首页> 美国卫生研究院文献>The Journals of Gerontology Series A: Biological Sciences and Medical Sciences >Long-Term Intranasal Insulin Aspart: A Profile of Gene Expression Memory and Insulin Receptors in Aged F344 Rats
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Long-Term Intranasal Insulin Aspart: A Profile of Gene Expression Memory and Insulin Receptors in Aged F344 Rats

机译:长期鼻内胰岛素门冬治疗:老年F344大鼠的基因表达记忆和胰岛素受体的概况

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摘要

Intranasal insulin is a safe and effective method for ameliorating memory deficits associated with pathological brain aging. However, the impact of different formulations and the duration of treatment on insulin’s efficacy and the cellular processes targeted by the treatment remain unclear. Here, we tested whether intranasal insulin aspart, a short-acting insulin formulation, could alleviate memory decline associated with aging and whether long-term treatment affected regulation of insulin receptors and other potential targets. Outcome variables included measures of spatial learning and memory, autoradiography and immunohistochemistry of the insulin receptor, and hippocampal microarray analyses. Aged Fischer 344 rats receiving long-term (3 months) intranasal insulin did not show significant memory enhancement on the Morris water maze task. Autoradiography results showed that long-term treatment reduced insulin binding in the thalamus but not the hippocampus. Results from hippocampal immunofluorescence revealed age-related decreases in insulin immunoreactivity that were partially offset by intranasal administration. Microarray analyses highlighted numerous insulin-sensitive genes, suggesting insulin aspart was able to enter the brain and alter hippocampal RNA expression patterns including those associated with tumor suppression. Our work provides insights into potential mechanisms of intranasal insulin and insulin resistance, and highlights the importance of treatment duration and the brain regions targeted.
机译:鼻内胰岛素是一种改善与病理性脑衰老相关的记忆缺陷的安全有效的方法。但是,不同制剂和治疗持续时间对胰岛素功效和治疗靶向细胞过程的影响尚不清楚。在这里,我们测试了鼻内胰岛素门冬氨酸(一种短效胰岛素制剂)是否可以缓解与衰老相关的记忆力下降,以及长期治疗是否会影响胰岛素受体和其他潜在靶标的调节。结果变量包括空间学习和记忆的测量,胰岛素受体的放射自显影和免疫组织化学测量以及海马微阵列分析。接受长期(3个月)鼻内胰岛素治疗的Fischer 344只老年大鼠在Morris水迷宫任务中未显示出明显的记忆增强。放射自显影结果显示,长期治疗可减少丘脑中胰岛素的结合,但不会降低海马体中的胰岛素。海马免疫荧光的结果显示,与年龄相关的胰岛素免疫反应性下降被鼻内给药部分抵消。微阵列分析突出了许多胰岛素敏感基因,表明门冬胰岛素能够进入大脑并改变海马RNA表达模式,包括与肿瘤抑制相关的表达模式。我们的工作提供了鼻内胰岛素和胰岛素抵抗的潜在机制的见解,并强调了治疗时间和目标脑区域的重要性。

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