Dhikav Vikas, Anand Kuljeet Singh
Department of Pharmacology, All India Institute of Medical Sciences, New Delhi 110029, India.
Med Hypotheses. 2007;68(6):1300-6. doi: 10.1016/j.mehy.2006.09.040. Epub 2006 Nov 13.
Hippocampus is the brain structure, vital for episodic and declarative memory. Atrophy of the human hippocampus is seen in a variety of psychiatric and neurological disorders e.g. recurrent depression, schizophrenia, bipolar disorder, post-traumatic stress disorder, epilepsy, head injury, and Alzheimer's disease (AD). Importantly, aging hippocampus also undergoes atrophy. In many instances, for example, AD, the atrophy precedes the development of symptoms while in others, there is a temporal relationship between atrophy and symptomatology. The presence of atrophied hippocampus is one of the most consistent features of many common psychiatric disorders. Several factors contribute to this atrophy. Stress is one of the most profound factors implicated and the mechanisms involve glucocorticoids, serotonin, excitatory amino acids etc. Hippocampal formation as a whole can undergo atrophy or its individual structural components e.g. apical dendrities can exhibit atrophy. Several drugs of unrelated classes have been shown to prevent atrophy indicating heterogenous manner in which hippocampal atrophy is produced. These include, tianeptine (affects structural plasticity in hippocampus and is an effective antidepressant); phenytoin (antiseizure and neuroprotective); fluoxetine (downregulates neurodegenerative enzyme and increases neuroprotective hippocampal S100 beta); lithium (neuroprotective and antiapoptotic); tricyclic antidepressants (increase hippocampal neurogenesis); antipsychotics (reduce hippocampal neuronal suppression); sodium valproate (increases neurogenesis) and mifepristone (antioxidant, neuroprotective and anti-glucocorticoid). Now the most important question is: to what extent does the hippocampal atrophy play a role in the genesis of symptoms of diseases or their progression? And if it does, can we achieve the same degree of prevention or reversal seen in experimental animals, in humans also. An even more important question is: whether the prevention of atrophy would be clinically useful in affecting disease, viz slowing its progression, reducing morbidity, complications or positively affecting the outcome of one or more of its clinically important aspects. If the answer to this is yes, we would have to know at what stage of the disease we use the drugs, dose, duration, follow-up and efficacy. The use of these drugs in the above mentioned conditions can not only test the potential of atrophy as a future drug target, but could also help in learning more about the hippocampus in both health and diseases.
海马体是一种对情景记忆和陈述性记忆至关重要的脑结构。人类海马体萎缩见于多种精神和神经疾病,如复发性抑郁症、精神分裂症、双相情感障碍、创伤后应激障碍、癫痫、头部损伤及阿尔茨海默病(AD)。重要的是,衰老的海马体也会发生萎缩。在许多情况下,如AD,萎缩先于症状出现,而在其他情况下,萎缩与症状学之间存在时间关系。萎缩的海马体的存在是许多常见精神疾病最一致的特征之一。有几个因素导致这种萎缩。压力是其中最主要的因素之一,其机制涉及糖皮质激素、血清素、兴奋性氨基酸等。整个海马体结构可能会萎缩,或者其各个结构成分,如顶端树突会出现萎缩。已证明几种不同类别的药物可预防萎缩,这表明海马体萎缩的产生方式具有异质性。这些药物包括噻奈普汀(影响海马体结构可塑性,是一种有效的抗抑郁药)、苯妥英(抗癫痫和神经保护作用)、氟西汀(下调神经退行性酶并增加具有神经保护作用的海马体S100β)、锂(神经保护和抗凋亡作用)、三环类抗抑郁药(增加海马体神经发生)、抗精神病药物(减少海马体神经元抑制)、丙戊酸钠(增加神经发生)及米非司酮(抗氧化、神经保护和抗糖皮质激素作用)。现在最重要的问题是:海马体萎缩在疾病症状的发生或进展中起多大作用?如果是这样,我们能否在人类中实现与实验动物相同程度的预防或逆转?一个更重要的问题是:预防萎缩在影响疾病方面是否具有临床实用性,即减缓其进展、降低发病率、并发症,或对其一个或多个临床重要方面的结果产生积极影响?如果答案是肯定的,我们必须知道在疾病的哪个阶段使用药物、剂量、持续时间、随访及疗效。在上述情况下使用这些药物不仅可以测试萎缩作为未来药物靶点的潜力,还可以帮助我们更多地了解健康和疾病状态下的海马体。
