Hallucinations and other psychotic symptoms in response to methylphenidate in children and adolescents with attention-deficit/hyperactivity disorder: a Cochrane systematic review with meta-analysis and trial sequential analysis.

BACKGROUND: There is little evidence in the literature on the association between methylphenidate treatment and psychotic symptoms in children and adolescents with attention-deficit/hyperactivity disorder (ADHD).
OBJECTIVE: We examine the occurrence of psychotic symptoms during methylphenidate treatment of children and adolescents with ADHD. The data arise from our two Cochrane systematic reviews on methylphenidate, reported elsewhere.
METHODS: Electronic databases were searched up to January 2016 (for observational studies) and March 2017 (for randomized trials). We summarized data as risk ratios and pooled prevalences. Trial Sequential Analysis was used to control for random errors. We assessed the risk of bias and the quality of evidence according to Cochrane guidelines.
RESULTS: Ten randomized trials (1103 participants), 17 non-randomized studies (76,237 participants) and 12 patient reports or series (18 patients) were identified. In the randomized trials, there was no significant difference in the risk of developing psychotic symptoms [10 of 654 (pooled prevalence, 2.5%) methylphenidate versus 1 of 508 (pooled prevalence, 1.7%) placebo patients; risk ratio, 2.07; 95% confidence interval, 0.58 to 7.35]. Nine of 10 trials had a high risk of bias, and according to the Trial Sequential Analysis, the required information size was not achieved, that is, the meta-analysis was considerably underpowered. There were 873 instances of psychotic symptoms in the non-randomized studies among 55,603 participants (pooled prevalence, 1.2%; 95% confidence interval, 0.7 to 2.4). In the comparative cohort study, methylphenidate significantly increased the risk for any psychotic disorder by 36% (risk ratio, 1.36; 95% confidence interval, 1.17 to 1.57). The overall risk of bias was rated as critical for this study.
CONCLUSIONS: Because of sparse data and low quality of evidence, we cannot confirm or refute whether methylphenidate increases the risk of psychotic symptoms in children and adolescents with ADHD. This possible adverse event may affect 1.1% to 2.5%, and physicians, patients and caregivers should be aware of this to ensure proper treatment in case of occurrence during methylphenidate treatment.

Introduction

Attention-deficit/hyperactivity disorder (ADHD) is a neurodevelopmental disorder with a worldwide prevalence of around 5.3% among children and adolescents (1). The diagnosis is made by a clinical evaluation of whether a child has presented excessive inattention, hyperactivity and impulsivity. These must be present before six years [International Statistical Classification of Diseases and Related Health Problems, 10th Revision (ICD-10)] or 12 years [Diagnostic and Statistical Manual of Mental Disorders, Fifth Edition (DSM-5)] and impairing his or her functioning and/or development. ADHD symptoms may persist into adulthood and 15% of the patients continue to fulfil the full criteria for ADHD at the age of 25 (2,3). Psychostimulants, including methylphenidate, are the recommended first-choice drug treatment for ADHD (4-7). Because so many children and adolescents are prescribed methyl-phenidate (8-10), it is important that the risk of adverse events is better understood.

By definition, a substance/medication-induced psychotic disorder must be present during treatment or appear soon after withdrawal (DSM-5), within 2 weeks [ICD-10 (F15.5)] or a month (DSM-IV-TR) depending on the diagnostic criteria used. Psychosis reflects an experience of impaired reality through symptoms such as hallucinations and delusions. However, psychotic symptoms are not always associated with a psychotic disorder and can occur in individuals who have an awareness that their experience does not reflect reality (11).

Psychotic symptoms have been reported in children and adolescents with ADHD prescribed methylphenidate in clinical trials and as patient reports (12). Clinical guidelines recommend a reduction or a withdrawal of methylphenidate if psychotic symptoms occur (13,14) and caution in prescribing methylphenidate in patients with a history of psychotic episodes or a family history of psychotic disorder (15).

To the best of our knowledge, no systematic review of the literature specifically examining psychotic symptoms in relation to methylphenidate use has been performed.

Three publications provide evidence- and expert-based guidance on ADHD medication adverse events, including psychotic symptoms (4,15,16). All three publications are largely based on the same meta-analyses carried out by the Food and Drug Administration (FDA) in 2006 to 2009 (12,17). The FDA examined the occurrence of psychotic symptoms and mania during drug therapy for ADHD (i.e., amphetamine, dextroamphetamine, atomoxetine, modafinil and methylphenidate) by reviewing clinical trial data as well as post-marketing spontaneous reports. Data were provided by manufacturers of ADHD medication and the FDA Adverse Event Reporting System safety database (12). The methodology used resulted in the exclusive inclusion of trials funded by pharmaceutical companies (12). Relevant trials conducted by independent research groups were not sought, and the restricted use of data sources could have influenced the data collection and ultimately the meta-analysis. Study selection of only industry-sponsored trials could have created an additional risk of bias (18). Furthermore, the risk of random errors, risk of bias and trial methodological quality were not assessed systematically. Despite these limitations, the report noted the absence of psychosis and mania events in placebo-treated patients and therefore advised that drugs for ADHD may be associated with such symptoms (17).

We have performed two Cochrane systematic reviews on the efficacy and safety of methylphenidate use in children and adolescents with ADHD, and we sought to avoid any methodological flaws and shortcomings (19-21). In the first review, we included randomized clinical trials (19). In the second review, we included observational studies, the methylphenidate group from randomized clinical trials without placebo or no intervention comparator group, follow-up periods from randomized clinical trials and patient reports (21).

This article highlights one of the many safety outcomes in the two Cochrane publications (19-21) and attempts to establish whether psychotic symptoms occur as an adverse event to methyl-phenidate treatment in randomized clinical trials and observational studies of children and adolescents with ADHD.

Methods

The design and methodology of our study followed the Cochrane Handbook for Systematic Reviews of Interventions (22) and PRISMA guidelines (23,24), which we have described in the protocols (25,26).

