Study design

The study was approved by the Central Committee on Research Involving Human Subjects and the Medical Research Ethics Committee (MREC) of Alkmaar Medical Center and was conducted in accordance with the Declaration of Helsinki (World Medical Association, 2013). The study was a 26-week single-center, double-blind trial that was randomized and placebo controlled. The trial consisted of two crossover, 12-week treatment phases and a placebo wash-out period of 2 weeks in the 13th and 14th week to avoid carryover effects (Fig. 1). Clozapine dosage and use of concomitant medications were at the discretion of the treating psychiatrist and remained as much unaltered as possible throughout the study. Subjects were randomly assigned to receive an identical number of either memantine or placebo tablets. During the memantine phase a dosage of 10 mg taken once daily was built up after 1 week to 20 mg taken once daily during 11 weeks as add-on therapy to ongoing clozapine treatment. The dose of 20 mg/day was similar to the dosage used in all four randomized placebo-controlled trials in patients with schizophrenia (de Lucena et al. Reference de Lucena, Fernandes, Berk, Dodd, Medeiros, Pedrini, Kunz, Gomes, Giglio, Lobato, Belmonte-de-Abreu and Gama2009; Lieberman et al. Reference Lieberman, Papadakis, Csernansky, Litman, Volavka, Jia and Gage2009; Lee et al. Reference Lee, Lee, Lee, Park, Kim and Kim2012; Rezaei et al. Reference Rezaei, Mohammad-Karimi, Seddighi, Modabbernia, Ashrafi, Salehi, Hammidi, Motasami, Hajiaghaee, Tabrizi and Akhondzadeh2013).

Fig. 1.

Patient disposition in a double-blind, randomized, placebo-controlled trial of memantine as adjunctive treatment to clozapine in refractory schizophrenia. SAE, Serious adverse event; AE, adverse event.

Randomization to starting with either memantine or placebo was designated on a 1:1 basis in blocks of four. The allocation sequence was produced independently by the pharmacist of the VU Medical Center in Amsterdam. The code was concealed for patients, care providers, raters and investigators until all subjects had completed the trial and data had been entered into a computer data file.

Study population, inclusion and exclusion criteria

The study was performed from August 2013 until August 2014, at 12 Flexible Assertive Community Treatment (FACT) facilities of the Mental Health Service Organization North Holland North (Netherlands) (van Veldhuizen, Reference van Veldhuizen2007). The original eligibility criterion of ‘out-patients’ was broadened to patients living either independently or in a sheltered home and patients admitted to open long-stay wards, receiving care from an out-patient facility. This was reported to the MREC of Alkmaar Medical Center. Eligible subjects were between the ages of 18 and 60 years, met Diagnostic and Statistical Manual of Mental Disorders, fourth edition (DSM-IV) criteria for schizophrenia on the Mini International Neuropsychiatric Interview Plus (MINI-Plus) (Overbeek et al. Reference Overbeek, Schruers and Griez1999), and failed to achieve remission criteria proposed by Andreasen et al. (Reference Andreasen, Carpenter, Kane, Lasser, Marder and Weinberger2005), defined as simultaneous ratings of mild or less (⩽3 points) on eight of the following Positive and Negative Syndrome Scale (PANSS) items: P1 delusions, G9 unusual thought content, P3 hallucinatory behavior, P2 conceptual disorganization, G5 mannerisms and posturing, N1 blunted affect, N4 passive or apathetic social withdrawal, N6 lack of spontaneity and flow of conversation. At inclusion, duration of clozapine therapy was at least 6 months with a minimum of 12 weeks with a clozapine plasma level above 350 ng/ml or intolerability to achieve this threshold (Schulte, Reference Schulte2003). Patients with a recent deterioration needing treatment in an acute treatment ward were not included. Other exclusion criteria included pregnancy, lactating women, and female subjects without adequate contraception, known hypersensitivity to memantine, co-medication with glutamate modulators, lactose intolerance, uncontrolled epilepsy, myocardial infarction, uncontrolled hypertension, renal insufficiency, liver failure or AD (Wesemann et al. Reference Wesemann, Sontag and Maj1983). The sample size was calculated at 52, based on an ES of 0.55 (α = 0.05, power = 0.80) and accounting for an estimated discontinuation rate of 20%. After complete description of the study to the subjects, written informed consent was obtained by the principal investigator. Care providers distributed study medication and monitored compliance on a daily basis in patients in sheltered homes and open long-stay wards and on a weekly basis in out-patients.

