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年轻的PDAPP和Tg2576小鼠海马体中的树突棘丢失及其由载脂蛋白E2基因型所介导的预防作用。

Dendritic spine loss in the hippocampus of young PDAPP and Tg2576 mice and its prevention by the ApoE2 genotype.

作者信息

Lanz T A, Carter D B, Merchant K M

机构信息

Neurobiology Unit, Pharmacia Corporation, Mail Stop 7251-209-506, 301 Henrietta Street, Kalamazoo, MI 49007, USA.

出版信息

Neurobiol Dis. 2003 Aug;13(3):246-53. doi: 10.1016/s0969-9961(03)00079-2.

Abstract

Postmortem AD brains exhibit dendritic spine loss in the hippocampus. To determine whether this pathology may be associated with amyloid burden, the present study used the Golgi stain technique to assess age- and genotype-dependent changes in dendritic spine density in CA1 hippocampus of two transgenic mouse lines that produce high levels of Abeta. Tg2576 and PDAPP mice, as well as a group of Tg2576 mice crossed with human apoE2-expressing transgenic mice, were compared to respective transgene-negative controls. Since the time course of amyloid plaque deposition in the PDAPP and Tg2576 mice is well characterized, we examined changes in spine density at ages that corresponded to different levels of amyloid plaque load. The data show age- and genotype-dependent reductions in spine density in both Tg2576 and PDAPP mice, albeit at somewhat different time courses. The spine loss occurred prior to plaque deposition and was ameliorated by the overexpression of human apoE2. These results suggest that a soluble Abeta species may affect hippocampal synapses and thereby contribute to functional deficits evident in these animals.

摘要

尸检的阿尔茨海默病大脑在海马体中表现出树突棘丢失。为了确定这种病理变化是否可能与淀粉样蛋白负荷有关,本研究使用高尔基染色技术来评估两种产生高水平β淀粉样蛋白的转基因小鼠品系的CA1海马体中树突棘密度的年龄和基因型依赖性变化。将Tg2576和PDAPP小鼠,以及一组与表达人载脂蛋白E2的转基因小鼠杂交的Tg2576小鼠与各自的转基因阴性对照进行比较。由于PDAPP和Tg2576小鼠中淀粉样斑块沉积的时间进程已得到充分表征,我们检查了与不同水平淀粉样斑块负荷相对应的年龄时的树突棘密度变化。数据显示,Tg2576和PDAPP小鼠的树突棘密度均出现年龄和基因型依赖性降低,尽管时间进程略有不同。树突棘丢失发生在斑块沉积之前,并且通过人载脂蛋白E2的过表达得到改善。这些结果表明,可溶性β淀粉样蛋白可能会影响海马体突触,从而导致这些动物出现明显的功能缺陷。

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