Data sources and search criteria

The literature search was carried out and updated for the two Cochrane systematic reviews (19,21) up to February 2015. CINAHL, Cochrane Library, EMBASE, MEDLINE, PsycINFO, ISI CPCI databases, Clinical Trials and ICTRP were searched from origin without restrictions in terms of language, year of publication or type of publication (25,26). Review articles were searched for additional, potentially relevant references. Similarly, the bibliography of a sample of included articles was searched for additional studies. In January 2016, we updated the search for observational studies, and included a “grey literature” search. Unpublished data were also sought from the United States FDA and the European Medicines Agency (21). To collect all new relevant randomized clinical trials, the literature search for randomized clinical trials was updated in March 2017 for the present review.

Where necessary, the authors of the articles included were contacted for additional data. Some authors provided additional, potentially relevant articles. Pharmaceutical companies were contacted for relevant published and unpublished data. Each step of the review was conducted by two review authors, apart from assessment and processing of the final literature search in March 2017, which was conducted by the first author.

Participant inclusion criteria and study selection

After removal of duplicates, authors screened titles and abstracts of the retrieved records. Full-text articles of records judged to be potentially relevant were assessed for eligibility according to our inclusion criteria. Eligibility criteria included children and adolescents with a diagnosis of hyperkinetic disorder or ADHD according to ICD or DSM diagnostic criteria, respectively (ICD-9, DSM-III and newer). At least 75% of the study participants had to be younger than 19 years and the mean age had to be younger than 19 years. We included trials irrespective of comorbidities, but at least 75% of the participants were required to have a normal intellectual capacity (IQ≥70 points). Study designs considered eligible for the assessment of safety were randomized clinical trials on methylphenidate with placebo or no intervention as a comparator, non-randomized studies and patient reports. Furthermore, the methylphenidate group from randomized clinical trials without placebo or no intervention comparator group as well as follow-up periods from randomized clinical trials were included in the observational study category (19,21).

For inclusion in the present review, co-medication was only accepted as over-the-counter drugs or if the co-medication was identical in the intervention and the control group.

Psychotic symptoms

To obtain data on any psychotic phenomena, we included articles reporting assessment and/or occurrence of “psychosis”, “psychotic”, “hallucination” and “delusion”. Only reports of symptoms during methylphenidate treatment or up to a month after withdrawal qualified for inclusion in the present review. Formal assessment of psychotic symptoms was not mandatory, and we accepted both spontaneous reports as well as formal assessment, for example, the Pittsburgh Side Effect Rating Scale, which includes hallucinations as an item (27).

Data extraction and quality assessment

Data were extracted using a template to facilitate a standardized extraction method between researchers. In our analyses, reports of psychotic symptoms leading to withdrawal were not separated from reports of psychotic symptoms in the observed study population. The risk of bias in randomized trials was rated at the study level using the Cochrane Collaboration Handbook for Systematic Reviews (22). We defined low risk of bias trials as trials that had a low risk of bias in all domains. We considered trials with one or more unclear or high risk of bias domains as trials with a high risk of bias (25). This procedure was based on the fact that randomized clinical trials with an unclear or a high risk of bias tend to overestimate benefits and underestimate harms compared with trials with a low risk of bias (28-34). Risk of bias in non-randomized studies, that is, comparative cohort studies and patient–control studies with data, were rated using the ROBINS-I tool (Risk Of Bias In Non-randomized Studies - of Interventions) (35). We assessed and graded the evidence according to Grading of Recommendations Assessment, Development, and Evaluation (GRADE) for a high risk of bias, imprecision, indirectness, heterogeneity and publication bias (36). We report our methodology in greater detail in our Cochrane reviews (19,21).

Data synthesis and statistical analysis

Data from parallel group and cross-over trials were summarized as risk ratios with 95% confidence intervals using the inverse variance method. We combined data from cross-over trials and parallel group trials. Because it might lead to a unit of analysis error, when cross-over trials are analysed as parallel group trials, we carried out a subgroup analysis of study designs. Whenever a cross-over trial reported data on psychotic symptoms in more than one of the groups exposed to methylphenidate, we combined the groups if the patients did not appear in more than one of the groups, otherwise we included data from the group with the highest dose exposure. Furthermore, we carried out a subgroup analysis for dose. For this, we defined low dosage treatment as ≤20 mg/day or ≤0.6 mg/kg/day and moderate/high dosage treatment as >20 mg/day or >0.6 mg/kg/day (19). We also carried out a subgroup analysis on the type of methylphenidate formulation. Here, we compared immediate-release with extended-release inclusive osmotic release oral system and methylphenidate transdermal system. Furthermore, we planned to carry out subgroup analyses on comorbidity and sex. We carried out a sensitivity analysis on age by excluding studies including young adults defined as study participants older than 15 years. We used the random-effect model as the primary method and the fixed-effect model as a sensitivity analysis (37). When carrying out a meta-analysis, a required information size should be estimated to better identify whether an apparent lack of effect may be because of inadequate data just as an a priori sample size calculation is performed for a single randomized clinical trial (38,39). For this, we used Trial Sequential Analysis, which combines the calculation of a required information size with trial sequential monitoring thresholds for benefit, harm or futility (39-41). Furthermore, we planned to assess whether there may be publication bias among randomized clinical trials by testing for funnel plot asymmetry.

Data from comparative cohort studies were summarized as risk ratios with 95% confidence interval using the inverse variance method. The occurrence of psychotic symptoms was calculated as pooled prevalences with 95% confidence intervals in six analyses. We report the pooled prevalence for the methylphenidate and the placebo group in the randomized clinical trials separately, the non-randomized studies and a “grand total” of all non-randomized studies and the methylphenidate group in randomized clinical trials. Furthermore, the pooled prevalence was calculated for two of the study designs included in the non-randomized study category, that is, cohort studies and the methylphenidate group in randomized clinical trials without placebo or no intervention comparator. We also calculated the pooled annual incidence of psychotic symptoms in non-randomized studies.

Data from patient reports were reported qualitatively, that is, number of patients experiencing psychotic symptoms and type of psychotic symptom.

