS7.5 01 02 AnalgMorphPal 82
lCarePharmacolTheEIS2023Nov
Other Opioid Analgesic
(5)
Dextropropoxyphene. PK : po well absorbed, liver metab., urine excr., HL 12-
15Hs. DOA : 4-6Hs. Indication : mild to moderate pain. SEs :. generally less severe than Mo.. CNS depression & seizure in overdose. DDI :. Potentiates oral anticoagulant. Predisposing carbamazepine toxicity. Preparation :. D HCl 32,5 mg (+) paracetamol 325mg. D. napsylate 100 mg. Dose : D. HCl 65mg q4-6H
FKUKWMS7.5 01 02 AnalgMorphPal 83
D. napsylate 100mg q4-6H
lCarePharmacolTheEIS2023Nov
Other Opioid Analgesic (6)
Fentanyl , alfentanil, remifentanil. Synthetic opioid for perioperative pain : IV., IM., SC., ED., or
transdermal. DOA : short (0,5 – 1H). Lo-Do fentanyl and alfentanyl → short- acting
(rapid redistribution);. La-Do saturate tissues → more prolonged actions. Patch : DOA 72Hs (does not peak plasma level for 12-
24Hs ) → need other analgesia during this time. Dose equiv. : 0,1mg fentanyl equiv. to 10mg IM Mo.. Indication : transdermal fentanyl for pts intolerant of oral
MO. /unable to take because dysphagia or drowsiness
(particularly useful in renal failure). Pts. intolerant of Mo. and requiring PE tx. Continuous IV
or SC infusion FKUKWMS7.5 01 02 AnalgMorphPal 84
lCarePharmacolTheEIS2023Nov
Other Opioid Analgesic
(7)
Methadone. Synthetic opioid ; PO, PR., injection. Tx. severe pain, Mo. intolerance. CI or great caution : frail, elderly,, confused, significant
hepatic or renal impairment. SE : similar to MO.; cumulative toxicity (+) → sedation
confusion. Single dose HL 15Hs; continued tx. HL 2-3Ds → reduce
both the dose and frequency of admin.. DOA : long DOA, 4-6Hs initially; 6-12Hs w. continued adm.. Dose : calculated from previous tx., adjusted for response
and toxicity
frequency : q 4-6H for first 1-3D; then q6-12Hs. Equiv. dose : 20mg PO equiv. to 30mg PO MO.
10mg IM equiv. to 10mg IM MO.. Preparation : 5mg,FKUKWMS7.5 01 02 AnalgMorphPal
10mg tablets; 10mg injection
lCarePharmacolTheEIS2023Nov
85
Other Opioid Analgesic
(8)
Oxycodone. Semi-synthetic derv. of codeine; wider
therapeutic range. Indication : LoDo. to tx. mild and moderate pain,
HiDo. for severe pain. Well absorbed PO and rectal; liver metab.,
exc.urine. DOA : oral 4-6H, rectal 6-12Hs. Dose : oral 5-10mg q4-6Hs; rectal 30mg q6-12Hs. Dose equiv. : 30mg PO or PR equiv. to 30mg PO
Mo.. Preparation : O. HCl 5mg tablet
O. pectinate 30mg suppository 86
FKUKWMS7.5 01 02 AnalgMorphPal
lCarePharmacolTheEIS2023Nov
Other Opioid Analgesic
(9)
Pentazocine. Synthetic; absorbed slowly orally; HL 2-3H
DOA : 3-4Hs; PO, PE. Indication : mild to moderate pain in pts not
receiving other opioid drugs. SEs : similar to other opioid, (+)
psychotomimetic SE. Not for chronic cancer - related pain because of
the high incidence of psychotomimetic SE and the
potential for DDIs w. opioid agonists (precipitated
withdrawal sy. and pain). Dose : no standard do. for chronic cancer pain;
freq. q3-4Hs. Dose equiv. : 180mg PO equiv. to 30mg PO Mo.
60mg IM equiv. to 10mg IM Mo.
FKUKWMS7.5 01 02 AnalgMorphPal 87. Preparation : tablet 25mg, 50mg; injection 30mg
lCarePharmacolTheEIS2023Nov
Other Opioid Analgesic
(10)
Pethidine. Irregularly absorbed per oral; liver metab., urine excr.; HL 3-4H. Rapid OOA , Short DOA : 2-3H. Indication : severe acute pain. Tx.-ceiling related to CNS toxicity; not used to tx. chronic cancer-
rel. pain. CI : pts taking MAO-I; caution : renal impairment. SE : less constipating, not antitussive, no miosis
CNS toxic. (nor-pethidine accumulation): agitation, tremor,
myoclonus, seizures. DDI :. phenobarbitone, phenytoin : diminish analgesia,
increase CNS toxicity
of pethidine. MAO-I : excitation, hyperpyrexia, seizures. Enhance toxicity of other CNS depressant drugs. No standard dose forFKUKWMS7.5
chronic 01
ca-pain, freq. q3H
02 AnalgMorphPal 88
lCarePharmacolTheEIS2023Nov
 Pethidine (continued). Norpethidine : renal imparment
( frequent or high doses)

agitation, tremor, myoclonus and seizures. Tx. myoclonus and seisures : BDZ and
anticonvulsants
Not responsive to naloxone

