Department of Psychiatry, Stony Brook University, United States of America.
Department of Family, Population and Preventive Medicine, Core Faculty, Program in Public Health, Stony Brook University, United States of America.
Schizophr Res. 2019 Apr;206:82-88. doi: 10.1016/j.schres.2018.12.010. Epub 2018 Dec 21.
Research on a putative link between apolipoprotein-ε4 allele (APOE-ε4) and schizophrenia has been inconclusive. However, prior studies have not investigated the association between APOE-ε4 and symptom trajectories, nor has the existing literature taken into account the potentially moderating effect of age in genetic association studies.
The association between APOE-ε4 and four symptom dimensions was investigated in a longitudinal study of 116 individuals with schizophrenia initially assessed during their first admission for psychosis and evaluated five times over the following 20years. A meta-analysis identified 29 case-control studies of APOE-ε4 allele frequency in schizophrenia, which were analyzed using random-effects meta-regression to test the potentially moderating effect of age.
Longitudinal models identified a specific association between APOE-ε4 and symptom trajectories, showing that APOE-ε4 portends worsening severity of hallucinations and delusions in late adulthood among people with schizophrenia, at a rate of a 0.46 standard deviation increase per decade. Meta-analysis showed a significant effect of age: the association between APOE-ε4 and schizophrenia was not detectable in younger people but became pronounced with age, such that APOE-ε4 increased the odds of diagnosis by 10% per decade.
Taken together, the meta-analysis and longitudinal analysis implicate APOE-ε4 as an age-related risk factor for worsening hallucinations and delusions, and suggest APOE-ε4 may play an age-mediated pathophysiological role in schizophrenia. The presence of an APOE-ε4 allele may also identify a subgroup of patients who require intensive monitoring and additional targeted interventions, especially in mid-to late-life.
载脂蛋白 E4 等位基因(APOE-ε4)与精神分裂症之间可能存在关联的研究尚无定论。然而,之前的研究并未探讨 APOE-ε4 与症状轨迹之间的关联,也没有考虑到年龄在遗传关联研究中可能起到的调节作用。
我们对 116 名首发精神分裂症患者进行了一项纵向研究,这些患者在首次入院时接受了评估,并在接下来的 20 年内进行了五次评估。元分析确定了 29 项关于 APOE-ε4 等位基因频率在精神分裂症中的病例对照研究,使用随机效应元回归分析这些研究,以检验年龄的潜在调节作用。
纵向模型确定了 APOE-ε4 与症状轨迹之间的特定关联,表明 APOE-ε4 预示着精神分裂症患者在成年后期幻觉和妄想症状严重程度的恶化,每十年增加 0.46 个标准差。元分析显示年龄的影响显著:在年轻人中,APOE-ε4 与精神分裂症之间没有关联,但随着年龄的增长,这种关联变得明显,即 APOE-ε4 使每十年的诊断几率增加 10%。
总的来说,元分析和纵向分析表明 APOE-ε4 是与年龄相关的恶化幻觉和妄想的危险因素,并提示 APOE-ε4 可能在精神分裂症中发挥与年龄相关的病理生理作用。携带 APOE-ε4 等位基因也可能确定需要加强监测和额外靶向干预的患者亚组,尤其是在中年到晚年。