Transition rates to schizophrenia and early intervention effectiveness in substance-induced and brief psychotic disorders: a randomized controlled trial

物质诱发和短暂性精神病性障碍向精神分裂症的转化率及早期干预效果:一项随机对照试验

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Abstract

This multisite, prospective randomized controlled trial examined transition rates to schizophrenia in individuals with recent-onset substance-induced psychotic disorder (SIPD) or brief psychotic disorder (BPD), and evaluated the efficacy of a specialized early intervention (SEI) designed to reduce this transition. We enrolled 1,000 participants (aged 16-40 years) across five Egyptian centers, randomly allocating them to SEI (n = 502) or treatment-as-usual (TAU; n = 498). TAU included standard antipsychotic treatment (primarily risperidone or haloperidol), monthly psychiatric follow-ups, and case management without structured psychosocial components. SEI combined monthly family psychoeducation, weekly cognitive-behavioral therapy, and low-dose risperidone (2 mg/day) with therapeutic drug monitoring. At 2-year follow-up, 26.3% of participants transitioned to schizophrenia. Transition rates were significantly higher in SIPD (29.1%) than in BPD (20.4%; HR = 1.48, p = 0.008), particularly among those with cannabis-associated SIPD (38.1%). SEI was associated with a 39% reduction in transition risk compared to TAU (HR = 0.61, p = 0.008). Key predictors included neurocognitive deficits (verbal learning OR = 0.79; working memory OR = 0.83), severe positive symptoms (OR = 1.15), and elevated inflammatory markers (CRP OR = 1.39). These findings suggest that SEI may reduce conversion, although causality cannot be definitively established. The study highlights the substantial risk of schizophrenia following a first psychotic episode, especially in the context of substance use. A comprehensive, multi-component early intervention appears effective in reducing transition rates, underscoring the importance of targeted preventive strategies.

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