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. 2021 Jul 28;11(7):e047717. doi: 10.1136/bmjopen-2020-047717

Table 1.

Characteristics of included studies (n=18)

Author-year (country) Study design No of participants
(% prescribed opioids)
Type of chronic pain
(specific condition)
Age mean (SD) % Female Baseline opioid dose Follow-up duration Medical cannabis dose Analgesic cointervention Funding source
Fallon, 2017 study I
(multicentre trial*)43
Parallel arm RCT n=399; nabiximols (n=20), placebo (n=199)
(100%)
100% chronic cancer pain 59.8 (10.9) 43% Receiving opioid therapy of <500 MME/day (nabiximols group: 199 MME/day±131; placebo group: 207 MME/day±135) 5 weeks THC 27 mg/mL; CBD 25 mg/mL (maximum allowed daily dosage of 10 sprays) Patients were excluded if they planned to undergo clinical interventions that would affect pain Otsuka Pharmaceutical
Fallon, 2017 study II
(multicentre trial*)43
Parallel arm RCT n=206; nabiximols (n=103), placebo=103
(100%)
100% chronic cancer pain 61.5 (11.3) 49% Receiving opioid therapy of <500 MME/day (nabiximols: 212 MME/day±136; placebo: 209 MME/day±121) 5 weeks THC 27 mg/mL; CBD 25 mg/mL (maximum allowed daily dosage of 10 sprays) Patients were excluded if they planned to undergo clinical interventions that would affect pain Otsuka Pharmaceutical
Johnson, 2010 (multicentre trial*)44 Parallel arm RCT n=177; THC: CBD extract (n=60), THC extract (n=58), placebo (n=59)
(100%)
100% chronic cancer pain 60.2 (12.3) 46% Receiving opioid therapy for at least 1 week before enrolment (THC:CBD: 258MME/day±789; THC: 188 MME±234; placebo: 367±886) 2 weeks One spray:
2.7 mg THC/2.5 mg CBD.
The maximum permitted dose:
eight actuations over 3 hours and
48 actuations over 24-hours
Patients were excluded if they planned to undergo clinical interventions that would affect pain GW Pharmaceuticals
Lichtman, 2018 (multicentre*)45 Parallel arm RCT n=398; nabiximol (n=199), placebo (n=198)
(100%)
100% chronic cancer pain 60 (11.5) 46% Receiving opioid therapy of <500 MME/day (nabiximols: 193 MME/day±130; placebo: 186 MME/day±131) 5 weeks THC 27 mg/mL; CBD 25 mg/mL (maximum allowed daily dosage of 10 sprays per day) Patients were excluded if they planned to undergo clinical interventions that would affect pain Otsuka Pharmaceutical
Portenoy, 2012 (multicentre*)46 Parallel arm RCT n=360; nabiximols low dose (1–4 sprays/day) (n=91), medium dose (6–10 sprays/day) (n=88), high dose (11–16 sprays/day) (n=90), placebo (n=91)
(100%)
100% chronic cancer pain 58 (12.2) 48% Receiving opioid therapy of <500 MME/day (median was 120 MME/day; range 3–16 660) 5 weeks THC 27 mg/mL; CBD 25 mg/mL (maximum allowed daily dosage of 10 sprays per day) Patients were allowed to use breakthrough opioid analgesic as required GW Pharmaceuticals; Otsuka Pharmaceutical
Barlowe, 2019 (USA)47 Retrospective chart review Enrolled in MCP (n=34), not enrolled in MCP (n=19) (100%) 100% CNCP (chronic painful pancreatitis) 49.9 (10.5) 45% Not enrolled in MCP 183 MME/day±284; enrolled in MCP 190 MME/day±273 Range 4–297 weeks NR NR NR
Bellnier, 2018
(USA)48
One-arm observational study n=29
(100%)
90% CNCP; 10% cancer pain 61 (10) 65% Patients were receiving a median opioid dose of 79.94 MME/day 13 weeks 10 mg capsules of
THC/ CBD in a 1:1 ratio 3-times daily
NR NR
Capano, 2020
(USA)49
One-arm observational study n=131
(100%)
100% chronic pain (cancer and non-cancer) 56.1 (range: 39– 70) 68% Receiving at least 50 MME/day 8 weeks 30 mg CBD/1 mg THC NR Ananda Professional
Haroutounian, 2016 (Israel)50 One-arm observational study n=73
