What alternatives are there to the use of opioid analgesics in the treatment of chronic pain in light of existing evidence and its limitations?



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What alternatives are there to the use of opioid analgesics in the treatment of chronic pain in light of existing evidence and its limitations? Michael C. Rowbotham, MD Scientific Director California Pacific Medical Center Research Institute

Disclosures Abbott Sanofi Bristol Myers Squibb Allergan Xenoport Boehringer-Ingelheim NUVO Hind Health Care Depomed

Alternatives to opioid analgesics Drugs most rigorous criteria for efficacy Dietary factors not well studied, but potentially important Alpha lipoic acid, acetyl-l-carnitine Cognitive-Behavioral Therapy, mindfulness-based tx, educational and group programs Exercise regimens CAM approaches many types Lee and Raja, PAIN 2011; Bell et al, PAIN in press

Alternatives to opioid analgesics Device-based Tx (stimulators, pumps) Extremely costly initially and for maintenance Long term efficacy relative to drugs uncertain Nerve blocks Little prospectively gathered data on long-term benefit Epidural steroids widely used, even for spinal pain types where benefit has not been demonstrated Costly! High strength capsaicin application Effective from 2 weeks onward substantial initial pain worsening is a risk Administered in office - need to pretreat for procedure pain

Medication Considerations Selecting the proper medication Safety and tolerability in older persons Polypharmacy Onset of action Relieve patient s symptoms quickly Ease of use Dosing schedule Dosing consistency

Effective Drug Categories Antidepressants Anticonvulsants Topicals Opioids

Efficacy of Antidepressants Tricyclics: highly effective in most pain disorders; also block sodium channels Studies have important limitations SSRIs: no efficacy or reduced efficacy SNRIs: duloxetine, milnacipran, venlafaxine effective Duloxetine most intensively studied; consistent efficacy in trials

Tricyclic Antidepressants: Adverse Events Commonly reported AEs: Blurred vision Cognitive changes Constipation Dry mouth Orthostatic hypotension Sedation Sexual dysfunction Tachycardia Urinary retention WEIGHT GAIN Desipramine Nortriptyline Imipramine Doxepin Amitriptyline Caution: all tricyclic antidepressants and venlafaxine have a high fatality rate from overdose compared to SSRIs. AEs = adverse events. Mackin GA. J Hand Ther. 1997;10:96-109; Beers MH. Arch Intern Med. 1997;157:1531-1536; McCue RE. Clinics in Geriatric Medicine. 1992;8:323-334; Kapur S et al. JAMA. 1992;268:3441-5.

Anticonvulsants: A Large and Diverse Family Na+ channel blocking carbamazepine lamotrigine oxcarbazepine phenytoin topiramate zonisamide lacosamide (mexiletine, tocainamide, flecainide) Other mechanisms gabapentin pregabalin valproate clonazepam tiagabine levetiracetam barbiturates

Gabapentin and Pregabalin Both FDA approved for pain Anticonvulsants: alpha-2-delta subunit on neuronal calcium channels Requires active transport system for absorption across intestinal wall - high doses poorly absorbed Well tolerated; serious adverse effects rare dizziness and sedation common adjust dose for renal impairment No significant drug interactions Generic gabapentin available Gabapentin prodrug and gastric retention versions

Gabapentin for acute pain Effective for acute post-operative pain (>11 published studies) Single dose (900 mg) reduces acute zoster pain and allodynia 0% -10% -20% -30% -40% -50% * ** ** Placebo GBP -60% -70% ** ** ** ** ** ** ** -80% -90% -100% 0 0.5 1 1.5 2 2.5 3 3.5 4 4.5 5 5.5 6 Hours After Medication Administration * Wilcoxon: p<0.05 ** Wilcoxon: p<0.01 Berry and Petersen, Neurology 2005

Gabapentin in PHN Results (UK): Reduction in Pain Score as Early as 1 Week Mean Change ( SE) 0.0-0.5-1.0-1.5-2.0-2.5-3.0 * * * *P < 0.01 (for both doses of gabapentin) Gabapentin 1800 mg (n = 115) Gabapentin 2400 mg (n = 108) Placebo (n = 111) * * 0 1 2 3 4 5 6 7 Week * * Additional benefits of using doses greater than 1800 mg/day were not demonstrated Rice AS et al. Pain. 2001;94:215-224.

Topical vs Transdermal Drug Delivery Systems Topical (lidocaine patch 5%) Transdermal (fentanyl patch) Peripheral tissue activity Applied directly over painful site Insignificant serum levels Systemic side effects unlikely Systemic activity Applied away from painful site Serum levels necessary Systemic side effects

Topicals Lidocaine patch - protective vehicle; low systemic uptake; approved for PHN NSAID topicals several options Capsaicin OTC - neurotoxin selectively activates c-nociceptors to produce burning pain (may be severe with initial applications) Other drugs and compounded drug combinations available; data anecdotal; unclear if topical or transdermal action Benefit outside of neuropathic pain and OA uncertain

Does existing clinical trial data allow a fair comparison of opioids with non-opioids? Few studies directly compare the classes by using a crossover design or randomize across classes in a parallel design Raja and Gilron studies important examples, but are small Both indicate opioids more efficacious than a TCA or gabapentin Partially enriched enrollment in many opioid trials Subject populations may differ Many potential subjects unwilling to try opioids

Rational Polypharmacy Combine approaches with evidence of efficacy in controlled clinical trials Limited number of longer term prospective combination trials Avoid unfavorable drug interactions (kinetic/ae) Multiple drugs all producing sedation Avoid duplication Eliminate ineffective tx before starting new tx Therapies for which there is only anecdotal evidence should always be 2nd or 3rd line

Three Caveats How representative are the subjects in efficacy trials? How consistent are the results of trials? What proportion of the available data is accessible?

Response to sequential treatment trials and duotherapy in epilepsy Kwan and Brodie, NEJM 2000; 342:314-319 Likelihood of success no different if first drug old vs new Thank you to Ken Laxer

Fifteen Studies of Qutenza were reported to FDA

Snapshot and Scorecard: The RReACT Database 373 analgesic trials posted on ClinicalTrials.gov Thank you to Kaitlin Greene and Robert Dworkin PHN 93 trials 57 completed 36 have results 23 published in peer-reviewed literature (40%) 164 studies DPN 106 completed 72 have results 29 published in peer-reviewed literature (39%) 116 studies Fibromyalgia 66 completed 44 have results 29 published in peer-reviewed literature (44%)