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Opioid Induced Neurotoxicity

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Title: Opioid Induced Neurotoxicity

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Opioid Induced Neurotoxicity

Burton Abbott, MD

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(No Transcript)
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Opioid Induced Neurotoxicity

Introduction
General Comments Regarding Opioids
Opioid Receptors and Metabolites
Predisposing Factors
Clinical Features
Management
Cases
Summary

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Opioid Induced Neurotoxicity

Neuroexcitatory sydrome described primarily in
cancer patients who are on high doses of opioids
Described as resulting from opioid metabolites
Described from 1990s to present
Best described for meperidine
Recently described for other opioids

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Opiates, Opioids and Narcotics

Opiate
A specific term
Naturally occurring or semisynthetic drugs
derived from the opium poppy
e.g. morphine
Opioid
A more general term
Naturally occurring, semisynthetic or synthetic
drugs that are opioid receptor agonists
e.g. morphine, methadone, fentanyl

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Opiates, Opioids and Narcotics

Narcotics
An imprecise term including opioids and other
drugs with potential for abuse
Pejorative connotations
Term generally not used in pain or palliative
care literature
Hanks GW, Cherny N. Opioid Analgesic Therapy.
In Oxford Textbook of Palliative Medicine 2nd
ed. 1998

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Prevalence of Cancer Pain
From Portenoy Cancer 632298, 1989
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Opioid Induced Neurotoxicity

Recent emphasis on treatment of pain and other
symptoms especially in cancer
Morphine use worldwide increased 2.5 x
between1972 and 1987
There appears to be a corresponding increase in
reports of opioid related hallucinations,
agitation, myoclonus, and seizures
Daeninck PJ, Bruera E. Acta Anaesthesiol Scand.
1999

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Opioid Induced Neurotoxicity

Difficult to really tell prevalence or if it is
increasing
Little written prior to 1990s
Mainly case reports up to the present time
Anecdotally, more reports in recent years
especially among oncologists and palliative care
physicians

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Opioid Induced Neurotoxicity

Thought to be relatively common among patients on
high dose opioids
Thwaites et al
Retrospective study
48 cancer patients all on continuous parenteral
hydromorphone infusion
Three neuroexcitatory symptoms agitation,
myoclonus, and seizures
These symptoms not associated with specific
diagnosis, age
Agitation, myoclonus, seizures independently
associated with
Dose (plt0.05, plt0.001, plt0.05)
Duration (plt0.01, plt0.05, plt0.01)
of hydromorphone
Thwaites et al. J Palliat Med 2004.

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Opioid Receptors

Three types of opioid receptors m, d, k
Several subtypes within each type
Beneficial and adverse effects mediated through
receptors
Opioid drugs are agonists with varying affinity
at these receptors
Inturrisi CE. Clin J Pain 2002

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Opioid Receptors

Inter-individual variation in receptor
type/subtype
?differences between individuals therapeutic
response/adverse effects with opioids
m receptor mediates most analgesic (and adverse)
effect
Most common opioids are predominantly m agonists
Naloxone is a m antagonist
Inturrisi CE. Clin J Pain 2002

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Opioid Metabolites

Neuroexcitation induced by opioid metabolites is
best documented for meperidine
BUT
This phenomenon has been described for ALL
opioids

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Opioid Metabolites

Opioids undergo hepatic metabolism
(glucuronidation or demethylation) then renal
clearance
Some opioid metabolites are active and some are
neuroexcitatory
Morphine
predominantly metabolized by glucuronidation to
M-3-G and M-6-G
Also N-demethylation to normorphine
Hydromorphone
Predominantly metabolized to H-3-G

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Opioid Metabolites

Meperidine is primarily metabolized via
N-demethylation to normeperidine
Normeperidine is a potent neuroexcitant
Normoperidine may result in neuroexcitation
(delirium, irritability, myoclonus, seizures)
even after relatively little meperidine
administration

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Opioid Metabolites
After Smith MT. Clinical and Experimental
Pharmacology and Physiology 2000
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Opioid Metabolites

In CSF, M-3-G exceeds morphine and M6G by
approximately 2 and 5 fold respectively
As M-3-G or H-3-G increase, neuroexcitatory
behaviors are seen
M-3-G and H-3-G have no analgesic activity, but
they are neuroexcitatory

Smith MT. Clinical and Experimental
Pharmacology and Physiology 2000
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Opioid Metabolites