Data were analysed using the program Comprehensive Meta Analysis (42) and the software Review Manager (43).

Results

A total of 14,334 records were retrieved in the literature searches, and 2736 records were considered potentially eligible after screening. After full-text assessments of these 2736 records, 80 articles describing 27 studies (10 randomized trials and 17 non-randomized studies) and 12 patient reports or series were included in the present review (Figure 1). Two studies were included on the basis of their published protocols; however, the results of the studies have still not been published (44,45). No data on psychotic symptoms were obtained from unpublished trials. Four hundred and twelve studies included in the Cochrane reviews on the efficacy and safety of methylphenidate (from the literature searches up to January 2016) did not report assessment or occurrence of psychotic symptoms.

FIGURE 1.

PRISMA flow diagram (24)

Included studies

We included 10 randomized clinical trials [four parallel group trials (46-50) and six cross-over trials (51-57)] totalling 1103 participants, 17 non-randomized studies (49,58-75) totalling 76,237 participants and 12 patient reports or small series describing 18 patients (76-88).

Randomized clinical trials

Table 1 shows the characteristics of the included studies, that is, number, age, sex and methylphenidate-naïvety of the participants; methylphenidate type, dose and dosage regimen; assessment; and type and number of psychotic symptoms. Two trials were designed as summer treatment programs (52,53), one trial used a laboratory classroom design (54) and the remaining were carried out in outpatient settings. Five trials excluded patients with comorbid psychotic disorder, schizophrenia or similar diagnoses (46,47,50,54,55). Two trials only included participants with comorbidity, that is, velocardiofacial syndrome (49) and non-nicotine substance use disorder (50). One trial excluded patients with a history of serious adverse reactions to methylphenidate or lack of response to methylphenidate (54).

TABLE 1.

Characteristics of included randomized clinical trials

Study ID, country	Study design	N	Age range Mean (SD) (years)	Male [n (%)]	MPH-naïve [n (%)]	MPH type, mean daily dose Dosage regimen	Time of MPH intervention	Mode of assessment	Type and number of psychotic events
Becker 2016/Froehlich 2015, USA	Cross-over	163	7-118.41 (1.24)	117 (72)	163 (100)	MPH-OROS<25 kg: 18/27/36 mg>25 kg: 18/36/54 mgOnce daily	3 weeks	Pittsburgh Side Effect Rating Scale, Parent rated	Hallucination Placebo: n=0/16318 mg: n=1/16327 mg: n=1/3136 mg: n=4/16354 mg: n=5/132
Buitelaar 1996, The Netherlands	Cross-over	52	6-139.29 (1.63)	46 (88)	52 (100)	MPH-IR, 20 mgTwice daily (at breakfast and at noon)	4 weeks	Modified Stimulant Drug Side Effects Rating scale, Parent rated	Interim analysis Hallucination: n=1
Childress 2009, NCT-00301236, USA	Parallel	253	6-128.7 (1.84)	163 (64)	175 (69)	MPH-ER, 10/20/30 mg (3 parallel groups)Once daily in the morning	5 weeks	Regular monitoring of serious adverse events	Tactile hallucination: n=1 (30 mg)
Palumbo 2008/Daviss 2008, NCT-00031395, USA	Parallel	122	7-129.5 (1.6)	98 (80)	57 (47)	MPH-IR, 30.2 mg 1 to 3 times daily (in the morning, noon and at 4 p.m.)	12 weeks	Pittsburgh Side Effect Rating Scale, Parent and teacher rated. Spontaneous self-reports.	Groups without co-intervention hallucination: n=0/59
Green 2011, NCT-00768820, Israel	Parallel	34	5-2011.1 (3.7)	20 (59)	21 (62)	MPH-IR, 15.7 mg 1 dose	1 day	Spontaneous reports	Psychotic symptoms: n=0
Pelham 1999, USA, Summer Treatment Program 1988	Cross-over	21	6-1210.3 (1.9)	19 (90)	7 (33)	MPH-IR, 0.9/0.75/0.3 mg/kg 1 to 3 times daily (morning, noon and afternoon at 3:30 p.m.)	1day×3 (placebo: 2 daysx3)	Pittsburgh Side Effect Rating Scale. Parent, teacher, and counselor rated	Hallucination: n=1
Pelham 2005, USA, Summer Treatment Program	Cross-over	36	6-139.6 (NA)	33 (92)	26 (72)	MTS, 0.45/0.9/1.8 mg/hWorn at least 12 hours dailyApplication time once daily (at 6 or 7 a.m.)	1 day×2	Pittsburgh Side Effect Rating Scale. Parent, teacher, and counselor rated	Hallucination: n=0
Riggs 2011, NCT-00264797, USA	Parallel	303	13-18 16.5 (1.3)	239 (79)	NA	MPH-OROS, 68 mgOnce daily in the morning	16 weeks	Systematic assessment of serious adverse events	Psychotic disorder: n=1
Schachar 2008, USA	Cross-over	18	6-1511.3 (2.2)	15[*] (88)	NA	MPH-IR or MPH-ER, 31.2 mg 1 to 2 times daily (morning- and lunch-time dose)	1 week	Spontaneous reporting	Psychosis: n=1
Waxmonsky 2008, NCT-00050622, USA, Summer Treatment Program	Cross-over	101	5-128.35 (2.05)	82 (81)	NA	MPH-IR, 15/30/54 mgThrice daily (7:45 a.m., 11:45 a.m. and 3:45 p.m.)	1day×3–4×3	Pittsburgh Side Effect Rating Scale. Staff and parent rated	NA

ER, extended-release; MPH, methylphenidate; MTS, MPH transdermal system; n, study participants; NA, not available; OROS, osmotic release oral system; IR, immediate-release

The sex of one patient is not stated

The median age for the randomized trials was 9.50 years and the interquartile range was 8.70 to 10.50 years. Across trials, 26% to 100% of the participants were diagnosed with ADHD combined subtype, 20% to 74% with the inattentive subtype, and 0% to 4% with the hyperactive-impulsive subtype. All randomized clinical trials used placebo as a comparator. Three of the six cross-over trials switched interventions daily (52,53,55) and only one cross-over trial included a wash-out period between the interventions (51). Six of the 10 randomized trials used rating scales including an item focusing on psychotic symptoms, that is, visual and auditory hallucinations (47,51-53,55,56), two trials assessed serious adverse effects without further specification (46,50) and two trials recorded spontaneous reports (49,54). Figure 2 presents the forest plot of the meta-analysis of randomized clinical trials. Only one of 10 trials was rated as having a low risk of bias (56). The remaining trials were rated as having a high risk of bias because of vested interest and inadequate information to assess whether the method used could induce bias (see Figure 2). The quality of evidence from the randomized clinical trials assessed according to GRADE guidelines was low owing to a high risk of bias and imprecision.

