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Comparison of amitriptyline supplemented with pregabalin, pregabalin supplemented with amitriptyline, and duloxetine supplemented with pregabalin for the treatment of diabetic peripheral neuropathic pain (OPTION-DM): a multicentre, double-blind, randomised crossover trial.
Tesfaye, Solomon; Sloan, Gordon; Petrie, Jennifer; White, David; Bradburn, Mike; Julious, Stephen; Rajbhandari, Satyan; Sharma, Sanjeev; Rayman, Gerry; Gouni, Ravikanth; Alam, Uazman; Cooper, Cindy; Loban, Amanda; Sutherland, Katie; Glover, Rachel; Waterhouse, Simon; Turton, Emily; Horspool, Michelle; Gandhi, Rajiv; Maguire, Deirdre; Jude, Edward B; Ahmed, Syed H; Vas, Prashanth; Hariman, Christian; McDougall, Claire; Devers, Marion; Tsatlidis, Vasileios; Johnson, Martin; Rice, Andrew S C; Bouhassira, Didier; Bennett, David L; Selvarajah, Dinesh.
Afiliação
  • Tesfaye S; Diabetes Research Unit, Sheffield Teaching Hospitals NHS Foundation Trust, Sheffield, UK; School of Health and Related Research, and Department of Oncology and Metabolism, University of Sheffield, Sheffield, UK. Electronic address: solomon.tesfaye@nhs.net.
  • Sloan G; Diabetes Research Unit, Sheffield Teaching Hospitals NHS Foundation Trust, Sheffield, UK.
  • Petrie J; Clinical Trials Research Unit, University of Sheffield, Sheffield, UK.
  • White D; Clinical Trials Research Unit, University of Sheffield, Sheffield, UK.
  • Bradburn M; Clinical Trials Research Unit, University of Sheffield, Sheffield, UK.
  • Julious S; Medical Statistics Group, University of Sheffield, Sheffield, UK.
  • Rajbhandari S; Department of Diabetes, Lancashire Teaching Hospitals NHS Trust, Chorley, UK.
  • Sharma S; Diabetes and Endocrine Centre, East Suffolk and North Essex NHS Foundation Trust, Ipswich, UK.
  • Rayman G; Diabetes and Endocrine Centre, East Suffolk and North Essex NHS Foundation Trust, Ipswich, UK.
  • Gouni R; Diabetes and Endocrine Centre, Nottingham University Hospitals NHS Trust, Nottingham, UK.
  • Alam U; Department of Cardiovascular & Metabolic Medicine, Institute of Life Course and Medical Sciences, University of Liverpool, Liverpool, UK; Liverpool University Hospital NHS Foundation Trust, Liverpool, UK.
  • Cooper C; Clinical Trials Research Unit, University of Sheffield, Sheffield, UK.
  • Loban A; Clinical Trials Research Unit, University of Sheffield, Sheffield, UK.
  • Sutherland K; Clinical Trials Research Unit, University of Sheffield, Sheffield, UK.
  • Glover R; Clinical Trials Research Unit, University of Sheffield, Sheffield, UK.
  • Waterhouse S; Clinical Trials Research Unit, University of Sheffield, Sheffield, UK.
  • Turton E; Clinical Trials Research Unit, University of Sheffield, Sheffield, UK.
  • Horspool M; NHS Sheffield Clinical Commissioning Group, Sheffield, UK.
  • Gandhi R; Diabetes Research Unit, Sheffield Teaching Hospitals NHS Foundation Trust, Sheffield, UK.
  • Maguire D; Department of Diabetes and Endocrinology, Harrogate and District NHS Foundation Trust, Harrogate, UK.
  • Jude EB; Department of Diabetes and Endocrinology, Tameside and Glossop Integrated Care NHS Foundation Trust, Ashton under Lyne, UK; Division of Diabetes, Endocrinology & Gastroenterology, University of Manchester, Manchester, UK.
  • Ahmed SH; School of Medicine, University of Liverpool, Liverpool, UK; Department of Diabetes and Endocrinology, Countess of Chester Hospital NHS Foundation Trust, Chester, UK.
  • Vas P; Department of Diabetes, King's College Hospital NHS Foundation Trust, London, UK.
  • Hariman C; Department of Diabetes and Endocrinology, The Royal Wolverhampton NHS Trust, Wolverhampton, UK.
  • McDougall C; Department of Medicine, University Hospital Hairmyres, NHS Lanarkshire, Hairmyres, UK.
  • Devers M; Department of Diabetes, University Hospital Monklands, NHS Lanarkshire, Monklands, UK.
  • Tsatlidis V; Department of Endocrinology and Diabetes, Gateshead Health NHS Foundation Trust, Gateshead, UK.
  • Johnson M; St Pancras Clinical Research, London, UK.
  • Rice ASC; Pain Research, Department of Surgery and Cancer, Faculty of Medicine, Imperial College London, London, UK.
  • Bouhassira D; Inserm U987, APHP, UVSQ, Paris-Saclay University, Paris, France.
  • Bennett DL; Nuffield Department of Clinical Neurosciences, University of Oxford, Oxford, UK.
  • Selvarajah D; School of Health and Related Research, and Department of Oncology and Metabolism, University of Sheffield, Sheffield, UK.
Lancet ; 400(10353): 680-690, 2022 08 27.
Article em En | MEDLINE | ID: mdl-36007534
ABSTRACT