FKUKWMS7.5 01 02 AnalgMorphPal 89
lCarePharmacolTheEIS2023Nov
Medication Management
Deprescribing:
to improving care and minimizing unecessary
polyfarmacy

Reduce the burden to pts due to. ADR of drug (s). DDI. Inappropriate medications

Reduce medication burden, decreased
mortality, shorter hospitalization, and
improvementsFKUKWMS7.5
in pts01overall health
02 AnalgMorphPal
lCarePharmacolTheEIS2023Nov
90
Medication Management
Drug candidates for
deprescribing :. WO. an indication. High risk and benefit ratio. Drug initiated to control ADR
associated w. another drug. Preventive drug whose benefit is
unlikely to be realizedgiven pts’s life
FKUKWMS7.5 01 02 AnalgMorphPal
lCarePharmacolTheEIS2023Nov
91
 Special challenges for
pharmacotherapy recognizing the
end is near is important :

Dysphagia of liquids, pulselessness on the
radial, respiration w. movement,
decreased urine out put, Cheyne-Stokes
breathing, death rattle, periods of
apnea,peripheral cyanosis.
Attention to symptoms arise or worsen ;
delirium, dyspnea, fatique, pain, cough,
death rattle, myoclonus, fever, and
emergency such as catastrophic
hemorrhage
FKUKWMS7.5 01 02 AnalgMorphPal 92
lCarePharmacolTheEIS2023Nov
 Medication management at this point :. Elimination of medications unlikely benefit. Switching to non oral ROA. Opioids,. Lorazepam,. Dexamethasone,. Haloperidol. Intensol formulation → 1ml instilled in the
buccal cavity. Discussed w. the family member and
caregivers

FKUKWMS7.5 01 02 AnalgMorphPal 93
lCarePharmacolTheEIS2023Nov
Non-drug treatment 01
 Education:
basic knowledge about pain (diagnosis, treatment,
complications, and prognosis), other available
treatment options, and information about over-the-
counter medications and self-help strategies.
 Exercise:
tailored for individual patient needs and lifestyle;
moderate-intensity exercise, 30 min or more 3-4
times a week and continued indefinitely.
 Physical modalities (heat, cold, and
massage)
Cold for acute injuries in first 48 hours, to decrease
bleeding or hematoma formation, edema, and
chronic
back pain.
Heat works well for relief of muscle aches and
abdominal
cramping.
FKUKWMS7.5 01 02 AnalgMorphPal 94
lCarePharmacolTheEIS2023Nov
Non-drug treatment 02
Physical or occupational therapy;
should be conducted by a trained
therapist
Chiropractic: Effective for acute back
pain. Potential spinal cord or nerve root
impingement should be ruled out
before any spinal manipulation
Acupuncture: Performed by qualified
acupuncturist. Effects may be short
lived and require repetitive treatments
FKUKWMS7.5 01 02 AnalgMorphPal 95
lCarePharmacolTheEIS2023Nov
Non-drug treatments 03
 Relaxation:
repetitive focus on sound, sensation, muscle tension,
inattention towards intrusive thoughts. Requires individual
acceptance and substantial training.. Meditation:
Guided or self-directed technique for calming the mind, allows
thoughts, emotions and sensations to travel through
conscious awareness without judgment.
Progressive muscle relaxation: Individual tensing and
relaxing of certain muscle groups.
 Hypnosis:
effective analgesic, state of inner absorption and focused
attention. Reduces pain by distraction, altered pain
perception, increased pain threshold.
Norelli L J et.al., : Behavioral approaches to pain management in the elderly, 24(2), Clinics in Geriatric Medicine, 2008.
FKUKWMS7.5 01 02 AnalgMorphPal 96
lCarePharmacolTheEIS2023Nov
Non-drug treatment 04
 Cognitive-behavioral therapy:
Pain is influenced by cognition, affect and behavior.
Conducted by a trained therapist, focuses on
changing individual cognitive activity to modify
associated behavior, thoughts, and emotions.
10-12 weekly individual or group sessions
Participants have to be cognitively intact
 Operant behavior therapy:
Use of negative and positive consequences to modify
the behaviors.
 Mind-body conditioning practices:
Yoga, tai chi, qigong.
Norelli L J, et.al.,: Behavioral approaches to pain management in the elderly, 24(2), Clinics in Geriatric Medicine, 2008.

FKUKWMS7.5 01 02 AnalgMorphPal 97
lCarePharmacolTheEIS2023Nov
Consequences of untreated pain
 Impaired function:
Pain can lead to decreased activity and ambulation leading to de-
conditioning, gait disturbances and injuries from falls.

 Sleep deprivation:
decrease pain thresholds, limit the amount of daytime energy, increased
risk of depression and mood disturbances.

 Increases financial and care giving burdens
placed on families and friends by increased utilization of health care
services.