FIGURE 2.

Risk ratio of nine randomized clinical trials comparing methylphenidate versus placebo for patients with ADHD.

The following risk of bias items were rated as low (green), unclear (yellow) or high risk of bias (red): A: Random sequence generation (selection bias). B: Allocation concealment (selection bias). C: Blinding of participants and personnel (performance bias). D: Blinding of outcome assessment (detection bias). E: Incomplete outcome data (attrition bias). F: Selective reporting (reporting bias). G: Vested interest. C and D are for a number of trials assessed as without risk of bias, but because of prevalent and easily recognizable adverse events of methylphenidate, this assessment may well be wrong (19). CI, confidence interval; IV, inverse variance; MPH, methylphenidate; Random, random-effect model.

The meta-analysis yielded 10 of 654 (pooled prevalence, 2.5%; 95% confidence interval, 1.4 to 4.3) methylphenidate patients versus 1 of 508 (pooled prevalence, 1.7%; 95% confidence interval, 0.7 to 4.0) placebo patients with psychotic symptoms (risk ratio, 2.07; 95% confidence interval, 0.58 to 7.35) (see Figure 2). The authors of one trial (55) reported assessment of hallucinations, but data were not available and therefore only nine trials were included in the meta-analysis.

Findings using a fixed-effect model were similar (risk ratio, 2.07; 95% confidence interval, 0.58 to 7.35). The combination of data from parallel group and cross-over trials was tested in a subgroup analysis (see Figure 2), and no significant difference was found between the parallel group trials (risk ratio, 1.78; 95% confidence interval, 0.19 to 16.96) and the cross-over trials (risk ratio, 2.22; 95% confidence interval, 0.48 to 10.28), and the degree of inconsistency across trials in the analysis was 0%. The only reported psychotic episode in the placebo group was in a cross-over trial without any wash-out period between interventions (54). A sensitivity analysis was carried out without this trial (54), but the results were comparable (risk ratio, 2.96; 95% confidence interval, 0.74 to 11.81). Furthermore, we carried out subgroup-analyses for methylphenidate dose and formulation, but there was no statistical difference between low and moderate/high dose of methylphenidate groups: p=0.95 (Figure 3) or between methylphenidate immediate-release and methylphenidate extended-release/osmotic release oral system/transdermal system: p=0.60. The sensitivity analysis of age yielded comparable results with (risk ratio, 2.07; 95% confidence interval, 0.58 to 7.35) and without trials including young adults (49,50) (risk ratio, 1.93; 95% confidence interval, 0.49 to 7.67).

FIGURE 3.

Risk ratio of nine randomized clinical trials comparing methylphenidate versus placebo. Subgroup analysis of dose. Low dose: ≤20 mg/day or ≤0.6 mg/kg/day methylphenidate. Moderate/high dose: >20 mg/day or >0.6 mg/kg/day methylphenidate. CI, confidence interval; IV, inverse variance; MPH, methylphenidate; Random, random-effect model.

We used Trial Sequential Analysis to control the risks of random errors because of sparse data. We calculated the diversity-adjusted required information size by using data from the four parallel group trials that were able to provide data (649 participants), a type 1 error of 5%, a type 2 error of 20%, an assumed control group risk of psychotic symptoms of 2%, a relative risk reduction or increase of 50% and the diversity of the meta-analysis (0%) (Figure 4). With these variables, the diversity-adjusted required information size was 4639 participants, and the meta-analysis is thus considerably underpowered, having only achieved 14.0% (649/4639) of the diversity-adjusted required information size. The unadjusted conventional intervention effect estimate was 1.77 (95% confidence interval, 0.16 to 19.35) using a constant of 0.5 for zero event handling. The Trial Sequential Analysis-adjusted confidence interval, however, ranged from 0.00 to 30,803.

FIGURE 4.

Trial Sequential Analysis of parallel group trials. The diversity-adjusted required information size to demonstrate or reject a relative risk reduction or an increase of 50% with a control group risk of psychotic symptoms of 2%, an alpha of 5%, a beta of 20% and a diversity of 0% is 4639 patients (red vertical dashed line). The red vertical lines to the left represent the trial sequential monitoring boundaries for benefit and harm and the red dashed outward-sloping lines to the right represent the futility boundaries. The horizontal solid blue line is the cumulative Z-curve, showing that only 14.0% (649/4639) of the diversity-adjusted required information size has been accrued. a, alpha; b, beta; D, diversity; DARIS, diversity-adjusted required information size; RRR, relative risk reduction.

Non-randomized studies

Seven of the 17 non-randomized studies were prospective cohort studies (60,63,65-67,71,72,74,75). Three studies were randomized clinical trials without placebo or no-intervention comparators and therefore assessed as prospective cohort studies by only including the methylphenidate groups (58,59,70). One study was a follow-up of a randomized clinical trial where all participants continued methylphenidate treatment, and, therefore, the follow-up period was assessed as a prospective cohort study (49). There were four retrospective cohort studies (61,62,64,73), of which one was a comparative cohort study (73). One retrospective self-controlled patient series study design was included, where psychotic events among patients during periods with no drug exposure were compared with psychotic events during methylphenidate treatment periods (69). One cross-sectional study was included (68).

