Gottfries C G
Gothenburg University, Department of Psychiatry and Neurochemistry, St. Jörgen's Hospital, Hisings Backa, Sweden.
Compr Gerontol C. 1988 Dec;2(1):47-62.
Clinical and neuropathological findings in a 51-year-old woman by Alois Alzheimer (1) led to a description of the disorder which Kraepelin (2) named Alzheimer's disease (AD). In this progressive dementia disorder the senile plaques and fibrillary tangles found at brain autopsy are the diagnostic hallmarks. As the same type of neuropathological changes are found in dementias of senile age, these disorders are named senile dementia of the Alzheimer type (SDAT). The two forms are often combined into one group, the Alzheimer dementias, (AD/SDAT) and, according to the DSM-III, classified as primary degenerative disorders (PDD). However, it must be emphasized that there is no scientific basis for sampling the two forms, the diagnoses of both AD and SDAT are exclusive. Several hypotheses are being proposed as to the etiology of AD/SDAT. Genetic factors, aluminium or other toxic factors, immunological disturbances, disturbed glucose metabolism, deficiency of essential nutrients, and stress, are some of the lines followed when seeking the etiology. The pathogenesis of the disorder involves not only structural changes but also neurochemical disturbances and neuroendocrine dysfunction, findings which are related to the behavioural disturbances seen in the disease. At present there are no reliable biological markers for AD/SDAT. Clinical investigations together with laboratory data and brain imaging support the assumption of several sub-groups within the Alzheimer type dementias. The neurochemical findings made in AD/SDAT have constituted the basis for formulating pharmacological treatment strategies. Drugs affecting the cholinergic and monoaminergic systems have been used, as well as neuropeptides and similar drugs. Gangliosides and phosphatidylserine have also been tested in clinical trials. Hitherto, this treatment has not been as successful as expected. Cholinergic drugs have given a marginal effect on memory functions. Emotional disturbances and disturbed motor performance have to some extent been influenced by the use of selective 5-hydroxytryptamine reuptake blockers and L-dopa. Whether this treatment is of clinical importance must be further investigated. Interesting neuropathological and neurochemical research is being conducted on AD/SDAT. However, clinical research aiming at delimiting homogeneous subgroups of dementia has not kept in step with neurobiological research. More effort must be put into clinical research if therapeutic progress is to be achieved.
阿洛伊斯·阿尔茨海默(1)对一名51岁女性的临床和神经病理学发现,促使人们对这种疾病进行了描述,克雷佩林(2)将其命名为阿尔茨海默病(AD)。在这种进行性痴呆症中,脑部尸检时发现的老年斑和神经原纤维缠结是诊断的标志。由于在老年痴呆症中也发现了相同类型的神经病理学变化,这些疾病被命名为阿尔茨海默型老年痴呆症(SDAT)。这两种形式通常合并为一组,即阿尔茨海默痴呆症(AD/SDAT),根据《精神疾病诊断与统计手册第三版》(DSM-III),被归类为原发性退行性疾病(PDD)。然而,必须强调的是,将这两种形式归为一组没有科学依据,AD和SDAT的诊断是相互排斥的。关于AD/SDAT的病因提出了几种假说。遗传因素、铝或其他有毒因素、免疫紊乱、葡萄糖代谢紊乱、必需营养素缺乏和压力等,是寻找病因时所遵循的一些方向。该疾病的发病机制不仅涉及结构变化,还涉及神经化学紊乱和神经内分泌功能障碍,这些发现与该疾病中出现的行为障碍有关。目前,AD/SDAT没有可靠的生物学标志物。临床研究以及实验室数据和脑成像支持了阿尔茨海默型痴呆症中存在几个亚组的假设。在AD/SDAT中取得的神经化学发现构成了制定药物治疗策略的基础。已经使用了影响胆碱能和单胺能系统的药物,以及神经肽和类似药物。神经节苷脂和磷脂酰丝氨酸也已在临床试验中进行了测试。迄今为止,这种治疗并没有像预期的那样成功。胆碱能药物对记忆功能有一定的影响。使用选择性5-羟色胺再摄取阻滞剂和左旋多巴在一定程度上影响了情绪障碍和运动功能障碍。这种治疗是否具有临床重要性必须进一步研究。关于AD/SDAT正在进行有趣的神经病理学和神经化学研究。然而,旨在界定痴呆症同质亚组的临床研究没有跟上神经生物学研究的步伐。如果要取得治疗进展,就必须在临床研究上投入更多的精力。
