Paracetamol, NSAIDS and opioid analgesics for chronic low back pain: a network meta‐analysis
Información
- DOI:
- https://doi.org/10.1002/14651858.CD013045Copiar DOI
- Base de datos:
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- Cochrane Database of Systematic Reviews
- Versión publicada:
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- 09 junio 2018see what's new
- Tipo:
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- Intervention
- Etapa:
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- Protocol
- Grupo Editorial Cochrane:
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Grupo Cochrane de Espalda y cuello
- Copyright:
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- Copyright © 2018 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd.
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Autores
Contributions of authors
MKB provided NMA methodology expertise and wrote the protocol.
AJM provided pharmacological and systematic review methodology expertise.
AN provided NMA methodology and statistical analysis expertise.
CGM, SK, CMW, NH, GLM, BMW, MH, NOC and MvT provided systematic review methodology and clinical area expertise.
JHM is the guarantor and provided clinical area, systematic review and NMA methodology expertise.
All authors read, contributed to and approved the final version of the manuscript.
Sources of support
Internal sources
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No sources of support supplied
External sources
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National Health and Medical Research Council, Australia.
Research Fellowship (CMW, SK), Principal Research Fellowship (RH, CGM, GLM)
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Australian Government Research Training Program Scholarship, Australia.
(MKB)
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UNSW Research Excellence Award, Australia.
(MKB)
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Neuroscience Research Australia PhD Candidature Supplementary Scholarship, Australia.
(MKB)
Declarations of interest
CGM and AJM are conducting an investigator‐initiated, NHMRC‐funded trial of opioids for acute LBP (OPAL). The OPAL trial has no funding from pharmaceutical companies. They have both received supplementary research funding from Pfizer and GlaxoSmithKline for two investigator‐initiated, NHMRC‐funded trials of paracetamol and pregabalin for low back pain (PACE & PRECISE).
GLM has received lecturing fees from Kaiser Permanente for their Physical Therapy Residency programme, and consultancy fees from workers' compensation boards in Australia, North America and Europe for advice on policy matters concerning acute back pain and persistent musculoskeletal pain states. GLM has received consultancy fees from Port Adelaide Football Club for professional services regarding pain and performance. GLM has received travel and consultancy fees from Arsenal Football Club for professional services regarding pain and performance. GLM has received travel support and expenses from the International Olympic Committee for committee roles focusing on pain management in elite sport. GLM receives guest lecturing fees from Noigroup Australasia and has received guest lecturing fees from Agile Physiotherapy (USA) and Results Physiotherapy (USA), for professional development courses. GLM receives speaker’s fees for lectures on pain and rehabilitation and royalties for books on pain and rehabilitation. GLM has received honoraria and travel support from Pfizer for two lectures and for participation in the ASIA Masterclass on Neuropathic Pain. These contributions did not mention drugs. GLM has also received travel support from Grünenthal to attend a European CRPS minimum standards of care summit. This contribution did not involve any drugs.
MKB has received travel support from the Chiropractor’s Association of Australia for speaking engagements unrelated to this topic.
MvT and CGM are on the Editorial Board of Cochrane Back and Neck. MvT was Co‐ordinating Editor until September 2017. Editors are required to conduct at least one Cochrane Review. This requirement ensures that they are aware of the processes and commitment needed to conduct reviews. None of the Editors are first authors. Any Editor who is a review author is excluded from editorial decisions on the review in which they are contributors.
BMW, MH, SK, NH, NOC, CMW, AN and JHM have no declarations.
This research project did not receive any specific grant from funding agencies in the public, commercial, or not‐for‐profit sectors.
Acknowledgements
Prof Georgia Salanti and A/Prof Andrea Cipriani for assistance with methodological development.
Dr Anna Chaimani for providing Stata code.
Dr Michel Rossignol, Dr Sarah Nevitt, Prof Roger Chou and Marilyn Walsh for their constructive feedback on the manuscript.