Study characteristics are presented in Table 2. All studies were carried out in outpatient clinics, except one study, which only included hospitalized patients (64). Comorbid schizophrenia, psychotic disorder or psychiatric disorder were exclusion criteria in two-thirds of the studies (58-60,63,65,66,70,71,73-75). Five studies only included patients with comorbid disorders, including schizophrenia (64), comorbid conduct disorder or oppositional-defiant disorder (59), severe mood dysregulation (60), sleeping difficulties (58) and velocardiofacial syndrome (49). One study only included patients with parents with severe mental illness (68). In the studies, 17.4% to 100% of the patients had the ADHD combined subtype, 11.6% to 70.2% had the inattentive subtype and 0.8% to 55% had the hyperactive-impulsive subtype. The median age for the non-randomized studies was 9.50 years and the interquartile range was 9.20 to 10.49 years.

TABLE 2.

Characteristics of included non-randomised studies

Study ID, country	N	Age range mean (SD) (years)	Male [n (%)]	MPH-naïve [n (%)]	MPH type, mean daily dose Dosage regimen	Time of intervention	Mode of assessment	Type and number of psychotic events
Ashkenasi 2011, NCT00989950, USA	26	6-129.3(1.95)	19(73)	NA	MTS, 10 ➔ max 30 mg (optimal dose)Applied once daily in the morningWorn for 9, 10, 11, and 12 h/day in 1 week each	Titration +4 weeks maintenance	Spontaneous reporting	Withdrawal due to hallucinations n=1
Arnold 2015, TOSCA study, NCT00796302,USA	168	6-128.89(2.01)	129(77)	NA	MPH-OROS, ➔ 44.8 mgOnce daily	3 weeks titration +6 weeks maintenance	NA	Hallucinations n=0/156 in 3 weeks (0/70 in 9 weeks)Delusions n=0/156 in 3 weeks (0/70 in 9 weeks)
Baweja 2016,USA	NA	NANA(NA)	NA	NA	MPH[*], NANA	6 weeks	Pittsburgh Side Effects Rating Scale	Hallucinations n=NA
Cherland 1999, Canada	98	4-17NA(NA)	NA	NA	MPH[*], NADose range: 5-80 mgNA	21 months	Spontaneous reporting	Psychotic effects n=7/96
Cortese 2015,Italy	1426	6-1810.55(2.75)	1247(87)	NA	MPH-IR, 18.3 mg2-3 times daily	up to 5 years	A structured form including any psychiatric symptomatology	Hallucination n=2
Didoni 2011, Italy	34	6-1710.7(2.7)	28(82)	34 (100)	MPH-IR, 39.9 mg 2-3 times daily.	> 1 year	Parents were requested in advance to report any adverse events during follow-up visits	Psychotic symptoms n=0
Elman 1998, Israel	5	NA NA (NA)	NA	NA	MPH[*], NANA	NA	NA	n=0
Findling 2009, NCT-00151957, USA	326	6-129.2(1.9)	212 (65)	∼ 0 (∼ 0)	MTS, 10➔15➔20➔30 mgApplied once daily (∼7 am)Worn for ∼9 hours (∼4 pm)	12 months	Systematic assessment	Psychosis/mania n=3
Green 2011, NCT-00768820, Israel	16	5-20NA(NA)	NA	0 (0)	MPH[*], NANA	6 months	Spontaneous reports	Psychotic symptoms n=0
Lee 2013/NA 2013, Republic of Korea, NCT01060150	55	12-1814.33(1.54)	43(78)	NA	MPH-OROS, 45.78 mgOnce daily	12 weeks	Adverse event checklist and general questioning	Hallucination n=0/55
	121	12-1813.8(1.49)	93(77)	NA	54.53 mgOnce daily	12 weeks	Adverse event checklist and general questioning	Withdrawal due to hallucinations n=1/121
MacKenzie 2016, Canada	141+MPH:NA	6-21NA(NA)	67(48)	NA	MPH[*], NANA	>12 months	Schizophrenia proneness instrument-child and youth version and structured interview for prodromal syndrome	Psychotic symptoms: Patients, +mph: n=6/NAControl, -mph: n=4/16
Man 2016, Hong Kong	76	6-19NA(NA)	NA	NA	MPH-IR and –ER, NANA	Mean: 2.17 years	Psychotic disorder or hallucination diagnostic code in the Clinical Data Analysis and Reporting System	Baseline period (no drug): n=NA Exposed period: n=NA
Mohammadi 2004, Iran	16	6-148.87(2.47)	11(69)	16 (100)	MPH[*], 1 mg/kgNA	6 weeks	NA	Hallucination, delusion n=0
Remschmidt 2005/Hoare 2005, UK and Germany	89	6-16NA(NA)	NA	0 (0)	MPH-OROS, 18, 36 or 54 mgOnce daily	1 year	NA	Delusion n=1 (18 mg)
Shyu 2015, Taiwan	ADHD: 73,049	NA9.4(3.3)	58,293(80)	NA	MPH[*], NANA	5 months – 12 years	Schizophrenia spectrum disorders based on insurance status, outpatient and hospitalization claims databases	Psychotic disorder:+MPH: 856/52,646 (1.6%)-MPH: 229/19,125 (1.2%)
	ADHD+MP H:53,600(73%)							Schizophrenia:+MPH: 452/52,752 (0.9%)-MPH: 120/19,119 (0.6)
Su 2015, China	239	6-169.2(2.02)	203(85)	NA	MPH-OROS, 18➔ 36 ➔54 mgOnce daily	8-week titration phase	Treatment-emergent adverse events were recorded throughout the study	Hallucination n=1
Wilens 2005, USA	407	6-139.2(1.8)	338(83)	0 (0)	MPH-OROS, 35.2➔44.2 mgOnce daily	21-24 months	Systematic assessment, parent rated	Withdrawal due to hallucinations n=1

Note. ➔, titrated to; MPH, methylphenidate; MTS, MPH transdermal system; n, study participants; NA, not available; OROS, osmotic release oral system; IR, immediate-release.

