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利用微阵列技术表征神经精神疾病:药物滥用和精神分裂症的尸检研究

The use of microarrays to characterize neuropsychiatric disorders: postmortem studies of substance abuse and schizophrenia.

作者信息

Lehrmann E, Hyde T M, Vawter M P, Becker K G, Kleinman J E, Freed W J

机构信息

Cellular Neurobiology Research Branch, National Institute on Drug Abuse, NIH/DHHS, Baltimore, MD 21224, USA.

出版信息

Curr Mol Med. 2003 Aug;3(5):437-46. doi: 10.2174/1566524033479690.

Abstract

Neuropsychiatric disorders are generally diagnosed based on a classification of behavioral and, in some cases, specific neurological deficits. The lack of distinct quantitative and qualitative biological descriptors at the anatomical and cellular level complicates the search for and understanding of the neurobiology of these disorders. The advent of microarray technology has enabled large-scale profiling of transcriptional activity, allowing a comprehensive characterization of transcriptional patterns relating to the pathophysiology of neuropsychiatric disorders. We review some of the unique methodological constraints related to the use of human postmortem brain tissue in addition to the generally applicable requirements for microarray experiments. Microarray studies undertaken in neuropsychiatric disorders such as schizophrenia and substance abuse by the use of postmortem brain tissue indicate that transcriptional changes relating to synaptic function and plasticity, cytoskeletal function, energy metabolism, oligodendrocytes, and distinct intracellular signaling pathways are generally present. These have been supported by microarray studies in experimental models, and have produced multiple avenues to be explored at the functional level. The quality and specificity of information obtained from human postmortem tissue is rapidly increasing with the maturation and refinement of array-related methodologies and analysis tools, and with the use of focused cell populations. The development of experimental models of gene regulation in these disorders will serve as the initial step towards a comprehensive genome-linked analysis of the brain and associated disorders, and help characterize the integration and coordinate regulation of complex functions within the CNS.

摘要

神经精神疾病通常是根据行为分类以及某些情况下特定的神经功能缺损来诊断的。在解剖学和细胞水平上缺乏明确的定量和定性生物学描述符,使得寻找和理解这些疾病的神经生物学变得复杂。微阵列技术的出现使得大规模转录活性分析成为可能,从而能够全面表征与神经精神疾病病理生理学相关的转录模式。除了微阵列实验的一般适用要求外,我们还回顾了一些与使用人类尸检脑组织相关的独特方法学限制。通过使用尸检脑组织对精神分裂症和药物滥用等神经精神疾病进行的微阵列研究表明,与突触功能和可塑性、细胞骨架功能、能量代谢、少突胶质细胞以及不同的细胞内信号通路相关的转录变化普遍存在。这些已得到实验模型微阵列研究的支持,并产生了多个在功能水平上有待探索的途径。随着阵列相关方法和分析工具的成熟与完善,以及聚焦细胞群体的使用,从人类尸检组织获得的信息的质量和特异性正在迅速提高。这些疾病中基因调控实验模型的开发将作为迈向大脑及相关疾病全面基因组关联分析的第一步,并有助于表征中枢神经系统内复杂功能的整合和协调调控。

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