Results

Recruitment took place between 1 October 2013 and 30 April 2014 and all follow-up assessments were completed by a research assistant who was blind to subject recruitment and intervention assignment. Of the 300 (30%) patients screened for eligibility in each country, 240 (80% in Hong Kong), 210 (70% in China) and 208 (69% in Taiwan) were found eligible and agreed to participate. About 30–35 patients in each country (12–17%) were approached but refused to participate, mainly due to lack of interest in the study or programme participation (n = 13–15), reluctance to talk about the illness (n = 10–12) and/or having concerns about time inconvenience for attending the intervention (n = 7–11). There were 35, 36 and 40 patients in the three countries who, after screening, withdrew from participating in this study and their demographic and clinical characteristics did not show significant difference from those of the participants in this study. Table 2 summarizes the demographic and clinical characteristics of the 342 patients in the three study groups (n = 114 in each group) and the non-participants (n = 388) who were eligible but not selected in the study. There were no significant differences in sociodemographic characteristics or antipsychotic medications between the study groups and the non-participants at baseline.

Table 2. Baseline sociodemographic and clinical characteristics of the MBPEG, conventional psychoeducation and usual-care groups and the non-participants

MBPEG, Mindfulness-based psychoeducation group; CPEG, conventional psychoeducation group; TAU, treatment as usual; s.d., standard deviation; HKD, Hong Kong dollar; df, degrees of freedom.

^a An analysis of variance (F test, df = 656) or the Kruskal–Wallis test by ranks (H statistic, df = 3) was used to compare the sociodemographic variables of patients among the three study groups and the non-participants.

^b US$1 = HK$7.80.

^c Patients were taking more than one type of psychotropic medication such as the use of either conventional and atypical antipsychotic or atypical antipsychotic together with one anti-depressant.

^d Dosage levels of neuroleptic/antipsychotic medications were compared with the average dosage of medication taken by the patients in haloperidol-equivalent mean values.

The study procedure and patient flow are presented in Fig. 1. Attritions over the 6-month treatment and 2-year follow-up periods were relatively low at 16–17% in the three study groups. Two CPEG participants during the follow-up period and one in the TAU group during the treatment period died due to chronic medical diseases, which were found unrelated to the interventions used. There were also no reported or observed adverse effects of the interventions. There were 10 and 13 participants who attended <6 (<50%) group sessions of the MBPEG and CPEG, respectively. Only limited amounts of data were missing across all measurements, with 2% of primary and 5% of secondary outcomes not being available. There was no difference in the distribution of item/measure completion between groups (χ² = 1.50, degrees of freedom = 2, p = 0.23). The three groups, and three countries under study, did not differ significantly on any baseline mean scores of the outcome variables and indicating minimal covariate effects.

Results of Box's and Levene's tests indicated no violations of the assumptions of homogeneity of variance–covariance matrices (p = 0.18) and equality of variances of the outcome variables between groups (p = 0.25), respectively. There were also few outliers, satisfactory multivariate normality and moderate correlations between the outcome measures (r = 0.20–0.46), supporting the use of the MANOVA test to compare the outcome scores between groups across the five assessment points (times 1–5). Results of mixed-model MANOVA indicated a significant interactive (group x time) treatment effect or a statistically significant difference between the three study groups (F _5,340 = 8.95, p = 0.0005; Wilks’ λ = 0.98, partial η ² = 0.34). When the results (between-group effects) for each of the outcome variables were considered separately (as shown in Table 3), the three groups indicated a significant difference on reduction in PANSS score (p = 0.003) and average length/duration of re-hospitalizations (p = 0.005), and improvement in level of functioning (SLOF score, p = 0.002) and insight into the illness/treatment (ITAQ score, p = 0.0008), using a Bonferroni's adjusted α of 0.01. An analysis of the adjusted mean scores at times 1–5 indicated that the MBPEG participants reported better progressive improvements in their length of re-hospitalizations (p = 0.05), symptom severity (p = 0.01), insight into illness/treatment (p = 0.005) and functioning (p = 0.01) than those in the CPEG. The TAU group reported progressive mild to moderate deteriorations in most of the outcome scores over the 24-month follow-up. Statistically significant differences were also found on the three SLOF subscales scores (self-maintenance, social functioning and community living skills; p = 0.002–0.005), and PANSS (positive and negative symptoms; p = 0.003 and 0.01, respectively) between the three groups across the follow-up period.

Table 3. Outcome measure scores at pre-test and four post-tests, results of MANOVA (group × time) and remission rates (n = 265)

Data are given as mean (standard deviation) unless otherwise indicated.

