Abstract
Background:
The mainstay of treatment for diabetic peripheral neuropathic pain is pharmacotherapy, but the current National Institute for Health and Care Excellence guideline is not based on robust evidence, as the treatments and their combinations have not been directly compared.
Objectives:
To determine the most clinically beneficial, cost-effective and tolerated treatment pathway for diabetic peripheral neuropathic pain.
Design:
A randomised crossover trial with health economic analysis.
Setting:
Twenty-one secondary care centres in the UK.
Participants:
Adults with diabetic peripheral neuropathic pain with a 7-day average self-rated pain score of ≥ 4 points (Numeric Rating Scale 0–10).
Interventions:
Participants were randomised to three commonly used treatment pathways: (1) amitriptyline supplemented with pregabalin, (2) duloxetine supplemented with pregabalin and (3) pregabalin supplemented with amitriptyline. Participants and research teams were blinded to treatment allocation, using over-encapsulated capsules and matching placebos. Site pharmacists were unblinded.
Outcomes:
The primary outcome was the difference in 7-day average 24-hour Numeric Rating Scale score between pathways, measured during the final week of each pathway. Secondary end points included 7-day average daily Numeric Rating Scale pain score at week 6 between monotherapies, quality of life (Short Form questionnaire-36 items), Hospital Anxiety and Depression Scale score, the proportion of patients achieving 30% and 50% pain reduction, Brief Pain Inventory – Modified Short Form items scores, Insomnia Severity Index score, Neuropathic Pain Symptom Inventory score, tolerability (scale 0–10), Patient Global Impression of Change score at week 16 and patients’ preferred treatment pathway at week 50. Adverse events and serious adverse events were recorded. A within-trial cost–utility analysis was carried out to compare treatment pathways using incremental costs per quality-adjusted life-years from an NHS and social care perspective.
Results:
A total of 140 participants were randomised from 13 UK centres, 130 of whom were included in the analyses. Pain score at week 16 was similar between the arms, with a mean difference of –0.1 points (98.3% confidence interval –0.5 to 0.3 points) for duloxetine supplemented with pregabalin compared with amitriptyline supplemented with pregabalin, a mean difference of –0.1 points (98.3% confidence interval –0.5 to 0.3 points) for pregabalin supplemented with amitriptyline compared with amitriptyline supplemented with pregabalin and a mean difference of 0.0 points (98.3% confidence interval –0.4 to 0.4 points) for pregabalin supplemented with amitriptyline compared with duloxetine supplemented with pregabalin. Results for tolerability, discontinuation and quality of life were similar. The adverse events were predictable for each drug. Combination therapy (weeks 6–16) was associated with a further reduction in Numeric Rating Scale pain score (mean 1.0 points, 98.3% confidence interval 0.6 to 1.3 points) compared with those who remained on monotherapy (mean 0.2 points, 98.3% confidence interval –0.1 to 0.5 points). The pregabalin supplemented with amitriptyline pathway had the fewest monotherapy discontinuations due to treatment-emergent adverse events and was most commonly preferred (most commonly preferred by participants: amitriptyline supplemented with pregabalin, 24%; duloxetine supplemented with pregabalin, 33%; pregabalin supplemented with amitriptyline, 43%; p = 0.26). No single pathway was superior in cost-effectiveness. The incremental gains in quality-adjusted life-years were small for each pathway comparison [amitriptyline supplemented with pregabalin compared with duloxetine supplemented with pregabalin –0.002 (95% confidence interval –0.011 to 0.007) quality-adjusted life-years, amitriptyline supplemented with pregabalin compared with pregabalin supplemented with amitriptyline –0.006 (95% confidence interval –0.002 to 0.014) quality-adjusted life-years and duloxetine supplemented with pregabalin compared with pregabalin supplemented with amitriptyline 0.007 (95% confidence interval 0.0002 to 0.015) quality-adjusted life-years] and incremental costs over 16 weeks were similar [amitriptyline supplemented with pregabalin compared with duloxetine supplemented with pregabalin −£113 (95% confidence interval −£381 to £90), amitriptyline supplemented with pregabalin compared with pregabalin supplemented with amitriptyline £155 (95% confidence interval −£37 to £625) and duloxetine supplemented with pregabalin compared with pregabalin supplemented with amitriptyline £141 (95% confidence interval −£13 to £398)].
Limitations:
Although there was no placebo arm, there is strong evidence for the use of each study medication from randomised placebo-controlled trials. The addition of a placebo arm would have increased the duration of this already long and demanding trial and it was not felt to be ethically justifiable.
Future work:
Future research should explore (1) variations in diabetic peripheral neuropathic pain management at the practice level, (2) how OPTION-DM (Optimal Pathway for TreatIng neurOpathic paiN in Diabetes Mellitus) trial findings can be best implemented, (3) why some patients respond to a particular drug and others do not and (4) what options there are for further treatments for those patients on combination treatment with inadequate pain relief.