(35%)
93.2% CNCP; 6.8% chronic cancer pain 51.2 (15.4)† 38%† Receiving a median opioid dose of 60 MME/day (range 45–90) 26 weeks Cigarettes: 6% to 14% THC,
0.2% to 3.8% CBD;
Oral: 11% to 19% THC, 0.5% to 5.5% CBD
All participants were encouraged to attempt gradual dose reduction and possible discontinuation of other analgesics No-external funding
Maida, 2008 (Canada)51 Prospective cohort Enrolled in MCP (n=47), not enrolled in MCP (n=65)
(100%)
100% chronic cancer pain 69.7 (10.1) 42% nabilone treated:60 MME/day±64; nabilone untreated: 67 MME/day±101 4 weeks On average 1.79 mg two times daily nabilone Patients were permitted to use concomitant analgesics Valeant Pharmaceuticals Canada
Narang, 2008 (USA)52 One-arm observational study n=30
(100%)
100% CNCP Median=43.5 (range=21–67) 53% Receiving an average opioid dose of 68 MME/day±57 4 weeks Flexible dose schedule, dronabinol 5–20 mg three times daily NR Solvay Pharmaceuticals
O’Connell, 2019 (USA)53 One-arm observational study n=77 (100%) 100% CNCP 54.1 (range=26–76) 58% Receiving a mean opioid dose of 140 MME/day±184 26 weeks NR NR No industry funding
Pritchard, 2020
(USA)54
Retrospective cohort cannabis and opioids couse (n=22), opioids only (n=61)
(100%)
100% chronic cancer pain 53.1 (11.7) 23% MCP enrolled: 144 MME/day±129; MCP not enrolled: 119 MME/day±100 26 weeks NR NR No industry funding
Pawasarat, 2020
(USA)55
Retrospective chart review Enrolled in MCP (n=137), not enrolled in MCP (n=95)
(100%)
100% chronic cancer pain 58 (IQR:14.7) 56% MCP enrolled: median 45 MME/day, IQR=135; MCP not enrolled: median 97.5 MME/day, IQR=150 Between 39 and 52 weeks for MCP enrolled;<26 weeks for not enrolled NR NR No industry funding
Rod, 2019
(Canada)56
One-arm observational study n=600 100% chronic pain (cancer and non-cancer) NR NR Receiving a mean opioid dose of 120 MME/day (range 90–240 MME/day) 26 weeks CBD and THC ranged between 4% and 6%.
Doses related directly to the opioid taper.
All participants indicated readiness to reduce opioid dose and also received psychological supports (eg, CBT, mindfulness, relaxation) No external funding
Takakuwa, 2020
(USA)57
One-arm observational study n=61
(100%)
100% CNCP (back pain) 50 (11.4) 38% Receiving a median opioid dose of 21 MME/day Median of 6.4 years among patients who ceased opioids completely NR NR The Society of Cannabis Clinicians
Vigil, 2017
(USA)58
Retrospective chart review Enrolled in MCP (n=37), not enrolled (n=29)(100%) 100% CNCP
(90% back pain)
56.3 (11.8) 36% Maximum daily dosage of <200 MME/day
(enrolled in MCP: mean 24 MME/day±23; not enrolled in MCP: mean 16 MME/day±14)
52 weeks NR NR University of New Mexico Medical Cannabis
Research Fund
Yassin, 2019
(Israel)59
One-arm observational study n=31
(100%)
100% CNCP (fibromyalgia) 33.4 (12.3) 90% Receiving oxycodone 5 mg three times/day 26 weeks THC to CBD ratio was 1:4;
20 g/month for 3 months, increased up to 30 g/month at the end of 6 months
Patients were permitted to use standardised analgesic therapy (duloxetine 30 mg once daily and Targin
5/2.5 mg two times a day). All other opiates and atypical analgesics were stopped
NR

*In Belgium, Bulgaria, Czech Republic, Estonia, Germany, Hungary, Latvia, Lithuania, Poland, Romania, the UK and the USA.

†Based on the whole population including opioid users and non-users.

CBD, cannabidiol; CBT, cognitive behavioural therapy; CNCP, chronic non-cancer pain; FU, follow-up; MME, milligram morphine equivalent; NR, not reported; RCT, randomised controlled trial; THC, tetrahydrocannabinol.