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{beta}-Site APP Cleaving Enzyme mRNA Expression in APP Transgenic Mice : Anatomical Overlap with Transgene Expression and Static Levels with Aging

机译:{beta}-站点APP裂解酶mRNA在APP转基因小鼠中的表达:转基因表达的解剖重叠和衰老的静态水平

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摘要

The principal enzyme responsible for the ß-site cleavage of amyloid precursor protein (APP) in the brain is a membrane-bound aspartyl protease ß-site APP cleaving enzyme (BACE). We examined human APP (hAPP) and BACE mRNA expression by in situ hybridization in young and old hAPP transgenic mice from two lines: Tg2576, hAPP KM670–671NL (hAPPSw) at 4 and 15 months; and PDAPP, hAPP V717F, at 4 and 11 months. In transgene-positive mice from both lines, hAPP expression was most prominent in cortical, cerebellar, and hippocampal neuronal populations. Cingulate, entorhinal, and hippocampal amyloid burden in transgene-positive 16-month Tg2576 mice was 4 to 8%, and in 12-month PDAPP mice, 2 to 4%; there was no cerebellar amyloid deposition. BACE expression in transgenic and nontransgenic mice was highest in the cerebellar granule cell layer and hippocampal neuronal layers, intermediate in cortex, lower in subcortical regions, and minimal or absent in white matter of the cerebellum. Emulsion-dipped sections confirmed a predominantly neuronal pattern of expression. The amount of hybridization signal did not differ between transgenic and nontransgenic mice, or young and old mice, within each line. Thus, hAPP and endogenous BACE expression in similar anatomical localizations allow for processing of hAPP and Aß formation in hAPP transgenic mice, but these are modified by additional age-related and anatomical factors.
机译:大脑中淀粉样前体蛋白(APP)的ß位裂解 的主要酶是膜结合的天冬氨酰 蛋白酶ß位APP裂解酶(BACE)。 。我们通过原位杂交 在来自两个系的Tg2576, hAPP的年轻和年老hAPP转基因小鼠中检查了人 APP(hAPP)和BACE mRNA的表达KM670–671NL(hAPP Sw )在第4和15个月时;和PDAPP, hAPP V717F,分别在4个月和11个月时发布。在两个系的转基因阳性小鼠中,hAPP表达在皮质, 小脑和海马神经元群体中最为突出。转基因阳性的 16个月Tg2576小鼠的扣带, 肠和海马淀粉样蛋白负荷为4%至8%,而在12个月的PDAPP小鼠中, 2至4%;没有小脑淀粉样蛋白沉积。转基因和非转基因小鼠中的BACE表达 在小脑 颗粒细胞层和海马神经元层中最高,在皮质中居中 ,在皮质下区域较低,并且小脑白质中的 很少或没有。浸有乳剂的切片证实了 主要是神经元表达模式。每行中转基因和非转基因小鼠, 或幼老小鼠之间的杂交 信号量没有差异。因此,在相似的解剖学位置,hAPP和内源性 BACE表达允许在hAPP转基因 小鼠中对hAPP和Aß形成进行 处理,但是这些被修饰其他与年龄相关的解剖因素

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  • 来源
    《American Journal of Pathology》 |2001年第1期|173-177|共5页
  • 作者单位

    From the Alzheimer Disease Research Unit,Massachusetts General Hospital, Charlestown;

    and the Department of Brain and Cognitive Sciences,Massachusetts Institute of Technology, Cambridge, Massachusetts;

    From the Alzheimer Disease Research Unit,Massachusetts General Hospital, Charlestown;

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