Type of methylphenidate formulation not available

The assessment of psychotic symptoms varied across studies. Rating scales including items focusing on psychotic symptoms were used in two studies (60,68). In one of these studies, structured interviews for prodromal syndrome was also used (68). A structured form including any psychiatric symptomatology was used in one study (62). In two database studies, a diagnostic code of schizophrenia spectrum disorders, psychotic disorders or hallucination was used (69,73). In the rest of the studies, the assessment varied from a systematic assessment of adverse events without further specification to recording of spontaneous reports.

In the non-randomized studies included, 873 instances of psychotic symptoms, including psychotic disorder, hallucinations, delusions and psychosis/mania, were reported to occur during methylphenidate treatment out of a total of 55,603 patients (pooled prevalence, 1.2%; 95% confidence interval, 0.7 to 2.4) (Figure 5). The meta-analysis was based on 14 studies as data from three studies were not available (60,68,69). There was no significant difference in the pooled prevalence in the cohort studies (1.1%; 95% confidence interval, 0.5 to 2.3) (61-67,71-75) compared with the methylphenidate group in the randomized clinical trials without placebo or no intervention comparator (1.9%; 95% confidence interval, 0.4 to 7.8) (58,59,70). The pooled annual incidence in the non-randomized studies was 2.2% (95% confidence interval, 0.2 to 4.1) on the basis of 12 studies with a total of 54,172 patients and 23,375.35 person-years because two studies did not report useable treatment durations (62,64). In the comparative cohort study, methylphenidate was associated with an increased risk for any psychotic disorder of 36% (risk ratio, 1.36; 95% confidence interval, 1.17 to 1.57) (73). The overall risk of bias was rated as critical for this study (Table 3) (73). Risk of bias assessment was only possible for one included study, that is the comparative cohort study (73), since it is a prerequisite for using ROBINS-I that the studies are comparative (35). Non-comparative studies are of critical risk of bias mostly due to confounding factors and therefore we considered all these studies as of critical risk of bias. The quality of evidence assessed according to GRADE guidelines was low owing to study design and a critical risk of bias.

FIGURE 5.

Prevalence of psychotic symptoms in non-randomized studies. CI, confidence interval

TABLE 3.

Risk of bias in non-randomised studies

	Shyu 2015
Bias due to confounding	Critical
Bias in selection of participants into the study	Moderate
Bias in classification of interventions	Moderate
Bias due to deviations from intended interventions	Critical
Bias due to missing data	Critical
Bias in measurement of outcomes	Serious
Bias in selection of the reported result	No information
Risk of bias judgement	Critical

The “grand total” pooled prevalence summarizing data from the non-randomized study category (58,59,61-67,70-75) and the methylphenidate group in the randomized clinical trials, that is, with placebo as a comparator (46-54,56,57), was 1.8% (95% confidence interval, 1.2 to 2.8).

Patient reports

In the 12 patient reports describing 18 patients (Table 4), 57.9% had ADHD combined subtype, 10.5% had the inattentive subtype and 5.3% had the hyperactive-impulsive subtype.

TABLE 4.

Characteristics of included patient reports

Study ID, country	N	Age, (years)	Sex	MPH-naïve (n)	MPH type, mean daily dose	Time of intervention	Type and number of psychotic events
Aguilera-Albesa 2010, Spain	2	6	F	NA	50% MPH-IR/50% MPH-ER, 10➔20 mgOnce daily	4 days	Hallucinations: n=2
		8	M	NA	MPH-ER, 18 mgOnce daily	2 days
Coignoux 2009, France	1	14	M	NA	MPH-ER, 54 mgOnce daily in the morning	6 months	Psychotic symptoms: n=1
Fernández-Fernández 2011, Spain	1	10	M	0	MPH-ER, 1.2 mg/kgOnce daily	1 week	Psychosis: n=1
Goetz 2011, Czech Republic	1	7	F	0	MPH-OROS, 18 mgOnce daily	2.5 months	Hallucination: n=1
Gross-Tsur 2004, Israel	3	7	M	NA	MPH[*], 7.5 mgOnce daily	1 year	Hallucinations: n=3
		12	M	NA	MPH[*], 10 mgOnce daily	Short period
		7.5	M	NA	MPH[*], 7.5 mgOnce daily	Months
Halevy 2009, Israel	1	8	M	1	MPH[*], 10 mgNA	Days	Hallucination: n=1
Herguner 2015, Turkey	1	6	M	NA	MPH-OROS, 18 mg[†]NA	2 months	Hallucination: n=1
Irmak 2014, Turkey	1	9	M	1	MPH[*], ➔1mg/kgNA	NA	Hallucination: n=1
Porfirio 2011, Italy	1	11	M	1	MPH-IR, 30 mgTwice daily	3 years	Hallucination: n=1
Rashid 2007, USA	1	10	M	0	MPH-IR, 20➔30 mgTwice daily	2 days	Hallucination: n=1
Shibib 2009, UK	4	14	F	1	MPH-ER, 30 mgOnce daily	4 months	Psychosis: n=4Hallucinations: n=3-4
		8	M	1	MPH-IR, 5➔20 mgTwice daily	7 days
		10	M	0	MPH-ER, 36➔54 mgOnce daily	3 weeks
		14	M	0	MPH-ER, 18 mgNA	24 hours
Tomás Vila 2010, Spain	1	10	M	0	50% MPH-IR/50% MPH-ER, 30 mgNA	2 weeks	Hallucination: n=1

Note. ➔, titrated to; ER, extended-release; F, female; M, male; MPH, methylphenidate; n: study participants; NA, not available; IR: immediate-release; OROS, osmotic release oral system

Type of methylphenidate formulation not available

The hallucinations started when acetaminophen suspension (120 mg/day) was administered in addition to methylphenidate and resolved after withdrawal of acetaminophen