 Diminished quality of life
by isolating individuals from important social stimulation, amplifying
the functional and emotional losses already experienced from
undertreated pain.
Jakobsson, U. et.al., Old people in pain: A comparative
FKUKWMS7.5 01study. Journal of Pain and Symptom Management, 26, 625-
02 AnalgMorphPal 98
636,2003.
lCarePharmacolTheEIS2023Nov
Weiner, D.K., et.al., Pain in nursing home residents; management strategies. Drugs and Aging, 18(1), 13-19,2001.
Cancer Pain
Initial tx. based on the severity. Mild pain (eg. pain rated ≤ 4) non-opioid or a
combination of non opioid and an opioid analgesic. Moderate to severe pain → usually requires an
opioid analgesic. Neuropathic pain tx. → anticonvulsant or
antidepressant medication. Nerve blocks and invasive surgical procedures →
option for pain control that is refractory to conventional
medication management
FKUKWMS7.5 01 02 AnalgMorphPal 99
lCarePharmacolTheEIS2023Nov
Cancer Pain
The analgesic ladder progresses in a stepwise manner. Acetaminophen. NSAIDs
and. Adjuvant medication (eg. coanalgesics such as
anticonvulsants and antidepressants for neuropathic
pain ) as initial tx.. If pain intensity >4 of 10 but not severe, weak opioid
analgesics may be added to the pain regimen.. Severe pain → strong opioids such as morphine,
hydroxymorphone, fentanyl, oxycodone are
recommended
FKUKWMS7.5 01 02 AnalgMorphPal 100
lCarePharmacolTheEIS2023Nov
Cancer Pain
Hydromorphone → good choice for iv. Opioid tx.. Does not have active metabolite
(could accumulate w. renal insufficiency)

Fentanyl (transdermal patch) → excellent for out pt.
(provide continuous release of opioid and convenient to
use). Intended for opioid tolerant pt. w. stable chronic pain

Kadian (ER morphine capsule) can be admin. Via gastric
feeding tube because the capsule is opened and
contentsflush through the gastric feeding tube w. water
Limitation → pt. manipulation of the gastric feeding
tube w. self-admin. and potential for morphine SEs
secondary to metabolite accumulation if renal insufficiency
persists FKUKWMS7.5 01 02 AnalgMorphPal
lCarePharmacolTheEIS2023Nov
101
Cancer Pain
Opioid tx. for breakthrough pain → spontaneous pain
(frequently idiopathic, occurring w. no known stimulus)
a) Incident pain (secondary to a stimulus that the pt. may
or may not be able to control)
→ can be reduced by take a dose of short-acting opioid
30 minutes before activity
Or
b) End-of-dose failure (pain at the end of the dosing interval
of the long-acting opioid)

Spontaneous breakthrough pain → tx. a short-acting
opioid as soon as the pain is experienced
Pt. on long-acting opioid, end-of- dose failure,
→ supplementary doses of a short-acting opioid doses eq. to
5% to 15% to the total daily dose to be taken every 2Hs as
needed.
FKUKWMS7.5 01 02 AnalgMorphPal 102
lCarePharmacolTheEIS2023Nov
Cancer Pain
Short-acting opioid/acetaminophen → have a
maximal dose to prevent liver toxicity w.
acetaminophen → creating a ceiling limit on
the analgesic efficacy
Plain short-acting opioids (eg. morphine,
oxycodone, hydromorphone) → should be
used for pt. requiring La-Do for breakthrough
pain
Fentanyl admin. by oral transmucosal (Actiq)
or buccal (Fentora) routes
→ approved for breakthrough pain
management in cancer pt.
FKUKWMS7.5 01 02 AnalgMorphPal 103
lCarePharmacolTheEIS2023Nov
Methadone
Opioid agonist w. analgesic activity at mu and
delta Rs. Long HL 15- 60Hs; DOA 6-12Hs
Good option for neuropathic pain → 5-HT
and NE reuptake inhibition and antagonist
effects at the NMDA –Rs
The single methadone conversion factor for
acute pain and does not account for chronic
use
Rotation to methadone → if pt. has
inadequate respons w. to other opioids or
experiences intolerable SE such delirium,
myoclonus, or nausea
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Methadone
Toxicity. Risk of fatal respiratory depression. QT interval prolongation > 500
milliseconds

reducing or discontinuing methadone. CIE → sign and symptoms of
methadone toxicity shallow breathing,
slowed respiration followed by periods of
not breathing, slurred speech or difficulty
talking FKUKWMS7.5 01 02 AnalgMorphPal
lCarePharmacolTheEIS2023Nov
105
Pharmacological Treatments for
Opioid-Related SEs
Side Effect Treatment.Constipation. Stool softener, laxative,
methylnaltrexone, oral
naloxone. Sedation. Methylphenidate,
modafinil. Pruritus. Diphenhydramine,
hydroxyzine. Nausea. Prochlorperazine, haloperidol,
metoclopramide, ondansetron,
antihistamine.Dysphoria. Haloperidol, opioid rotation. Cognitive impairment. Methylphenidate, modafinil,
opioid rotation. Myoclonus FKUKWMS7.5. 01
Clonazepam,
02 AnalgMorphPal dose reduction, 106
opioid rotation lCarePharmacolTheEIS2023Nov
Thank You
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