Maurice T, Lockhart B P, Privat A
INSERM U336, Développement, Plasticité et Vieillessement du Système Nerveux, Ecole Nationale Supérieure de Chimie, Montpellier, France.
Brain Res. 1996 Jan 15;706(2):181-93. doi: 10.1016/0006-8993(95)01032-7.
Substantial evidences suggest that the increased cerebral deposition, and neurotoxic action of the beta-amyloid peptide, the major constituent of senile plaques, may represent the underlying cause of the cognitive deficits observed in Alzheimer's disease. Herein, we attempted to verify this hypothesis by inducing a potential Alzheimer's-type amnesia after direct intracerebroventricular administration of aggregated beta 25-35-amyloid peptide in mice. In this aim, mnesic capacities were evaluated after 6-13 days, using spontaneous alternation in the Y-maze, step-down type passive avoidance and place learning in a water-maze. Pretraining administration of aggregated beta 25-35 peptide induced dose-dependent decreases in both alternation behaviour and passive avoidance, at doses of 3 and 9 nmol/mouse. A reduced but still significant impairment was observed when the peptide was not aggregated, or 'aged', by preincubation for 4 days at 37 degrees C. The beta 1-28 peptide, at 3 nmol/mouse, also induced a marked decrease in step-down latency. Posttraining, but not preretention, administration of beta 25-35 peptide also significantly impaired learning. The beneficial effects of cholinergic agents on beta 25-35-induced amnesia was examined using the cholinesterase inhibitor tacrine (THA, 1.3 and 4.3 mumol/kg i.p.) and the nicotinic receptor agonist (-)-nicotine (NIC, 0.06 and 0.2 mumol/kg i.p.). Both drugs induced a dose-dependent abrogation of the beta 25-35-induced decreases in alternation behaviour and passive avoidance. Furthermore, THA, at 1.3 mumol/kg, and NIC, at 0.2 mumol/kg, also reversed the beta 25-35-induced impairment of place learning and retention in the water-maze. Histological examination of Cresyl violet-stained brain sections indicated a moderate but significant cell loss within the frontoparietal cortex and the hippocampal formation of mice treated with aged beta 25-35 peptide (9 nmol). Examination of Congo red-stained sections in the same animals demonstrated the presence of numerous amyloid deposits throughout these brain areas. These results confirm that the deposition of beta-amyloid peptide in the brain is in some way related to impairment of learning and cholinergic degeneration and suggest that the [25-35] fragment of the beta-amyloid protein, sufficient to induce neuronal death in cultures, also induces an Alzheimer's-type amnesia in mice.
大量证据表明,老年斑的主要成分β-淀粉样肽在大脑中的沉积增加及其神经毒性作用,可能是阿尔茨海默病中观察到的认知缺陷的潜在原因。在此,我们试图通过在小鼠脑室内直接注射聚集的β25-35淀粉样肽后诱导潜在的阿尔茨海默病型失忆来验证这一假设。为此,在6-13天后,使用Y迷宫中的自发交替、阶梯式被动回避和水迷宫中的位置学习来评估记忆能力。在3和9 nmol/只小鼠的剂量下,预先注射聚集的β25-35肽会导致交替行为和被动回避的剂量依赖性降低。当该肽未通过在37℃下预孵育4天进行聚集或“老化”时,观察到损伤有所减轻但仍很显著。3 nmol/只小鼠剂量的β1-28肽也会导致阶梯式潜伏期显著缩短。在训练后而非预保留时注射β25-35肽也会显著损害学习。使用胆碱酯酶抑制剂他克林(THA,1.3和4.3 μmol/kg腹腔注射)和烟碱受体激动剂(-)-尼古丁(NIC,0.06和0.2 μmol/kg腹腔注射)研究了胆碱能药物对β25-35诱导的失忆的有益作用。两种药物均能剂量依赖性地消除β25-35诱导的交替行为和被动回避的降低。此外,1.3 μmol/kg的THA和0.2 μmol/kg的NIC还能逆转β25-35诱导的水迷宫中位置学习和记忆的损伤。对甲酚紫染色的脑切片进行组织学检查表明,用老化的β25-35肽(9 nmol)处理的小鼠额叶顶叶皮质和海马结构内存在中度但显著的细胞损失。对同一动物的刚果红染色切片检查表明,在这些脑区中存在大量淀粉样沉积物。这些结果证实,β-淀粉样肽在大脑中的沉积在某种程度上与学习损伤和胆碱能变性有关,并表明β-淀粉样蛋白的[25-35]片段在培养物中足以诱导神经元死亡,在小鼠中也会诱导阿尔茨海默病型失忆。
