A randomized controlled trial comparing lithium plus valproic acid versus lithium plus carbamazepine in young patients with type 1 bipolar disorder: the LICAVAL study

LICAVAL was a randomized, unicenter, open-label, parallel-group, equivalence trial comparing the efficacy and tolerability of Li/VPA and Li/CBZ in treating type 1 BD in young individuals. Participants were allocated in a 1:1 ratio. No changes were made to trial design or outcomes after its commencement. Study reporting followed the Consolidated Standards for Reporting of Trials (CONSORT) statement [23].

LICAVAL was designed and implemented by the Mood Disorder Unit (GRUDA) at the Department and Institute of Psychiatry, University of São Paulo Medical School (IPq-FMUSP). IPq-FMUSP is a tertiary referral center located in São Paulo (Brazil).

Our study protocol complied with the Declaration of Helsinki [24]. It was approved by the institutional review board at IPq-FMUSP (protocol number: 0820/08) and registered at www.​clinicaltrials.​gov (ClinicalTrials.gov identifier: NCT00976794). Study participation was voluntary and required written informed consent. No compensation was involved.

Research volunteers were self-selected or referred. Recruitment was made through advertisements at the GRUDA website (www.​progruda.​com) and posters placed at IPq-FMUSP and other psychiatric units. Our recruitment included individuals who were hospitalized or required hospitalization.

Potential participants were pre-screened through phone interviews and further assessed at GRUDA by using the Structured Clinical Interview for the Diagnostic and Statistical Manual of Mental Disorders-IV-TR Axis I Disorders (SCID-I) [25].

Eligible participants were between 18 and 35 years old and had a diagnosis of type 1 BD in any phase of illness according to the SCID-I. Patients with clinical and psychiatric comorbidities were included as long as these comorbidities were stable. Exclusion criteria were schizophrenia, schizoaffective disorder, unstable clinical illness, and use of antipsychotics or fluoxetine in the previous month.

Study participants were allocated to receive Li/VPA or Li/CBZ. Participants were assessed weekly in the first month and fortnightly in the second month. Those who had clinical response after 2 months (acute phase of treatment) were assessed monthly for 22 months. Each assessment included all of our diagnostic instruments (see the ‘Outcomes’ section below). These medications should be administered orally. Li was initiated at 300 mg twice daily and increased weekly by 300 mg/day to reach serum levels between 0.4 and 0.8 mEq/L. VPA was initiated at 250 mg twice daily and increased weekly by 500 mg/day to reach serum levels between 50 and 125 μg/mL. CBZ was initiated at 200 mg once a day for the first two days and increased every two days by 200 mg/day to reach serum levels between 8 and 12 μg/mL. Adherence was assessed through pill counts. (Participants were asked to bring their prescribed medication during study visits.)

Other medications allowed at the discretion of psychiatrists were lorazepam 0.5–4 mg/day for insomnia and anxiety and sertraline 25–200 mg/day for bipolar depression. Sertraline was allowed only if depressive symptoms persisted after four weeks of study participation. Participants who finished their participation at the LICAVAL study were followed up at GRUDA for four additional visits over 8 weeks.

Our primary outcome was the number of participants achieving/maintaining response and remission during the acute and maintenance phases of BD treatment, respectively. Participants’ response in the acute phase of treatment was classified as response (symptom severity reduction of at least 50% with no worsening of symptoms in the opposite pole), no response (symptom severity reduction of less than 50%), and loss of response (response followed by symptom severity reduction of less than 50% in at least one visit or at the physician’s discretion). During the maintenance phase, remission was defined as a symptom severity reduction of at least 75% with no worsening of symptoms in the opposite pole.

According to our study protocol, our secondary out-come was the number of participants achieving BD remission during the maintenance phase of treatment. However, our sample size finishing this phase of the study was insufficient for this analysis. Thus, we decided to include other outcomes of interested of interest as secondary outcomes: (1) BD severity according to the Clinical Global Impressions Scale modified for use in bipolar disorder (CGI-BP) [26]. The CGI-BP is a Likert-type interviewer-rated instrument that measures severity of BD, ranging from 1 (normal, not ill) to 7 (very severely ill). (2) Symptom severity according to the Hamilton Depression Rating Scale (HAM-D) and the Young Mania Rating Scale (YMRS). These are validated and widely used interviewer-rated instruments. The HAM-D is a 17-item scale measuring depression severity [27, 28]. It has Likert-type grading, and scores range from 0 to 52. The YMRS is an 11-item multiple choice scale that measures manic symptom severity in children and young adults [29, 30]. Its scores range from 0 to 60; (3) Time-to-relapse after the acute phase of treatment; (4) use of medications: mean daily doses and serum levels of Li, VPA, and CBZ and mean daily of sertraline; (5) treatment safety and tolerability according to the Udvalg for Kliniske Undersøgelser (UKU) Side Effect Rating Scale, a 48- item clinician-rated structured interview that assesses side effects of psychotropic medications; (6) time-to-discontinuation due to side effects. At baseline, all participants provided sociodemographic information.

We used simple randomization with an allocation ratio of 1:1. Study participants were randomly assigned prior to their first study visit. To prevent selection bias, our random sequence was known by administrative staff only. These staff members were responsible for the following tasks during our study: randomization implementation, visit scheduling, and pill counting. They had no other participation in our study design, implementation, or data analysis.

Our study was open-label. Participants and psychiatrists knew which treatment was being administered. To reduce information bias, outcomes were assessed by blinded raters who had no contact with study records.

All analysis were performed by using the IBM SPSS Statistics software version 22 (IBM, Armonk, NY, USA). Significance level was 0.05.

We started our analysis by evaluating central tendency, dispersion, and distribution of all variables. Missing data were imputed through last observation carried forward. Groups were compared with an intention-to-treat approach, but we analyzed only data from participants with at least two visits.

We also used Kaplan–Meier curves to analyze time-to-relapse and time-to-discontinuation due to side effects in each group. Curves were then compared by using the log-rank test (Mantel–Cox).

Our study was conducted from January 2009 to December 2012, including patient recruitment. After screening, 64 participants were included: 36 (56.3%) in the Li/VPA group and 28 (43.8%) in the Li/CBZ group (see participant flow in Fig. 1). Owing to withdrawal of consent, four patients were excluded before any treatment (three in the Li/VPA group and one in the Li/CBZ group).

Our sample (Table 1) was composed predominantly of females (66.6%) and the average age was 27.8 years. A total of 27 (45.0%) participants had depression, 17 (28.3%) had mania/hypomania, and 16 (26.7%) had a mixed state.