Clinical assessments

We used the Cambridge Neuropsychological Test Automated Battery (CANTAB), a computerized, non-linguistic cognitive testing battery (Levaux et al. Reference Levaux, Potvin, Sepehry, Sablier, Mendrek and Stip2007). Test selection was based on six cognitive domains, recommended by the Measurement and Treatment Research to Improve Cognition in Schizophrenia (MATRICS): reaction time and psychomotor speed, sustained visual attention, verbal memory, visuospatial memory, learning and association ability, working visuospatial memory and strategy use, spatial planning and motor control and emotion recognition (Nuechterlein et al. Reference Nuechterlein, Green, Kern, Baade, Barch, Cohen, Essock, Fenton, Frese, Gold, Goldberg, Heaton, Keefe, Kraemer, Mesholam-Gately, Seidman, Stover, Weinberger, Young, Zalcman and Marder2008; Barnett et al. Reference Barnett, Robbins, Leeson, Sahakian, Joyce and Blackwell2010). One cognitive domain of the MATRICS Consenus Cognitive Battery (MCCB) was not assessed, because Intra/Extra-Dimensional Set-Shifting (IED) for reasoning and problem solving was too difficult for our patient population with severe cognitive disturbances.

Two cognitive domains were selected as primary outcomes: memory and executive function (see Table 2 † Footnote ¹ ). Memory was assessed by computing a composite score of the sum of the CANTAB scores of four tasks: verbal recognition memory (VRM) free recall and VRM recognition, and paired associates learning (PAL) total errors and PAL first trial memory score. To reduce practice effects a parallel form of the VRM task, equivalent in difficulty, was used for the second and fourth measurement. Executive function was assessed by computing a composite of three CANTAB task scores: One Touch Stockings of Cambridge (OTS) problems solved on first choice, and spatial working memory (SWM) strategy and SWM between errors.

The PANSS was used to assess severity of positive, negative and total symptoms of schizophrenia (Kay et al. Reference Kay, Fiszbein and Opler1987). We assessed the effect of memantine on two subdomains of negative symptoms: (1) expressive deficits [flat affect (N1), poor rapport (N3), lack of spontaneity and flow of conversation (N6), mannerisms and posturing (G5), motor retardation (G7) and avolition (G13)]; and (2) social amotivation [emotional withdrawal (N2), passive/apathetic social withdrawal (N4) and active social avoidance (G16)] (Liemburg et al. Reference Liemburg, Catelein, Stewart, van der Gaag, Aleman and Knegtering2013; Millan et al. Reference Millan, Fone, Steckler and Horan2014). Global severity of psychopathology was determined by using the Clinical Global Impression Severity Scale (CGI-S) (Guy, Reference Guy and Guy1976).

Careful clinical procedures were performed to assess safety and tolerability of memantine add-on therapy to clozapine. Physical examination included measurements of waist circumference and blood pressure. Regular controls of white blood cell count and differentiation were combined with measurements of liver and renal function, blood glucose, lipids and plasma clozapine level (12 ± 0.5 h after ingestion). The occurrence and intensity of side effects were assessed by self-rating on the Liverpool University Neuroleptic Side-Effect Rating Scale (LUNSERS) (Day et al. Reference Day, Wood, Dewey and Bentall1995) augmented with rating of Likert scales for possible side effects of memantine (thrombosis, dyspnoea, and mycosis).

All outcomes were rated before treatment initiation, after 12 weeks, after 14 weeks, and after 26 weeks. Two raters were trained in diagnostic interviewing and all clinical assessments. Inter-rater exact and adjacent agreement (within one scale point) was 96% for the PANSS, based on seven assessments (two live patient interviews and five videotaped patient interviews).