MANOVA, Multivariate analysis of variance; MBPEG, mindfulness-based psychoeducation group; CPEG, conventional psychoeducation group; TAU, treatment-as-usual; time 1, baseline measurement at the start of intervention; time 2, 1-week post-intervention; time 3, 6 months post-intervention; time 4, 12 months post-intervention; time 5, 24 months post-intervention; ITAQ, Insight and Treatment Attitudes Questionnaire; SLOF, Specific Level of Functioning Scale; PANSS, Positive and Negative Syndrome Scale; RR, relative risk; CI, confidence interval; NNT, number needed to treat.

^a Possible range of scores of each scale indicated in parentheses.

^b Average number of readmissions to a psychiatric in-patient unit over the previous 6–12 months at the five measurements (times 1 to 5).

^c Duration/length of readmissions to a psychiatric in-patient ward/unit in terms of average number of days of hospital stay over the previous 6 months at times 1 to 5.

^d Complete remission rates defined as 4-month simultaneous ratings of all PANSS item scores ⩽3.

^e χ² Frequency between MBPEG and TAU, CPEG and TAU.

^f RR using TAU as reference.

* p < 0.01, ** p < 0.005, *** p < 0.001.

The Helmert's contrasts tests indicated that the mean differences of the following outcomes between the MBPEG and the psychoeducation or routine-care group between two time points were significant at 0.05 and contributed to the overall multivariate significance:

1. (a) Average length of re-hospitalizations in the MBPEG was significantly greater reduced from times 1 to 4, whereas it was slightly reduced in the CPEG and consistently increased in routine care over time;

2. (b) Patients’ functioning in the MBPEG was significantly greater improved from times 1 to 4; and for the CPEG, it also consistently improved over time and differed significantly from that of the patients in routine care who showed a consistent deterioration of functioning over time;

3. (c) Patients’ mental state in the MBPEG was also significantly greater improved from times 1 to 4; and for the CPEG, it was improved and differed significantly from that in routine care at times 2 to 3; and

4. (d) Insight into illness score of the MBPEG was significantly greater enhanced from times 1 to 4 than the other two groups, whereas for the CPEG it increased slightly over time.

The above significant outcomes (ITAQ, SLOF, PANSS and length of re-hospitalizations) did not yield significant differences between the MBPEG participants in the six clinics (F _1,110 = 2.13–2.81, p = 0.15–0.28) and in groups of patients with low (<6 sessions) and high (⩾6 sessions) attendance of the intervention (F _1,105 = 2.15–3.45, p = 0.10–0.19). Appendix table in the additional information summarizes the mean scores and standard deviations of the outcome measures of the participants in the three study groups at the six clinics over the follow-up.

Complete remissions (4-month simultaneous ratings of all PANSS item scores ⩽3) were not significantly more likely in the MBPEG and CPEG than in the TAU group at times 2 and 3, but significant differences emerged during times 4 and 5. In addition, there was a significant difference on remission rate at the latest post-test between the MBPEG and CPEG [at 24 months: 38.9% v. 27.0%, χ² = 4.1, p = 0.010, relative risk (RR) = 1.9, 95% confidence interval (CI) 0.9–3.0, number needed to treat (NNT) = 2.0]. However, there were no significant differences on these rates between the three study groups across the six clinics or three countries (p = 0.12–0.38).

The differences on the estimated odds between the two intervention groups, and between the MBPEG and TAU-alone group, were significant at 12 months (Δ = 1.6 and 1.3, 95% CI 0.58–2.83 and 0.45–2.31, p = 0.022 and 0.039) and 24 months follow-up (Δ = 2.9 and 1.9, 95% CI 0.98–4.38 and 0.65–2.89, p = 0.001 and 0.010). Mixed-effects logistic regression indicated a significant differential change in proportional ORs over the 24-month follow-up; 37 and 26% of the MBPEG and CPEG participants, respectively, but only 7.2% of the TAU group were in remission (χ² = 8.9 and 8.0, p = 0.001 and 0.003, RR = 3.5 and 3.1, 95% CI 2.0–7.2 and 1.6–6.3, NNT = 3.2 and 4.6).

There were no significant differences in the medication dosages based on the converted haloperidol equivalents between MBPEG and CPEG groups (F _1,220 = 3.70, p = 0.10). Similarly, no significant differences were found across the three groups in psychotropic medications used and types, frequency or hours of participation in other individual- or family-based psychosocial interventions or psychiatric treatments (Kruskal–Wallis statistics, p = 0.12–0.25).