Departments of Neurology, Psychiatry and Alzheimer's Disease Research Center, Mount Sinai School of Medicine, New York, NY, 10029, USA.
Mol Neurodegener. 2009 Dec 17;4:51. doi: 10.1186/1750-1326-4-51.
Recent reports suggest that latrepirdine (Dimebon, dimebolin), a retired Russian antihistamine, improves cognitive function in aged rodents and in patients with mild to moderate Alzheimer's disease (AD). However, the mechanism(s) underlying this benefit remain elusive. AD is characterized by extracellular accumulation of the amyloid-beta (Abeta) peptide in the brain, and Abeta-lowering drugs are currently among the most popular anti-amyloid agents under development for the treatment of AD. In the current study, we assessed the effect of acute dosing of latrepirdine on levels of extracellular Abeta using in vitro and in vivo experimental systems.
We evaluated extracellular levels of Abeta in three experimental systems, under basal conditions and after treatment with latrepirdine. Mouse N2a neuroblastoma cells overexpressing Swedish APP were incubated for 6 hr in the presence of either vehicle or vehicle + latrepirdine (500pM-5 muM). Synaptoneurosomes were isolated from TgCRND8 mutant APP-overexpressing transgenic mice and incubated for 0 to 10 min in the absence or presence of latrepirdine (1 muM or 10 muM). Drug-naïve Tg2576 Swedish mutant APP overexpressing transgenic mice received a single intraperitoneal injection of either vehicle or vehicle + latrepirdine (3.5 mg/kg). Picomolar to nanomolar concentrations of acutely administered latrepirdine increased the extracellular concentration of Abeta in the conditioned media from Swedish mutant APP-overexpressing N2a cells by up to 64% (p = 0.01), while a clinically relevant acute dose of latrepirdine administered i.p. led to an increase in the interstitial fluid of freely moving APP transgenic mice by up to 40% (p = 0.01). Reconstitution of membrane protein trafficking and processing is frequently inefficient, and, consistent with this interpretation, latrepirdine treatment of isolated TgCRND8 synaptoneurosomes involved higher concentrations of drug (1-10 muM) and led to more modest increases in extracellular Abeta(x-42 )levels (+10%; p = 0.001); of note, however, was the observation that extracellular Abeta(x-40 )levels did not change.
Here, we report the surprising association of acute latrepirdine dosing with elevated levels of extracellular Abeta as measured in three independent neuron-related or neuron-derived systems, including the hippocampus of freely moving Tg2576 mice. Given the reported association of chronic latrepirdine treatment with improvement in cognitive function, the effects of chronic latrepirdine treatment on extracellular Abeta levels must now be determined.
最近的报告表明,拉替拉滨(Dimebon,dimebolin),一种已退役的俄罗斯抗组胺药,可改善老年啮齿动物和轻度至中度阿尔茨海默病(AD)患者的认知功能。然而,其获益的机制仍不清楚。AD 的特征是脑外的淀粉样β(Abeta)肽积累,目前降低 Abeta 的药物是最受欢迎的用于治疗 AD 的抗淀粉样药物之一。在目前的研究中,我们使用体外和体内实验系统评估了拉替拉滨急性给药对细胞外 Abeta 水平的影响。
我们在三个实验系统中评估了 Abeta 的细胞外水平,在基础条件下和用拉替拉滨处理后。在存在载体或载体+拉替拉滨(500pM-5 μM)的情况下,将过表达瑞典 APP 的小鼠 N2a 神经母细胞瘤细胞孵育 6 小时。从 TgCRND8 突变 APP 过表达转基因小鼠中分离出突触小体,并在不存在或存在拉替拉滨(1 μM 或 10 μM)的情况下孵育 0 至 10 分钟。接受单次腹腔注射载体或载体+拉替拉滨(3.5 mg/kg)的未经药物处理的 Tg2576 瑞典突变 APP 过表达转基因小鼠。急性给予纳摩尔至皮摩尔浓度的拉替拉滨可使过表达瑞典突变 APP 的 N2a 细胞的条件培养基中外泌 Abeta 的浓度增加高达 64%(p=0.01),而临床相关的急性剂量拉替拉滨腹腔给药可使自由移动的 APP 转基因小鼠的间质液增加高达 40%(p=0.01)。膜蛋白转运和加工的重建通常效率低下,并且与这一解释一致,拉替拉滨处理分离的 TgCRND8 突触小体需要更高浓度的药物(1-10 μM),并导致细胞外 Abeta(x-42)水平适度增加(+10%;p=0.001);然而,值得注意的是,观察到细胞外 Abeta(x-40)水平没有变化。
在这里,我们报告了令人惊讶的关联,即急性拉替拉滨给药与三种独立的神经元相关或神经元衍生系统中测量的细胞外 Abeta 水平升高相关,包括自由移动的 Tg2576 小鼠的海马体。鉴于慢性拉替拉滨治疗与认知功能改善的报告关联,现在必须确定慢性拉替拉滨治疗对细胞外 Abeta 水平的影响。
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