BACKGROUND:

Diabetic peripheral neuropathic pain (DPNP) is common and often distressing. Most guidelines recommend amitriptyline, duloxetine, pregabalin, or gabapentin as initial analgesic treatment for DPNP, but there is little comparative evidence on which one is best or whether they should be combined. We aimed to assess the efficacy and tolerability of different combinations of first-line drugs for treatment of DPNP.

METHODS:

OPTION-DM was a multicentre, randomised, double-blind, crossover trial in patients with DPNP with mean daily pain numerical rating scale (NRS) of 4 or higher (scale is 0-10) from 13 UK centres. Participants were randomly assigned (111111), with a predetermined randomisation schedule stratified by site using permuted blocks of size six or 12, to receive one of six ordered sequences of the three treatment pathways amitriptyline supplemented with pregabalin (A-P), pregabalin supplemented with amitriptyline (P-A), and duloxetine supplemented with pregabalin (D-P), each pathway lasting 16 weeks. Monotherapy was given for 6 weeks and was supplemented with the combination medication if there was suboptimal pain relief (NRS >3), reflecting current clinical practice. Both treatments were titrated towards maximum tolerated dose (75 mg per day for amitriptyline, 120 mg per day for duloxetine, and 600 mg per day for pregabalin). The primary outcome was the difference in 7-day average daily pain during the final week of each pathway. This trial is registered with ISRCTN, ISRCTN17545443.

FINDINGS:

Between Nov 14, 2017, and July 29, 2019, 252 patients were screened, 140 patients were randomly assigned, and 130 started a treatment pathway (with 84 completing at least two pathways) and were analysed for the primary outcome. The 7-day average NRS scores at week 16 decreased from a mean 6·6 (SD 1·5) at baseline to 3·3 (1·8) at week 16 in all three pathways. The mean difference was -0·1 (98·3% CI -0·5 to 0·3) for D-P versus A-P, -0·1 (-0·5 to 0·3) for P-A versus A-P, and 0·0 (-0·4 to 0·4) for P-A versus D-P, and thus not significant. Mean NRS reduction in patients on combination therapy was greater than in those who remained on monotherapy (1·0 [SD 1·3] vs 0·2 [1·5]). Adverse events were predictable for the monotherapies we observed a significant increase in dizziness in the P-A pathway, nausea in the D-P pathway, and dry mouth in the A-P pathway.

INTERPRETATION:

To our knowledge, this was the largest and longest ever, head-to-head, crossover neuropathic pain trial. We showed that all three treatment pathways and monotherapies had similar analgesic efficacy. Combination treatment was well tolerated and led to improved pain relief in patients with suboptimal pain control with a monotherapy.

FUNDING:

National Institute for Health Research (NIHR) Health Technology Assessment programme.
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Texto completo: 1 Base de dados: MEDLINE Assunto principal: Diabetes Mellitus / Neuropatias Diabéticas / Neuralgia Tipo de estudo: Clinical_trials / Guideline / Health_technology_assessment / Prognostic_studies Limite: Humans Idioma: En Ano de publicação: 2022 Tipo de documento: Article
Texto completo
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PubMed Links
Buscar no Google

Texto completo: 1 Base de dados: MEDLINE Assunto principal: Diabetes Mellitus / Neuropatias Diabéticas / Neuralgia Tipo de estudo: Clinical_trials / Guideline / Health_technology_assessment / Prognostic_studies Limite: Humans Idioma: En Ano de publicação: 2022 Tipo de documento: Article