Morphine-6-glucuronide
is a potent m agonist
Has analgesic activity
Morphine-3-glucuronide
Has nociceptive activity
Is not a m antagonist
Related to neuroexcitation (agitation, delirium,
hyperalgesia/allodynia, myclonus, seizures)
Christrup LL. Acta Anaesthesiol Scand. 1997

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Morphine Metabolites in Renal Insufficiency
n18 patients Followed over 4 to 26
weeks ?inverse relationship between estimated
creatinine clearance and ratio of metabolite to
morphine
Ravenscroft P, Schnider J. Clinical and
Experimental Pharmacology and Physiology 2000
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Opioid Induced Neurotoxicity

Predisposing Factors
High opioid doses
Prolonged opioid use
Recent rapid dose escalation
Dehydration
Renal failure
Advanced age
Other psychoactive drugs
Daeninck PJ, Bruera E. Acta Anaesthesiol
Scand. 1999

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Opioid Induced Neurotoxicity

Differential Diagnoses
Metabolic (Na, K, Ca)
Hyoxemia
Hypercarbia
Sepsis
Drug effect
Uremic encephalopathy
Hepatic encephalopathy
Terminal Delirium

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Opioid Induced Neurotoxicity

Management
Consider consultation with palliative care MD on
call
Discontinue offending opioid
Hydration
Begin alternative opioid
Consider benzodiazepine
NO role for naloxone
Daeninck PJ, Bruera E. Acta Anaesthesiol
1999

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Opioid Induced Neurotoxicity

Management
Consider nonopioid (adjuvant) medications (e.g.
bisphosphonates, gabapentin)
Consider consultation with
Radiation oncology
Anesthesia (e.g. regional anesthesia)
Orthopedic surgery
Occupational therapy (e.g. splinting, seating)

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Opioid Rotation

Retrospective study of 80 patients who had
undergone opioid rotation for neuroexcitatibility
symptoms
Cognitive deterioration, hallucinations,
myoclonus
These symptoms improved in 58/80 (plt0.01)
Significant improvement in pain control per VAS
New opioid dose was significantly lower than that
thought to be equianalgesic

de Stoutz et al. J Pain Symptom Manage 1995
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Opioid Rotation to Which Opioid?

It is felt that any change to one of the common
opioids indicated for chronic use is beneficial
To a different class if possible
Methadone, fentanyl/sufentanil
No neuroexcitatory metabolites identified
Less common for patient to be on any of these
medications from the community
Note that neuroexcitation has been described for
all opioids

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Case 1

Mrs. I.H. 54 y.o. woman with metastatic ovarian
carcinoma diagnosed in 2002
Transferred Feb. 21/05
Received call from rural physician (Community
Cancer Program) re out of control pain and
widespread twitching
The note accompanying patient
Her pain has recently been escalating and we
likely need a new strategy.
Admitted at 1525 h
Pain everywhere but worst in abdomen, R hip
area, R leg

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Case 1 contd

History included laparotomy R hemicolectomy,
debulking surgery incl hysterectomy BSO,
radiation, chemotherapy
Stage 4 ovarian carcinoma widespread mets
Present meds
Hydromorphone 60 mg/h continuous SQ infusion (
had received total of 240 mg SQ additionally that
day)
Fentanyl for breakthrough pain ( 400 mcg / day)
Amitriptyline
Ketamine
Dexamethasone
Huge increase in opioids in the prior 2 weeks

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Case 1 Contd

In obvious distress
Agitated, confused
Myoclonic jerks
Pupils 4mm reactive
Afebrile
Labs
WBCs 11.6 CBC otherwise N
Coags N
Lytes N, urea 8.9, creatinine 110,
urea/creatinine 81 (N lt 70), glucose 9.5
Corrected Ca 2.49, Mg N
Albumin 26
LD 423 other liver enzymes essentially N
Urine conc otherwise N

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Case 1 contd

CT massive abdominal and retroperitoneal
adenopathy
Assessed as having severe neuropathic pain and
opioid induced neurotoxicity
Treatment on Day 1
Stopped hydromorphone, ketamine, amitriptyline
NS bolus 500 ml ? 250 ml/h x 2 hours then 125
ml/h
Furosemide 20 mg IV
Sufentanil 25 mcg SQ x 1
Sufentanil 10 mcg/h SQ
Methadone 2.5 mg po TID
Lorazepam 0.5-1 mg SL Q4H prn (used 4 doses /
day early in stay then little used)
Dexamethasone continued

