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抗精神病药物相关基因-miRNA 相互作用在 T 淋巴细胞中。

Antipsychotic drug-associated gene-miRNA interaction in T-lymphocytes.

机构信息

School of Biomedical Sciences and Pharmacy, Faculty of Health and Medicine, The University of Newcastle, NSW, Australia.

出版信息

Int J Neuropsychopharmacol. 2014 Jun;17(6):929-43. doi: 10.1017/S1461145713001752. Epub 2014 Jan 30.

DOI:10.1017/S1461145713001752
PMID:24480591
Abstract

Antipsychotic drugs (APDs) can have a profound effect on the human body that extends well beyond our understanding of their neuropsychopharmacology. Some of these effects manifest themselves in peripheral blood lymphocytes, and in some cases, particularly in clozapine treatment, result in serious complications. To better understand the molecular biology of APD action in lymphocytes, we investigated the influence of chlorpromazine, haloperidol and clozapine in vitro, by microarray-based gene and microRNA (miRNA) expression analysis. JM-Jurkat T-lymphocytes were cultured in the presence of the APDs or vehicle alone over 2 wk to model the early effects of APDs on expression. Interestingly both haloperidol and clozapine appear to regulate the expression of a large number of genes. Functional analysis of APD-associated differential expression revealed changes in genes related to oxidative stress, metabolic disease and surprisingly also implicated pathways and biological processes associated with neurological disease consistent with current understanding of the activity of APDs. We also identified miRNA-mRNA interaction associated with metabolic pathways and cell death/survival, all which could have relevance to known side effects of APDs. These results indicate that APDs have a significant effect on expression in peripheral tissue that relate to both known mechanisms as well as poorly characterized side effects.

摘要

抗精神病药物(APD)对人体的影响非常深远,远远超出了我们对其神经精神药理学的理解。这些影响中的一些表现在周围血淋巴细胞中,在某些情况下,特别是在氯氮平治疗中,会导致严重的并发症。为了更好地了解淋巴细胞中 APD 作用的分子生物学,我们通过基于微阵列的基因和 microRNA(miRNA)表达分析,研究了氯丙嗪、氟哌啶醇和氯氮平在体外的影响。JM-Jurkat T 淋巴细胞在 APD 或单独载体存在的情况下培养 2 周,以模拟 APD 对表达的早期影响。有趣的是,氟哌啶醇和氯氮平似乎都调节了大量基因的表达。与 APD 相关的差异表达的功能分析显示,与氧化应激、代谢疾病相关的基因发生了变化,令人惊讶的是,还涉及与神经系统疾病相关的途径和生物学过程,这与目前对 APD 活性的理解一致。我们还确定了与代谢途径和细胞死亡/存活相关的 miRNA-mRNA 相互作用,所有这些都可能与 APD 的已知副作用有关。这些结果表明,APD 对周围组织的表达有显著影响,这与已知的机制以及描述不佳的副作用都有关。

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