Sixteen patients developed new psychotic symptoms during methylphenidate treatment and two patients experienced exacerbation of pre-existing psychotic symptoms, that is, chronic pattern of partial somatic hallucinations (83) and comorbid schizotypal personality disorder and infantile psychosis (77). The newly developed psychotic symptoms reported were primarily hallucinations, including visual, auditory and tactile hallucinations. The duration of methylphenidate treatment until the development of psychotic symptoms varied from 1 day to 3 years. Time from ingestion of methylphenidate to initiation of psychotic symptoms varied from 1 hour to 1 day. The duration of psychotic symptoms varied from 2 hours to 1 day, except for one patient, who had psychotic symptoms for 1 week coinciding with the co-administration of acetaminophen (88). The psychotic symptoms remitted upon methylphenidate withdrawal in 16 of 16 patients. In two of four patients, a re-challenge with methylphenidate was followed by the recurrence of symptoms (80,81). Furthermore, eight patients were reported to be followed up between 3 months and 3 years after the occurrence of psychotic symptoms (77,79,80,82,83,88), and only one patient continued to have symptoms (77). At follow-up, he was still receiving methylphenidate and was diagnosed with schizophrenia.

The quality of evidence from the patient reports assessed according to GRADE guidelines was very low owing to the study design.

Discussion

The data included here are a subset of data from the most comprehensive systematic reviews of methylphenidate to date (19,21). Despite this, relatively few studies assessed or reported psychotic symptoms.

Only nine of 185 randomized clinical trials and 23 of 259 non-randomized studies and patient reports of methylphenidate in children and adolescents with ADHD reported assessment of psychotic symptoms. One randomized clinical trial and six non-randomized studies and patient reports of psychotic symptoms were identified from the updating search in March 2017. Psychotic symptoms in relation to methylphenidate treatment have occasionally been reported since 1967 (12) and because of the relatively infrequent reports in the literature, it is fair to assume that serious reporting bias exists. We sought to obtain supplemental data from published and unpublished trials through correspondence with pharmaceutical companies, without success. Because of the sparse number of trials included in the meta-analysis, we did not construct a funnel plot. Psychotic symptoms only occurred in six randomized trials (two parallel, four cross-over) and therefore the test power would be too small to distinguish chance from real asymmetry (22).

The evidence that our present results are based on is of low and very low quality according to our assessment following GRADE guidelines and may be prone to bias.

Meta-analysis showed no difference in the risk of psychotic symptoms between the methylphenidate and the placebo groups in the randomized clinical trials (risk ratio, 2.07; 95% confidence interval, 0.58 to 7.35). It is worth noting that the only episode of psychotic symptoms in the placebo group occurred in a cross-over trial without wash-out periods (54), which makes the event dubious. However, the sensitivity analysis without this trial showed comparable results. The combination of data from parallel and cross-over trials was tested in another subgroup analysis and no statistically significant difference was present. A sensitivity analysis on age excluding trials including study participants older than 15 years showed comparable results. A subgroup analysis on dose was carried out showing no statistically significant difference in the occurrence of psychotic symptoms in the low-dose group compared with the moderate/high-dose group. Similarly, a subgroup analysis of methylphenidate formulation showed no statistically significant difference between the methylphenidate immediate-release and the methylphenidate extended-release/osmotic release oral system/transdermal system. It was not possible to carry out subgroup analyses, involving diagnostic criteria, comorbidity or sex because of the limited available data. No data from the first period of cross-over trials were available and thus could not be included in the Trial Sequential Analysis. Our meta-analysis of parallel trials was considerably underpowered according to the Trial Sequential Analysis, having only achieved 14.0% of the diversity-adjusted required information size. The result of the Trial Sequential Analysis highlights that the absence of evidence of an association in our analysis is not evidence suggesting that no association exists. Our results are primarily based on trials at high risk of bias (9/10) and accordingly low-quality evidence. However, the high risk of bias ought not necessarily to be interpreted as adding uncertainty about the occurrence of the reported psychotic symptoms, but rather uncertainty about the low frequency of the occurrence. In fact, the high risk of bias, including vested interest, may be a reason for under-reporting of psychotic symptoms (18,28-34). Furthermore, psychotic symptoms during methylphenidate treatment might not be reported if it is not judged to be an adverse event, but rather a natural occurring phenomenon or symptoms of comorbidity. Reporting bias in the studies included would lead to an underestimation of the prevalence of psychotic symptoms. However, 412 studies included in the two Cochrane systematic reviews (19,21) did not report assessment or occurrence of psychotic symptoms and were excluded from this study. If psychotic symptoms were not reported because they did not occur, the exclusion of the studies might have led to an overestimation of prevalence.

In the hope of finding supplemental important data to the randomized trials, we chose to include non-randomized studies. The risk of bias was critical in the one non-randomized study that could be rated (owing to study designs). This comparative cohort study showed a significantly increased risk of any psychotic disorder with methylphenidate (risk ratio, 1.36; 95% confidence interval, 1.17 to 1.57). As the authors themselves speculate, the patients exposed to methylphenidate might have had a higher symptom severity than the patients not exposed to methylphenidate. An underlining psychotic disorder might develop in time, especially for the patient group with a higher symptom severity, and therefore might not have been caused by methylphenidate treatment, but rather the full development of the disorder itself. Furthermore, because of the study design, the authors could not control for substance use disorders, which could have also confounded the results. Exposure to cannabis, alcohol and other psychoactive drugs is known to be associated with a significantly higher prevalence of subclinical psychosis (11). These limitations are difficult to avoid in non-randomized studies.

