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人类大脑中功能性递质神经化学研究方法的比较。

A comparison of methodologies for the study of functional transmitter neurochemistry in human brain.

作者信息

Dodd P R, Hambley J W, Cowburn R F, Hardy J A

机构信息

Department of Pharmacology, University of Sydney, Australia.

出版信息

J Neurochem. 1988 May;50(5):1333-45. doi: 10.1111/j.1471-4159.1988.tb03013.x.

Abstract

A number of different approaches to the study of functional neurochemistry in human brain are discussed. The advantages and disadvantages of three main techniques are contrasted: (i) using animal tissue preparations as models of the human brain; (ii) using human peripheral tissue preparations as models of dynamic CNS processes; and (iii) studying human tissue, obtained postmortem, directly. Animal models are often readily obtained and reliable, and the high degree of inbreeding of common laboratory animals ensures that they usually yield consistent results. However, there are a number of human disorders for which animal models are either poor or unavailable, and species differences make extrapolation from the animal to the human case difficult. Human peripheral tissue models rely on a degree of homology between peripheral and CNS processes; in most cases, the evidence for such homologies derives from animal, rather than human, studies. Moreover, several examples are known where a peripheral process mimics the equivalent glial cell activity more closely than the neuronal, which can be a serious drawback for studies of neurotransmission. The use of postmortem human brain tissue presents a number of obvious difficulties, resulting from variations in the patient's age, agonal state, sex, preterminal medication, postmortem delay, etc. Human beings are genetically and nutritionally heterogeneous, so that data variability is usually greater here than when using tissue from laboratory animals. However, it is possible to control for a number of these factors, for example, by matching samples for basal metabolic rate and tissue integrity, and recently developed tissue freezing and storage techniques permit the use of within-subject experimental designs to help reduce experimental variation. A range of neurotransmitter functions are well retained in such tissue samples, so that regional variations, differential transmitter activities, drug effects, etc., can be studied in normal tissue samples, as well as in samples taken from cases of neurological and psychiatric disease. This allows, for example, changes in neuroanatomical indices to be correlated with localised alterations in a specific neurotransmitter function. A systematic approach to the analysis and matching of tissue samples is advocated. The three approaches should be considered to be complementary, especially for the study of human brain diseases.

摘要

本文讨论了多种研究人类大脑功能神经化学的不同方法。对比了三种主要技术的优缺点:(i)使用动物组织制剂作为人类大脑的模型;(ii)使用人类外周组织制剂作为动态中枢神经系统过程的模型;(iii)直接研究死后获得的人类组织。动物模型通常很容易获得且可靠,常见实验动物的高度近交确保它们通常能产生一致的结果。然而,有许多人类疾病的动物模型要么不佳,要么无法获得,而且物种差异使得从动物推断到人类情况很困难。人类外周组织模型依赖于外周和中枢神经系统过程之间的一定程度的同源性;在大多数情况下,这种同源性的证据来自动物研究而非人类研究。此外,已知有几个例子表明,外周过程比神经元更紧密地模拟了等效的神经胶质细胞活动,这对于神经传递研究可能是一个严重的缺点。使用死后人类脑组织存在一些明显的困难,这是由患者的年龄、濒死状态、性别、临终前用药、死后延迟等差异导致的。人类在基因和营养方面存在异质性,因此这里的数据变异性通常比使用实验动物组织时更大。然而,可以控制其中一些因素,例如,通过匹配基础代谢率和组织完整性的样本,并且最近开发的组织冷冻和存储技术允许使用受试者内实验设计来帮助减少实验变异。一系列神经递质功能在这样的组织样本中得到很好的保留,因此可以在正常组织样本以及从神经和精神疾病病例中获取的样本中研究区域差异、不同的递质活性、药物作用等。例如,这使得神经解剖学指标的变化能够与特定神经递质功能的局部改变相关联。提倡采用系统的方法来分析和匹配组织样本。这三种方法应被视为互补的,特别是对于人类脑部疾病的研究。

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