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editorial
. 2018 May 23;27(4):327–335. doi: 10.1017/S2045796018000239

Table 1.

Summary of the studies described in the manuscript

Article Study design Diagnosis Sample (M/F) Age (years old) CBD dosage/formulation CBD timing Augmentation Scales, test and measurements Main results
Zuardi et al. (1995) Case report Treatment-resistant SKZ 1 (0/1) 19 1500 mg/day of gelatin capsules (with powder CBD dissolved in corn oil) 4 weeks Diazepam co-medication allowed BPRS
IOSPI
UKU
Significant reduction of all items of BPRS score
No side effects
Zuardi et al. (2006) Case report Treatment-resistant SKZ 3 (3/0) 23
23
22
CBD in two daily doses, from 40 mg/day until 1280 mg/day 29 days / BPRS
PANSS-N
CGI
UKU
SAS
BARS
Mild or no symptoms improvements
No side effects
Zuardi et al. (2009) Open-label pilot study Parkinson disease with psychotic symptoms 6 (4/2) 58.8 ± 14.9 150 mg/day up to 400 mg/day of gelatin capsules (with powder CBD dissolved in corn oil) 4 weeks Median of 1050 mg/day of L-dopa BPRS
PPQ
UPDRS
CGI
MMSE
FAB
Significant reduction psychotic symptoms.
No side effects
Hallak et al. (2010) Double-blinded, placebo-controlled study SKZ 28 (18/10) More than 18 300 mg CBD, 600 mg CBD or placebo in gelatin capsules One single dose / BPRS
PANSS
SCWT
Single acute administration of CBD did not improve SCWT performances. Possible sedative effect with 600 mg dose
Leweke et al. (2012) Double-blinded, randomised, parallel-group, controlled clinical trial of CBD v. amisulpride SKZ or schizophreniform psychosis 20 (15/5) CBD group + 19 (17/2) amisulpride group 18–50 200 mg/day up to 800 mg/day CBD or amisulpride 4 weeks Lorazepam co-medication allowed BPRS
PANSS
EPS
CGI
SAS
Significant clinical improvement in both groups.
Anandamide and FAAH substrates levels higher in CBD group.
Fewer side effects in the CBD group
Leweke (2013) Double-blind, randomised, placebo-controlled, cross-over clinical trial pf CBD v. First-episode paranoid SKZ 29 NIA 600 mg/day CBD 14 days NIA NIA CBD improved psychotic symptoms compared with baseline
McGuire et al. (2018) Double-blind, randomised, placebo-controlled, parallel-group trial SKZ or a related psychotic disorder 43 (28/15) CBD group + 45 (23/22) placebo group 18–65 1000 mg/day CBD (10 mL of a 100 mg/mL oral solution) or placebo in two doses 6 weeks Antipsychotic medication PANSS
SANS
CGI GAF
BACS
SAS
Significant reduction of positive symptoms, better cognitive performance and overall functioning in CBD group
No significant side-effects. No correlations between CBD plasma levels and scale scores
Boggs et al. (2018) Double-blind, randomised, placebo-controlled, parallel group trial SKZ 18 (12/6) CBD group + 18 (13/5) Placebo group 18–65 600 mg/day oral CBD 6 weeks Antipsychotic medication MCCB
PANSS
No improvement in cognitive scores and no reduction of psychotic symptoms
Crippa et al. (2011) Double-blind, randomised, placebo-controlled, repeated measures, within-subjects cross-over trial Treatment-naïve generalised social anxiety disorder 10 (10/0) 20–33 400 mg CBD of gelatin capsules (with powder CBD dissolved in corn oil) One single dose / VAMS
SPECT
Significant reduction of subjective anxiety in CBD group
Functional activity changes in limbic and paralimbic cerebral regions in CBD group
No side effects
Bergamaschi et al. (2011) Double-blind, randomised, placebo-controlled, clinical trial Treatment-naïve generalised social anxiety disorder 12 (6/6) CBD group
12 (6/6) place group
12 (6/6) HC
600 mg CBD in gelatin capsules (with powder CBD dissolved in corn oil) One single dose / VAMS
SSPS
BSS
Significant reduction of anxiety symptoms, cognitive impairment and speech performance discomfort in CBD group
Zuardi et al. (2010) Case report Bipolar disorder type I, manic episode with psychotic features 2 (0/2) 25
17
600 mg CBD (up to 1200 mg/day) 25 days Olanzapine during the first 2 weeks BPRS
YMRSUKU
No significant symptoms improvements with CBD.
No side effects
Crippa et al. (2013) Case report Cannabis dependence and cannabis withdrawal syndrome 1 (0/1) 19 300 up to 600 mg on in gelatin capsules (with powder CBD dissolved in corn oil) 10 days / WDSM
WSC
BAI
BDI
Reduction of withdrawal, anxiety and dissociative symptoms
No significant effect on long-term cannabis dependence
Shannon and Opila-Lehman (2015) Case report Cannabis dependence, bipolar disorder 1 (1/0) 27 18 up to 24 mg CBD oil Prolonged over time / PSQI
HAM-A
CBD was effective in quitting cannabis abuse, in reducing anxiety symptoms and improving quality of life
Morgan et al. (2013) Double-blind, randomised, placebo-controlled clinical trial Tobacco use disorder 18 (12/6) CBD group
12 (6/6) placebo group
18–35 CBD (400 µg dose for each depress of the solution aerosol in the inhaler) via a pressurised metered dose inhaler 1 week / STAI
BDI
BIS
Significant reduction of cigarettes smoked in CBD group. No significant effects on craving. No side effects

BACS, Brief Assessment of Cognition in Schizophrenia; BAI, Beck Anxiety Inventory; BARS, Barnes Akathisia Rating Scale; BDI, Beck Depression Inventory; BIS, Behaviour Impulsivity Scale; BPRS, Brief Psychiatric Rating Scale; BSS, Bodily Symptoms Scale; CBD, cannabidiol; CGI, Global Clinical Impression Scale; EPS, Extrapyramidal Symptoms Rating Scale; FAAH, fatty acid amide hydrolase; FAB, Frontal Assessment Battery; GAF, Global Assessment of Functioning; Hamilton Anxiety Rating Scale; HC, healthy controls; IOPSI, Interactive Observation Scale for Psychiatric Inpatients; MCCB, Matrix Consensus Cognitive Battery; MMSE, Mini-Mental Status Examination; MWSC, Marijuana Withdrawal Symptom Checklist; NIA, no information available; PANSS-N, Negative Subscale of Positive and Negative Syndrome Scale; PPQ, Parkinson Psychosis Questionnaire; PSQI, Pittsburgh Sleep Quality Index; SANS, Scale for Assessment of Negative Symptoms; SAS, Social Anxiety Scale; SAS, Simpson-Angus Scale for Parkinson; SCWT, Stroop Color-Word Test; SKZ, schizophrenia; SPECT, single-photon emission computer tomography; SPSS, Self-Statements during Public Speaking Scale; STAI, Spielberger Trait Anxiety Inventory; UKU, UKU Side Effect Rating Scale; UPDRS, Unified Parkinson's Disease Rating Scale; VAMS, Visual Analogue Mood Scale; WDS, Withdrawal Discomfort Score; YMRS, Young Mania Rating Scale.