The pooled prevalence of psychotic symptoms during methylphenidate treatment in the randomized clinical trials (2.5%; 95% confidence interval, 1.4 to 4.3) was not different from the pooled prevalence in the non-randomized studies (1.2%; 95% confidence interval, 0.7 to 2.4). Estimates from both study designs were smaller than the reported prevalence in the general population [17% for children and 7.5% for adolescents (89)]. However, the same applied for the pooled prevalence in the placebo group in the randomized clinical trials (1.7%; 95% confidence interval, 0.7 to 4.0) and the prevalence in the group without methylphenidate exposure in the comparative cohort study (1.2%, 229/19,125). This might be explained by the way in which psychotic symptoms were evaluated. Nine of 27 studies included in our review used a structured form or rating scales, including items focusing on psychotic symptoms, that is, visual and auditory hallucinations. In the remaining studies, adverse events were assessed by general questioning or recording of spontaneous reports, which are both insufficient and inadequate. Only one study used structured interviews (68). Rating scales and structured interviews are much more sensitive than general questioning about adverse events and recording of spontaneous reports of adverse events, and the proportions reported here might therefore be underestimates of the true value. In the meta-analysis of prevalence in the general population (89), psychotic symptoms were assessed using clinical interviews and questions of whether the child/adolescent ever hears voices or sounds that no one else can hear. A clinical interview is the gold standard for assessing the presence and severity of psychotic symptoms, but is resource-demanding. Screening with self-report questionnaires entails a risk of overestimating the prevalence of psychotic symptoms because of a high rate of false positives (89). However, the above question on auditory hallucinations shows good sensitivity, specificity as well as positive and negative predictive value for psychotic symptoms in general (90), and ought to be included in adverse effect rating scales.

The quality of patient reports is considered very low and by including patient reports in a review a trade-off is made between being all-inclusive and not knowing whether unreliable information is republished (22). Consequently, patient reports can hardly contribute to the causality, but might point towards an association. The percentage of methylphenidate-naïve participants varied considerably (0% to 100%) between studies and the duration of methylphenidate treatment to the occurrence of psychotic symptoms in patient reports varied from 1 day to 3 years. Accordingly, if psychotic symptoms occur as an adverse event, the available data do not suggest whether such symptoms occur in the short or long term.

Genetic studies have shown a possible common heritability of ADHD and schizophrenia, but whether those findings can influence the occurrence of psychotic symptoms in methylphenidate users remain unclear. A Danish study reported an increased relative risk of 4.3 for schizophrenia in adults with ADHD compared with the general population (91). In a nationwide Taiwanese cohort, children with ADHD had an increased risk of developing any psychotic disorder (adjusted hazard ratio, 5.2) or schizophrenia (adjusted hazard ratio, 4.65) compared with non-ADHD controls (73). A small but significant genetic susceptibility was found in rare chromosomal variants (92), but needs to be replicated. Similarly, genetic variations at SNAP25 can be associated differentially with both psychiatric conditions (93).

Approximately two-thirds (16/27) of the included studies, randomized as well as non-randomized, had comorbid psychotic disorders as an exclusion criterion, making the results less generalizable to ADHD patients with known susceptibility to psychotic symptoms. However, in a retrospective cohort study with five patients in a prodromal schizophrenic state, none developed psychotic symptoms in response to methylphenidate (64). In contrast, methylphenidate exacerbated psychotic symptoms in two patient reports (77,83). Methylphenidate mediates its effect through the dopaminergic and noradrenergic neurotransmitter systems, and increases the concentration of dopamine in the synaptic cleft (94). Hyperdopaminergic activity in patients with schizophrenia is believed to cause psychotic symptoms (95). Thus, one might believe that methylphenidate may unmask psychotic symptoms in genetically vulnerable patients through a synergistic mechanism. If this is so, the occurrence of psychotic symptoms during methylphenidate treatment in clinical studies, with the exclusion of these vulnerable patients, would not seem to reflect the occurrence of psychotic symptoms in the population of ADHD patients in a clinical setting.

Results in relation to current knowledge

This systematic review provides an overview of the existing literature and the results are in line with the FDA report (12). Psychotic symptoms occurring during methylphenidate treatment may represent an adverse event. No significant difference in the risk of developing psychotic symptoms was present in the randomized clinical trials, but according to the Trial Sequential Analysis, the meta-analysis was considerably underpowered. In the included comparative cohort study, methylphenidate significantly increased the risk of any psychotic disorder by 36%. The prevalence of psychotic symptoms obtained in our review from the non-randomized studies was much lower than the corresponding numbers for the general population and this was considered to be because of methodological differences, in particular, assessment strategy, but could also be because of bias and low quality of evidence.

Implications for future research

Future high-quality, long-term randomized placebo-controlled trials assessing methylphenidate-induced psychotic symptoms concurrently with beneficial effects are needed and in particular trials with large sample sizes, inclusion of patients vulnerable to psychotic adverse events and assessment of psychotic symptoms by clinical interviews or standardized rating scales. Long duration of placebo administration and inclusion of patients vulnerable to psychotic adverse events might be ethically questionable and therefore also non-randomized studies may be of great importance.

An adverse effect rating scale of methylphenidate should include assessment of psychotic symptoms, for example, a question of whether the child/adolescent ever hears voices or sounds that no one else can hear. Furthermore, the severity and implication for the child of psychotic symptoms ought to be assessed in a clinical interview as psychotic symptoms are not necessarily associated with a psychotic disorder (11).

Conclusions

Because of sparse data and low quality of evidence, we cannot confirm or refute whether methylphenidate increases the occurrence of psychotic symptoms in children and adolescents with ADHD.

It seems that it is not possible to make definitive conclusions on the occurrence of psychotic symptoms in relation to methylphenidate because of methodological issues. A number of limitations are highlighted in the discussion, but the present review does have a number of strengths: it was conducted according to Cochrane guidelines, which involve thoroughness. Protocols were published before the reviews were conducted. The literature search was thorough and systematic, and pharmaceutical companies were contacted to obtain data from unpublished trials. We believe that our approach has led to the best possible gathering of relevant literature on the subject.

The results of the meta-analyses in our main publication (19) suggest that methylphenidate treatment of children and adolescents with ADHD may improve ADHD symptoms, general behaviour and quality of life. However, the magnitude of the beneficial effects cannot be established because of the low quality of the evidence. Within the short study duration typical of the included trials, methylphenidate is associated with an increased risk of non-serious adverse events, such as sleep problems and decreased appetite, but because of sparse data, we could not determine whether methylphenidate increases the risk of serious adverse events (19).