Version history
| Published | Title | Stage | Authors | Version |
| 2018 Jun 09 | Paracetamol, NSAIDS and opioid analgesics for chronic low back pain: a network meta‐analysis | Protocol | Matthew K Bagg, Andrew J McLachlan, Christopher G Maher, Steven J Kamper, Christopher M Williams, Nicholas Henschke, Benedict M Wand, G L Moseley, Markus Hübscher, Neil E O'Connell, Maurits W van Tulder, Adriani Nikolakopoulou, James H McAuley | |
PICO
All theoretically possible comparisons between the opioid analgesic interventions of interest. NSAIDs and paracetamol are not included for the sake of simplicity.
| Bias Domain | Source of Bias | PossibleAnswers |
| Selection | (1) Was the method of randomization adequate? | Yes/No/Unsure |
| Selection | (2) Was the treatment allocation concealed? | Yes/No/Unsure |
| Performance | (3) Was the patient blinded to the intervention? | Yes/No/Unsure |
| Performance | (4) Was the care provider blinded to the intervention? | Yes/No/Unsure |
| Detection | (5) Was the outcome assessor blinded to the intervention? | Yes/No/Unsure |
| Attrition | (6) Was the drop‐out rate described and acceptable? | Yes/No/Unsure |
| Attrition | (7) Were all randomized participants analyzed in the group to which they were allocated? | Yes/No/Unsure |
| Reporting | (8) Are reports of the study free of suggestion of selective outcome reporting? | Yes/No/Unsure |
| Selection | (9) Were the groups similar at baseline regarding the most important prognostic indicators? | Yes/No/Unsure |
| Performance | (10) Were cointerventions avoided or similar? | Yes/No/Unsure |
| Performance | (11) Was the compliance acceptable in all groups? | Yes/No/Unsure |
| Detection | (12) Was the timing of the outcome assessment similar in all groups? | Yes/No/Unsure |
| Other | (13) Are other sources of potential bias unlikely? | Yes/No/Unsure |
| 1 | A random (unpredictable) assignment sequence. Examples of adequate methods are coin toss (for studies with 2 groups), rolling a dice (for studies with 2 or more groups), drawing of balls of different colours, drawing of ballots with the study group labels from a dark bag, computer‐generated random sequence, preordered sealed envelopes, sequentially‐ordered vials, telephone call to a central office, and preordered list of treatment assignments. Examples of inadequate methods are: alternation, birth date, social insurance/security number, date in which they are invited to participate in the study, and hospital registration number. |
| 2 | Assignment generated by an independent person not responsible for determining the eligibility of the patients. |
| 3 | Index and control groups are indistinguishable for the patients or if the success of blinding was tested among the patients and it was successful. |
| 4 | Index and control groups are indistinguishable for the care providers or if the success of blinding was tested among the care providers and it was successful. |
| 5 | Adequacy of blinding should be assessed for each primary outcome separately. This item should be scored “yes” if the success of blinding was tested among the outcome assessors and it was successful or: |
| 6 | The number of participants who were included in the study but did not complete the observation period or were not included in the analysis must be described and reasons given. If the percentage of withdrawals and drop‐outs does not exceed 20% for short‐term follow‐up and 30% for long‐term follow‐up and does not lead to substantial bias a ‘‘yes’’ is scored. (N.B. these percentages are arbitrary, not supported by literature). |
| 7 | All randomized patients are reported/analyzed in the group they were allocated to by randomization for the most important moments of effect measurement (minus missing values) irrespective of noncompliance and cointerventions. |
| 8 | All the results from all prespecified outcomes have been adequately reported in the published report of the trial. This information is either obtained by comparing the protocol and the report, or in the absence of the protocol, assessing that the published report includes enough information to make this judgment. |
| 9 | Groups have to be similar at baseline regarding demographic factors, duration and severity of complaints, percentage of patients with neurological symptoms, and value of main outcome measure(s). |
| 10 | If there were no cointerventions or they were similar between the index and control groups. |
| 11 | The reviewer determines if the compliance with the interventions is acceptable, based on the reported intensity, duration, number and frequency of sessions for both the index intervention and control intervention(s). For example, physiotherapy treatment is usually administered for several sessions; therefore it is necessary to assess how many sessions each patient attended. For single‐session interventions (e.g. surgery), this item is irrelevant. |
| 12 | Timing of outcome assessment should be identical for all intervention groups and for all primary outcome measures. |
| 13 | Other types of biases. |
| Paracetamol, NSAIDs and opioid analgesics for chronic low back pain: network meta‐analysis | |||
| Patient or population: non‐specific chronic low back pain Settings: primary and secondary care, (additional detail unknown at protocol stage) Intervention: paracetamol, NSAIDs or opioid analgesics Comparison: intervention A vs intervention B, of X possible comparisons (unknown at protocol stage) | |||
| Outcomes | Outcome type | Outcome measure | Comments |
| Pain | Continuous | Pain intensity on 0 to 100 mm VAS | Measured at end of treatment |
| Safety | Dichotomous | Proportion of participants that experience a serious adverse event during treatment | |
| GRADE Working Group grades of evidence | |||
