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首页> 外文期刊>Neurobiology of Aging: Experimental and Clinical Research >Altered levels and distribution of IGF-II/M6P receptor and lysosomal enzymes in mutant APP and APP + PS1 transgenic mouse brains.
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Altered levels and distribution of IGF-II/M6P receptor and lysosomal enzymes in mutant APP and APP + PS1 transgenic mouse brains.

机译:突变APP和APP + PS1转基因小鼠大脑中IGF-II / M6P受体和溶酶体酶的水平和分布改变。

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摘要

The insulin-like growth factor-II/mannose-6-phosphate (IGF-II/M6P) receptor participates in the trafficking of lysosomal enzymes from the trans-Golgi network or the cell surface to lysosomes. In Alzheimer's disease (AD) brains, marked up-regulation of the lysosomal system in vulnerable neuronal populations has been correlated with altered metabolic functions. To establish whether IGF-II/M6P receptors and lysosomal enzymes are altered in the brain of transgenic mice harboring different familial AD mutations, we measured the levels and distribution of the receptor and lysosomal enzymes cathepsins B and D in select brain regions of transgenic mice overexpressing either mutant presenilin 1 (PS1; PS1(M146L+L286V)), amyloid precursor protein (APP; APP(KM670/671NL+V717F)) or APP+PS1 (APP(KM670/671NL+V717F)+PS1(M146L+L286V)) transgenes. Our results revealed that levels and expression of the IGF-II/M6P receptor and lysosomal enzymes are increased in the hippocampus and frontal cortex of APP and APP+PS1, but not in PS1, transgenic mouse brains compared with wild-type controls. The changes were more prominent in APP+PS1 than in APP single transgenic mice. Additionally, all beta-amyloid-containing neuritic plaques in the hippocampal and cortical regions of APP and APP+PS1 transgenic mice were immunopositive for both lysosomal enzymes, whereas only a subset of the plaques displayed IGF-II/M6P receptor immunoreactivity. These results suggest that up-regulation of the IGF-II/M6P receptor and lysosomal enzymes in neurons located in vulnerable regions reflects an altered functioning of the endosomal-lysosomal system which may be associated with the increased intracellular and/or extracellular A beta deposits observed in APP and APP+PS1 transgenic mouse brains.
机译:胰岛素样生长因子II /甘露糖6-磷酸(IGF-II / M6P)受体参与了溶酶体酶从反式高尔基体网络或细胞表面到溶酶体的运输。在阿尔茨海默氏病(AD)大脑中,脆弱神经元群体中溶酶体系统的明显上调与代谢功能的改变有关。为了确定IGF-II / M6P受体和溶酶体酶是否在具有不同家族性AD突变的转基因小鼠的大脑中发生改变,我们测量了过表达转基因小鼠某些脑区域中受体和溶酶体酶组织蛋白酶B和D的水平和分布突变的早老素1(PS1; PS1(M146L + L286V)),淀粉样前体蛋白(APP; APP(KM670 / 671NL + V717F))或APP + PS1(APP(KM670 / 671NL + V717F)+ PS1(M146L + L286V) )转基因。我们的研究结果表明,与野生型对照相比,APP和APP + PS1的海马和额叶皮质中IGF-II / M6P受体和溶酶体酶的水平和表达增加,而PS1转基因小鼠的大脑中IGF-II / M6P受体和溶酶体酶的表达却增加了。在APP + PS1中的变化比在APP单转基因小鼠中更明显。此外,APP和APP + PS1转基因小鼠的海马区和皮质区中所有含β淀粉样蛋白的神经噬菌斑均对两种溶酶体酶免疫阳性,而只有一部分噬菌体表现出IGF-II / M6P受体免疫反应性。这些结果表明,位于脆弱区域的神经元中IGF-II / M6P受体和溶酶体酶的上调反映了内体溶酶体系统功能的改变,这可能与观察到的细胞内和/或细胞外A beta沉积物增加有关在APP和APP + PS1转基因小鼠的大脑中。

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