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Research ArticlePraxis

PEER simplified decision aid: neuropathic pain treatment options in primary care

Karenn Chan, Danielle Perry, Adrienne J. Lindblad, Scott Garrison, Jamison Falk, James McCormack, Christina S. Korownyk, Jessica Kirkwood, Joey Ton, Betsy Thomas, Samantha Moe, Nicolas Dugré, Michael R. Kolber and G. Michael Allan
Canadian Family Physician May 2021, 67 (5) 347-349; DOI: https://doi.org/10.46747/cfp.6705347
Karenn Chan
Assistant Professor in the Department of Family Medicine at the University of Alberta (UA) in Edmonton.
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Danielle Perry
Clinical Evidence Expert for the College of Family Physicians of Canada (CFPC).
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Adrienne J. Lindblad
Clinical Evidence Expert Lead for the CFPC and Associate Clinical Professor in the Department of Family Medicine at UA.
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Scott Garrison
Associate Professor in the Department of Family Medicine at UA.
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Jamison Falk
Associate Professor in the College of Pharmacy at the University of Manitoba in Winnipeg.
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James McCormack
Professor in the Faculty of Pharmaceutical Sciences at the University of British Columbia in Vancouver.
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Christina S. Korownyk
Associate Professor in the Department of Family Medicine at UA.
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Jessica Kirkwood
Assistant Professor at UA.
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Joey Ton
Clinical Evidence Experts for the CFPC.
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Betsy Thomas
Clinical Evidence Experts for the CFPC.
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Samantha Moe
Clinical Evidence Experts for the CFPC.
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Nicolas Dugré
Pharmacist at the CIUSSS du Nord-de-l’Ile-de-Montréal and Clinical Associate Professor in the Faculty of Pharmacy at the University of Montreal in Quebec.
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Michael R. Kolber
Professor in the Department of Family Medicine at UA.
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G. Michael Allan
Director of Programs and Practice Support at the CFPC and Adjunct Professor in the Department of Family Medicine at UA.
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This decision aid is for clinicians for discussion of treatment options for patients living with neuropathic pain. It is derived from our accompanying systematic review of randomized controlled trials (RCTs; e130).1 Effectiveness data were generated from RCTs comparing active treatment to control. The evidence focuses on the proportion of patients achieving a clinically meaningful reduction in pain, generally defined as a 30% or more reduction in pain.

How was this tool was developed?

Icon arrays were developed using risk ratio estimates from meta-analyses of patients attaining a clinically meaningful improvement in pain. The control response rate was standardized to 29%, the approximate control response rate averaged for all included studies. The risk ratio for each intervention was applied to the average 29% control rate to attain the estimated benefit of that intervention. Standardizing control rates allows for easier comparison of estimated benefits of differing interventions. The estimates are from placebo-controlled trials and are not direct comparisons, so differences between interventions are approximations with some uncertainty.

Our systematic review identified the best available evidence for most interventions.1 For anticonvulsant medications, we included evidence for gabapentin, pregabalin, oxcarbazepine, and topiramate, with 90% of the studies examining gabapentin or pregabalin. All 4 anticonvulsant medications demonstrated similar efficacy; more adverse events were seen with oxcarbazepine and topiramate. For serotonin-norepinephrine reuptake inhibitors, we included duloxetine, venlafaxine, and desvenlafaxine, with 75% of the literature focused on duloxetine. Efficacy and adverse events were similar, regardless of the drug. To improve quality, we excluded partially reported crossover trials. This worked for other therapies, but in the case of tricyclic antidepressants, it left only 2 very low-quality RCTs with conflicting results. For clarity, we used a recent systematic review of tricyclic antidepressants2 and meta-analyzed responder data, including partially reported crossover trials (meta-analysis available from authors on request). We did not identify any relevant RCTs for exercise or topical lidocaine.

The decision aid

The tool is a 1-page summary (2-sided) of estimated effectiveness of treatment options for neuropathic pain; a printable version is available from CFPlus.* Accompanying the icon array (Figure 1)3 is a blue arrow that indicates the level of evidence associated with each of the listed interventions, based on the GRADE (Grading of Recommendations Assessment, Development and Evaluation) working group criteria,3 which reflects confidence in risk ratio estimates. Figure 21,2,4 includes classification of therapies by benefits and harms, withdrawals due to adverse events, typical adverse events, prescribing considerations, and estimated costs.