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Case 1 contd

Feb 21 1730 h feeling much better jerking
improved
Feb 22 -much less pain sensorium cleared
- sufentanil inc. to 12 mcg/h SQ
- methadone inc. to 5 mg po BID
Feb 23-28- no evidence of neuroexcitation
- persisting pain
- steady inc. in both methadone and sufentanil
Feb 28 - Methadone 7.5 mg po TID
- Sufentanil 40 mcg/h
- Anesthesia consult

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Case 1 contd

Feb 28 Anesthesia consult constant severe pain
resistant to aggressive opioid management Pain
likely due to tumor involving lumbosacral plexus
- no change in systemic medications
- epidural marcaine 1.25 mg/ml
hydromorphone 60 mcg/ml
rate 10 ml/h
Mar 1 Improved pain control of low back and
right leg, but persisting higher in back

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Case 1- contd

Over the next week, generally good baseline pain
control apart from periodic exacerbations
Relatively stable doses of opioids from that
point
No further myoclonus, agitation, hyperalgesia
To attempt to treat the periodic exacerbations,
anesthesia started ketamine IV then ketamine in
epidural
March 6 generally comfortable, had a good night
March 9 Passed away peacefully

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Spectrum of Opioid-Induced Neurotoxicity
Seizures
Opioidtolerance
Mild myoclonus(eg. with sleeping)
Severe myoclonus
34
Case 2

Ms. W.P. 73 yo woman with metastatic NSCLC
Diagnosed early Oct. 2001
Seen Oct. 18/01 by oncology in community hospital
ER with low back pain, dyspnea
At that time morphine long-acting 200 mg bid
plus morphine 2.5 mg IV q3h (prn but given
regularly)
Morphine long-acting increased to 300 mg bid,
with plans for 300 mg tid, plus 5 mg IV q3h prn
Over the next 2 days became twitchy on morphine,
changed to hydromorphone infusion
Over the subsequent 2 days, hydromorphone
increased from a few mg/hr to 30 mg/hr, with no
improvement in distress
Increase in agitation, fluctuating LOC, non-stop
myoclonus

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Case 2 contd

Oct. 22/01 transferred to SBGH palliative care
On exam at time of transfer (approx 1330h)
Lethargic but easily rousable, disoriented,
restless.
Resps. approx 20, reg.
Pupils 3-4 mm, reactive
Generalized myoclonus non-stop
Normal electrolytes, calcium, urea, creatinine
Assessed as having severe opioid induced
neurotoxicity.

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Case 2 contd

Hydromorphone D/Cd
NS 500 ml IV bolus, followed by NS with KCl 10
mEq/l 250 ml/hr IV. (This was decreased to 200
ml/hr overnight, D/Cd Oct 23 1300h)
Furosemide 40 mg IV q8h
Lorazepam 0.5 mg IV push x1 dose _at_ 1345h
Sufentanil 5 µg IV push x1 dose _at_ 1425h
Sufentanil 10 µg/hr IV infusion started
mid-afternoon Oct. 22 ? 20 µg/hr Oct.
23Breakthrough sufentanil 25-50 µg SL q 30 min
prn. Received total breakthrough of 75 µg Oct. 22
and 250 µg Oct. 23
Marked improvement in myoclonus by 1700h Oct. 22

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Case 2 contd

Methadone 10 mg po bid added Oct 25 ? 15 mg po
bid Oct 26 at which time sufentanil D/Cd.
Good pain control
No neuroexcitation symptoms
Max methadone dose was 25 mg po bid, Nov. 07
Nov. 20 marked decline
No longer able to swallow methadone switched to
hydromorphone 6 mg SQ q4h
Died comfortably Nov. 24

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Consider the following

Hydromorphone 30 mg/hr SQ 720 mg/day
3600 mg/day SQ morphine if a 51 ratio used
7200 mg/day po morphineRipamonti et al J Clin
Oncol 1998 mg po Morphine/day
MorphineMethadone 30 90
3.7 1
90 300
7.75 1 gt 300
12.25 1
Calculated equivalence to 7200 mg/day po
morphine 588 mg/d po methadone
ie. throw out your opioid conversion tables with
opioid neurotoxic patients

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Opioid Induced Neurotoxicity

A substantial part of the current opioid had been
started to treat opioid induced
hyperalgesia/restlessness
That is the opioid was increased to treat its
own adverse effects
Significant tolerance to the offending opioid
that is not crossed over to alternative opioids
It is not possible to calculate dose
equivalencies of the new opioid do not use
conversion charts in these situations

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Summary