Conclusions:
The three treatment pathways appear to give comparable patient outcomes at similar costs, suggesting that the optimal treatment may depend on patients’ preference in terms of side effects.
Trial registration:
The trial is registered as ISRCTN17545443 and EudraCT 2016-003146-89.
Funding:
This project was funded by the National Institute for Health and Care Research (NIHR) Health Technology Assessment programme, and will be published in full in Health Technology Assessment; Vol. 26, No. 39. See the NIHR Journals Library website for further project information.
About the Series
Health Technology Assessment
ISSN (Print): 1366-5278
ISSN (Electronic): 2046-4924
Declared competing interests of authors: Solomon Tesfaye reports honoraria as speaker fees from Wörwag Pharma (Stuttgart, Germany), Pfizer Inc. (Pfizer Inc., New York, NY, USA), Novo Nordisk (Bagsværd, Denmark), Merck & Co. Inc. (Kenilworth, NJ, USA), Eva Pharma (Cairo, Egypt), Hikma Pharmaceuticals plc (London, UK), Abbott Laboratories (Abbott Park, IL, USA), AstraZeneca (Cambridge, UK), Nevro (Redwood City, CA, USA), Procter & Gamble Health Limited (Mumbai, India), Astellas Pharma Inc. (Tokyo, Japan) and Berlin-Chemi (Berlin, Germany), and is on the advisory boards (from 2018 to present) of Bayer AG (Leverkusen, Germany), NeuroPn Therapeutics (Norcross, GA, USA), Wörwag Pharma, Angelini (Rome, Italy), Grünenthal (Aachen, Germany), TRIGOcare International GmbH (Wiehl, Germany), Nevro, Mitsubishi Tanabe Pharma Corporation (Osaka, Japan) and Confo Therapeutics (Gent, Belgium). Uazman Alam reports honoraria for educational meetings from Eli Lilly and Company (Indianapolis, IN, USA), Napp Pharmaceuticals Ltd (Cambridge, UK), Sanofi (Paris, France) and Boehringer Ingelheim (Ingelheim am Rhein, Germany). Edward Jude reports honoraria and research support from AstraZeneca, Bayer AG, Menarini (Florence, Italy), Napp Pharmaceuticals Ltd, Novo Nordisk and Sanofi. Syed Haris Ahmed reports honoraria for educational meetings from Novo Nordisk (Bagsværd, Denmark), Eli Lilly and Company (Indianapolis, IN, USA) and Sanofi (Paris, France). Prashanth Vas reports honoraria from Merck & Co. Inc. and Sanofi. Martin Johnson reports honoraria for advisory boards and speaker fees from Grünenthal (2015 to present), and is a co-chairperson, since 2014, of the Chronic Pain Policy Coalition (London, UK) and a council (2012 to present) and ordinary member of the British Pain Society (London, UK). Didier Bouhassira reports honoraria for consulting activities for Bayer AG, Grünenthal, Novartis Pharmaceuticals UK Ltd (London, UK) and Air Liquide (Paris, France). David L Bennett has acted as a consultant on behalf of Oxford University Innovation Limited (Oxford, UK) for AditumBio (San Francisco, CA, USA), Amgen Inc. (Thousand Oaks, CA, USA), Bristows LLP (London, UK), Latigo Biotherapeutics Inc. (Thousand Oaks, CA, USA), GlaxoSmithKline plc, Ionis Pharmaceuticals (Carlsbad, CA, USA), Eli Lilly and Company, OliPass (Gyeonggi, Republic of Korea), Regeneron Pharmaceuticals (Tarrytown, NY, USA) and Theranexus (Lyon, France) (2020–21). David L Bennett has received research funding from Eli Lilly and Company and AstraZeneca, and has received an industrial partnership grant from the Biotechnology and Biological Sciences Research Council (BBSRC) (Swindon, UK) and AstraZeneca. David L Bennett reports grants and contracts for a number of studies from the following: the UK Research and Innovation (Swindon, UK) (Versus MR/W002388/1), Medical Research Council (MRC) (MR/T020113/1), BBSRC (BB/S006788/1), Action Medical Research for Children (West Sussex, UK), MRC Research Grant, Wellcome Trust Senior Clinical Scientist Fellowship, Novo Nordisk Foundation (Hellerup, Denmark), European Union Horizon 2020, MRC Clinical Research Training Fellowship and Wellcome Trust Strategic Award. Dinesh Selvarajah reports membership of the advisory boards of Impeto Medical (Issy-les-Moulineaux, France) (2017), PelliTec Inc. (Chester, UK) (2020) and FeetMe Inc. (Paris, France) (2019). Cindy Cooper reports membership of the following committees: the National Institute for Health and Care Research (NIHR) Clinical Trial Unit (CTU) Support Funding Committee (2016 to present), NIHR CTU Standing Advisory Committee (2016–22), NIHR Programme Grant for Applied Research Subcommittee (2017–21) and Trial Steering Committees for other NIHR-funded trials.
Last reviewed: September 2021; Accepted: March 2022.
