Department of Chemical Engineering, Virginia Tech, Blacksburg, United States.
Department of Chemistry and Biochemistry, University of California, San Diego, La Jolla, United States.
Elife. 2024 Apr 22;12:RP92393. doi: 10.7554/eLife.92393.
Genome-wide association studies have revealed >270 loci associated with schizophrenia risk, yet these genetic factors do not seem to be sufficient to fully explain the molecular determinants behind this psychiatric condition. Epigenetic marks such as post-translational histone modifications remain largely plastic during development and adulthood, allowing a dynamic impact of environmental factors, including antipsychotic medications, on access to genes and regulatory elements. However, few studies so far have profiled cell-specific genome-wide histone modifications in postmortem brain samples from schizophrenia subjects, or the effect of antipsychotic treatment on such epigenetic marks. Here, we conducted ChIP-seq analyses focusing on histone marks indicative of active enhancers (H3K27ac) and active promoters (H3K4me3), alongside RNA-seq, using frontal cortex samples from antipsychotic-free (AF) and antipsychotic-treated (AT) individuals with schizophrenia, as well as individually matched controls (n=58). Schizophrenia subjects exhibited thousands of neuronal and non-neuronal epigenetic differences at regions that included several susceptibility genetic loci, such as , and . By analyzing the AF and AT cohorts separately, we identified schizophrenia-associated alterations in specific transcription factors, their regulatees, and epigenomic and transcriptomic features that were reversed by antipsychotic treatment; as well as those that represented a consequence of antipsychotic medication rather than a hallmark of schizophrenia in postmortem human brain samples. Notably, we also found that the effect of age on epigenomic landscapes was more pronounced in frontal cortex of AT-schizophrenics, as compared to AF-schizophrenics and controls. Together, these data provide important evidence of epigenetic alterations in the frontal cortex of individuals with schizophrenia, and remark for the first time on the impact of age and antipsychotic treatment on chromatin organization.
全基因组关联研究揭示了 >270 个与精神分裂症风险相关的基因座,但这些遗传因素似乎不足以完全解释这种精神疾病的分子决定因素。表观遗传标记,如翻译后组蛋白修饰,在发育和成年期间仍然具有很大的可塑性,允许环境因素(包括抗精神病药物)对基因和调节元件的可及性产生动态影响。然而,到目前为止,很少有研究在精神分裂症患者死后大脑样本中对特定细胞的全基因组组蛋白修饰进行了分析,也很少有研究对这些表观遗传标记进行抗精神病药物治疗的影响进行了研究。在这里,我们使用来自未接受抗精神病药物治疗(AF)和接受抗精神病药物治疗(AT)的精神分裂症个体以及单独匹配的对照者(n=58)的额皮质样本,进行了 ChIP-seq 分析,重点分析了活性增强子(H3K27ac)和活性启动子(H3K4me3)的组蛋白标记物,并进行了 RNA-seq 分析。精神分裂症患者在包括几个易感性遗传基因座在内的区域表现出数千个神经元和非神经元的表观遗传差异,例如 、 和 。通过分别分析 AF 和 AT 队列,我们确定了特定转录因子及其调节因子、表观遗传和转录组特征在抗精神病药物治疗后发生的与精神分裂症相关的改变;以及那些代表抗精神病药物治疗的后果而不是精神分裂症在死后人类大脑样本中的特征的改变。值得注意的是,我们还发现,与 AF 精神分裂症患者和对照组相比,AT 精神分裂症患者的额皮质中年龄对表观基因组景观的影响更为明显。总之,这些数据为精神分裂症患者额皮质中的表观遗传改变提供了重要证据,并首次说明年龄和抗精神病药物治疗对染色质组织的影响。
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