Figure 1
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Figure 1

PEER SIMPLIFIED DECISION AID / NEUROPATHIC PAIN

How many people will have their neuropathic pain meaningfully improved (≥30%) by different treatments?

Figure 2
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Figure 2

Treatment Options for Neuropathic Pain

We did not report on cannabinoids for neuropathic pain, as we have done so before.5 While this previous icon array does address neuropathic pain, it includes other types of neuropathic pain not included in this analysis, so effect estimates are not directly comparable. The tool is not a guideline, and the evidence was not assessed by an independent guideline committee. Information presented here will be combined with similar systematic reviews and tools on other types of chronic pain to inform future guideline development.

Footnotes

  • Competing interests

    None declared

  • * Easy-to-print versions of Figures 1 and 2 are available at www.cfp.ca. Go to the full text of the article online and click on the CFPlus tab.

  • This article is eligible for Mainpro+ certified Self-Learning credits. To earn credits, go to www.cfp.ca and click on the Mainpro+ link.

  • This article has been peer reviewed.

  • La traduction en français de cet article se trouve à www.cfp.ca dans la table des matières du numéro de mai 2021 à la page e111.

  • Copyright© the College of Family Physicians of Canada

References

  1. 1.↵
    1. Falk J,
    2. Thomas B,
    3. Kirkwood J,
    4. Korownyk CS,
    5. Lindblad AJ,
    6. Ton J, et al.
    PEER systematic review of randomized controlled trials. Management of neuropathic pain in primary care. Can Fam Physician 2021;67:e130-40.
    OpenUrlAbstract/FREE Full Text
  2. 2.↵
    1. Moore RA,
    2. Derry S,
    3. Aldington D,
    4. Cole P,
    5. Wiffen PJ.
    Amitriptyline for neuropathic pain in adults. Cochrane Database Syst Rev 2015;(7):CD008242.
  3. 3.↵
    1. Schünemann H,
    2. Brożek J,
    3. Guyatt G,
    4. Oxman A
    , editors. GRADE handbook: introduction to GRADE handbook. GRADE Working Group; 2013. Available from: guidelinedevelopment.org/handbook. Accessed 2021 Mar 26.
  4. 4.↵
    1. Moe S,
    2. Allan GM.
    What is the incidence of iatrogenic opioid use disorder? Tools for Practice #240. Edmonton, AB: Alberta College of Family Physicians; 2019. Available from: https://gomainpro.ca/wp-content/uploads/tools-for-practice/1563807207_incidenceoudtfp240fv.pdf. Accessed 2021 Mar 26.
  5. 5.↵
    1. Allan GM,
    2. Ramji J,
    3. Perry D,
    4. Ton J,
    5. Beahm NP,
    6. Crisp N, et al.
    Simplified guideline for prescribing medical cannabinoids in primary care. Can Fam Physician 2018;64:111-20 (Eng), e64-75 (Fr).
    OpenUrlAbstract/FREE Full Text
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Canadian Family Physician: 67 (5)
Canadian Family Physician
Vol. 67, Issue 5
1 May 2021
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PEER simplified decision aid: neuropathic pain treatment options in primary care
Karenn Chan, Danielle Perry, Adrienne J. Lindblad, Scott Garrison, Jamison Falk, James McCormack, Christina S. Korownyk, Jessica Kirkwood, Joey Ton, Betsy Thomas, Samantha Moe, Nicolas Dugré, Michael R. Kolber, G. Michael Allan
Canadian Family Physician May 2021, 67 (5) 347-349; DOI: 10.46747/cfp.6705347

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PEER simplified decision aid: neuropathic pain treatment options in primary care
Karenn Chan, Danielle Perry, Adrienne J. Lindblad, Scott Garrison, Jamison Falk, James McCormack, Christina S. Korownyk, Jessica Kirkwood, Joey Ton, Betsy Thomas, Samantha Moe, Nicolas Dugré, Michael R. Kolber, G. Michael Allan
Canadian Family Physician May 2021, 67 (5) 347-349; DOI: 10.46747/cfp.6705347
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