Adverse events (AEs) were defined as any undesirable experience occurring to a subject during the study, whether or not they were considered to be related to memantine ingestion. All AEs, reported by either the subject or treatment staff, were recorded. Admission to a psychiatric hospital was no reason to break the code or for withdrawal from the study. A medical emergency was the only reason to break the code and withdraw the subject from the study.

Statistical analysis

To determine the effects of memantine on the hypothesized cognitive functions, schizophrenia symptoms, safety measures, and side effects, the two phases (memantine or placebo) of the crossover trial were compared using a linear mixed-effects model conducted in SPSS Statistics version 22.0.0 (SPSS Inc., 2014). This analytic approach can estimate random and fixed effects simultaneously (Putt & Chinchilli, Reference Putt and Chinchilli1999). A natural log transformation was applied to cognitive function scores assessed via the CANTAB, which are non-normally distributed, so that estimates from the linear mixed-effects models would be trustworthy.

We conducted the analyses using an intention-to-treat (ITT) analytic approach and a per-protocol analytic approach, which included only protocol completers. Protocol completion was defined as having completed both treatment phases without a serious protocol violation in the memantine phase. There was no significant difference in study completion rate by random group assignment (group 1 = 23/26, group 2 = 21/26; χ² ₁ = 1.209, p = 0.47). We also tested a number of covariates in the model, which are potentially related to the dependent variables. Covariates included patient age and gender, years of education, age of onset, duration of psychosis and duration of untreated psychosis. We followed the backwards trimming method described by Singer & Willett (Reference Singer and Willett2003) to construct our models: as covariates were entered into the model, one at a time, those that were significantly related to one of the model's parameters were retained. Only the patient's years of education variable was related to the slope paramater; thus, this variable was retained in the final model and the others were discarded.

We first tested a model with random intercepts. However, the models failed to converge or produced errors in the Hessian matrix, so the intercept parameter was fixed to ensure trustworthy parameter estimates. The slope parameter was treated as a fixed effect after it was found that models with random slopes resulted in worse model fit. This indicates that models with fixed intercepts and slopes (i.e. constraining these parameters to be equal across participants) do not significantly differ from models in which these parameters are individually estimated. All tests of significance were two-tailed, and α was set to 0.05. Standardized ESs (Cohen's d) were calculated (Cohen, Reference Cohen1988). We performed a post-hoc analysis to assess whether memantine had a more pronounced effect on expressive deficits or social amotivation. To evaluate possible differences between in-patients admitted to long-stay wards and other included patients we performed a post-hoc analysis of demographic variables and baseline characteristics and also conducted a post-hoc analysis of out-patients, excluding patients admitted to long-stay wards.

Reliability of analyses

To include the full, randomized sample in the analyses, restricted maximum likelihood estimation was used, which has been shown to provide unbiased estimates when data are missing at random or missing completely at random (MCAR) (Little & Rubin, Reference Little and Rubin2002). There was some degree of missing data in our sample (see Tables 2 and 3 and online Supplementary Tables S1 and S2 for valid n's), but the data were determined to be MCAR (39) (χ² ₇₃₇ = 144.40, p = 1.00), so the missing data did not introduce bias into the analyses.

Two steps were taken in the analytic strategy to address unique sources of potential bias in the crossover design: (1) a period effect parameter and a period × treatment interaction were tested to determine whether the order in which memantine was received was related to the outcome and whether there was a larger effect in one of the phases of the trialFootnote ² ; and (2) carryover effects were controlled for in all analyses.

Other possible confounders were analysed, such as change in clozapine dosage, concomittant medication, substance use, and use of psychotherapy during the study. The element of expectation of the placebo response was tested by examining whether pretrial expectations of positive benefits of memantine moderated the effect on the outcomes of active drug and placebo. Further, we analysed the degree of successful blinding by examining the degree of accurate appraisal of receipt of memantine from the perspective of the patient and the rater.